| 00:03 | it started here, um three of in the front. Your job is |
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| 00:08 | watch that orange light, not the time. If he goes out, |
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| 00:12 | me know, Okay, um it be charged, but I don't I |
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| 00:16 | know. So, today is kind one of these days that for |
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| 00:21 | it's exciting, this is the type stuff I live for. This is |
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| 00:24 | I stayed in school and stuff like for you guys. It's probably gonna |
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| 00:28 | a little boring. Don't you love when a professor tell you the class |
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| 00:30 | going to be boring? Yeah, we're gonna do is we're gonna look |
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| 00:34 | uh some physiological mechanics that take place the at the level of the plasma |
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| 00:42 | . Alright. And so I just a bunch of big words in |
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| 00:44 | like, physiology. And you're oh God, physiology. Alright. |
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| 00:48 | really what we're gonna do is we're be asking the question if the if |
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| 00:52 | if that membrane, the plasma membrane a barrier, how do things move |
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| 00:56 | and forth across it. Alright. the reason we're going to ask these |
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| 01:00 | , because remember what we've done is compartmentalized the materials inside the cell versus |
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| 01:06 | the cell. And so we need be able to communicate between those two |
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| 01:11 | . And so, what we're gonna is we're looking at these chemical laws |
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| 01:15 | these chemical ideas that take place at level. So the idea here is |
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| 01:21 | order to understand how the nervous system . You need to understand these basic |
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| 01:25 | rules. If you need if you understand how muscles work, you need |
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| 01:29 | understand this basic rule. If you to know how the kidney works, |
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| 01:32 | need to understand these rules. Do see why we do this when I |
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| 01:36 | I teach this class generally, and usually, what we're looking at here |
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| 01:39 | kind of two lectures jammed together because the way the summer work. I |
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| 01:44 | the classes when I teach this is , everything that you're gonna learn after |
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| 01:48 | this week is based on or built everything we've talked about this week. |
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| 01:56 | . And so learning this stuff makes the other stuff easier. All |
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| 02:01 | And so the first part here, going to be kind of talking about |
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| 02:04 | rules about how molecules move. And gonna kind of look at this in |
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| 02:09 | in a way to make it easier understand, understand that there's some chemical |
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| 02:13 | and some physical laws like physics type that we're not even gonna bother looking |
|
| 02:17 | . All. Right. So, of this stuff, you just kinda |
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| 02:19 | to nod your head and go, , that's just how it works. |
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| 02:22 | ? But what it's gonna do, gonna help us then understand how things |
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| 02:27 | moving back and forth and how we take advantage of them. Alright? |
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| 02:30 | gonna try to use some examples to it easy for us to understand. |
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| 02:33 | so the first thing we're gonna do we're gonna look at this process called |
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| 02:36 | and what we have here in this picture that we're looking at is we |
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| 02:39 | have some sort of beaker with some in it. We've thrown a bunch |
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| 02:43 | of molecules in in this case it be diet could be whatever you |
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| 02:46 | You can think about iced tea and sugar into it or something. And |
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| 02:50 | you imagine if you drop sugar into ice tea, you guys put sugar |
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| 02:53 | your iced tea, right? You drink iced tea? Okay. No |
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| 02:58 | , this is at least you said , this is the south. We |
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| 03:01 | to learn how to drink our T I know it is sweet |
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| 03:04 | but don't tell them yet. We'll to that in a minute. We'll |
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| 03:07 | about sweet tea in a second. right. But you put sugar and |
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| 03:11 | and it just goes right down to bottom right? And if you left |
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| 03:14 | there and gave it an infinite amount time, those sugar molecules which are |
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| 03:19 | kind of densely packed are gonna be . Now I don't like hanging out |
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| 03:23 | these other molecules. I want to out and give me some elbow |
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| 03:26 | And so that's really what the process diffusion is. It's basically these molecules |
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| 03:30 | into each other and bumping into each with the same degree of frequency until |
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| 03:34 | they spread out. And so that still bump into each other with the |
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| 03:38 | degree of frequency, but they're they're spread out throughout the environment in which |
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| 03:42 | in right now, this is a simple model of diffusion and there's some |
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| 03:48 | that govern diffusion and we're gonna look the first two rules about the rate |
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| 03:51 | diffusion. The rate of diffusion is upon the steepness of the gradient. |
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| 03:57 | , what that means in english is you think about a skateboard and you |
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| 04:01 | yourself on a skateboard and you and do this in Houston, are you |
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| 04:05 | go anywhere? No, that's You said no, sir? |
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| 04:09 | okay. Yeah. No. No. Do you go anywhere because |
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| 04:14 | , it's flat in Houston. So you get on a skateboard, it's |
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| 04:17 | going to move anywhere. But let's we move a little bit west, |
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| 04:22 | moving in the hill country, we ourselves a little bit of a hill |
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| 04:25 | I stand on that tape, or I going to start moving a little |
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| 04:29 | ? All right. But if I myself to colorado, Now, I've |
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| 04:32 | these steep slopes. If I get the skateboard, am I gonna be |
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| 04:36 | ? Yes, And I'm gonna be fast or slow fast. In other |
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| 04:40 | , the steeper the hill becomes the I go. And that's the simple |
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| 04:44 | you already understand, and that's gonna the same principle that applies here, |
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| 04:48 | steeper, the greater the more stuff have close together, the faster those |
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| 04:53 | bump into each other and the faster disperse. All right, So, |
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| 04:56 | rate of diffusion increases. Alright, # one. The second thing is |
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| 05:04 | to do with temperature. All Now, we're getting to the sweet |
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| 05:09 | . All right. If I dump in the tea, we said that |
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| 05:13 | over time it might take an infinite of time, but eventually it's those |
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| 05:17 | sugar going to spread around. But want our tea sweet right now because |
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| 05:23 | hot. It's texas. So, do we do if it's unsweetened tea |
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| 05:28 | we put sugar in it? What we do to it? How do |
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| 05:31 | get that sugar mixed in? We it. And really what we're saying |
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| 05:35 | how do we defuse the sugar? so what we do is we mix |
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| 05:39 | by stirring. And really what we're is we're not just stirring. We're |
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| 05:44 | applying kinetic energy, which is what is. The temperature is just applying |
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| 05:49 | to the molecules so that they begin around. And so as you increase |
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| 05:56 | , you'll get increased diffusion now to us a step down here in the |
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| 06:01 | . And because it's hot all the , what we do is we take |
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| 06:04 | tea while it's still hot and we throw the sugar into it and then |
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| 06:08 | sugar because of the heat of the the fluid basically disperses. And that's |
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| 06:13 | we get sweet tea and we just ourselves a step because this takes time |
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| 06:17 | it's no fun. And we all sweet tea in the first place. |
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| 06:20 | right. So, temperature has a effect on the rate of diffusion. |
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| 06:26 | causes diffusion to occur much more All right. When you drop the |
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| 06:31 | , you're removing kinetic energy and so move much more slowly, so things |
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| 06:36 | much more slowly. All right, , this is just a simple |
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| 06:42 | And you'll notice that what we have we have an open environment. |
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| 06:45 | So, if you could think of body as being remember, we had |
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| 06:48 | two areas intracellular fluid and extra cellular . If we put a whole bunch |
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| 06:53 | stuff into the extra cellular fluid, gonna diffuse and equally distribute itself around |
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| 06:58 | extra cellular fluid. But our bodies those two compartments And so we have |
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| 07:02 | concern ourselves. Now with that barrier those two compartments. How do we |
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| 07:07 | the stuff over in this compartment over that compartment? And here's where we're |
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| 07:11 | start looking at a couple of different . Alright, Of course it helps |
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| 07:15 | I actually press the button to allow to do that. There we |
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| 07:24 | All right. So, with regard movement here, now, we can |
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| 07:28 | this would be like where the extra fluid, this is intracellular fluid. |
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| 07:32 | have this lipid bi layer and that bi layer we said serves as a |
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| 07:35 | between the two compartments. What it is that it excludes things that sit |
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| 07:40 | water, things that are water So just like me, I can't |
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| 07:45 | through this wall. I need to some mechanism to allow me to pass |
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| 07:49 | that wall. What would be the to allow me to pass through this |
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| 07:54 | ? A door? And that's what have is we have different types of |
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| 07:58 | . Now, the truth is, that some molecules are very, very |
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| 08:03 | and or are lipid soluble, meaning they're able to pass through the lipid |
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| 08:08 | layer. So when that occurs, happens is those materials are going to |
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| 08:13 | the same rules we learned over where there's lots we move away from |
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| 08:18 | to where we are equally distributed. you move from an area of high |
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| 08:22 | to an area of low concentration so . So good. So, that's |
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| 08:27 | rule that we first learned. We from areas of high concentration areas of |
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| 08:30 | concentration. If that molecule is capable passing through that lipid bi layer, |
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| 08:38 | uses the process of simple diffusion to so what that means is that that |
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| 08:43 | , that membrane is permeable to that ? All right. But if that |
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| 08:48 | is impermeable, that substance, that needs some other mechanism to get |
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| 08:52 | And so that means it needs some . It needs to be facilitated. |
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| 08:57 | we call the other mechanisms facilitated Alright. And there's a bunch of |
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| 09:03 | types. One type of facilitated diffusion using a channel. Alright, |
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| 09:08 | channel mediated diffusion is like a Alright. We have a door that |
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| 09:14 | me to go back and forth. door happens to be closed, but |
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| 09:17 | can open it. Right. And when you're dealing with channel media |
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| 09:21 | you have an open path that allows to pass through it. When that |
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| 09:27 | is open, it's completely open on sides. Just like if we open |
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| 09:30 | those doors because we have two doors , if we open those doors, |
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| 09:33 | anything wander in or out? dogs, raccoons, bees, other |
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| 09:40 | . Right. So there's nothing that's barrier in a channel if it's |
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| 09:45 | And the only thing that you're dependent now is a concentration gradient. If |
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| 09:49 | have lots of stuff on this side very little stuff on that side, |
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| 09:53 | move into the cell and I have of stuff on this side. And |
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| 09:57 | little stuff on that side. Then move out of the cell. The |
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| 10:01 | thing to understand here though is that doors are specific, they are specific |
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| 10:07 | the type of molecules that they allow pass through them. All right. |
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| 10:12 | other type is the carrier mediated if you want to think about carrying |
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| 10:16 | different types of carrier media, but looking right here right now alright, |
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| 10:20 | carrier mediated, this is just like door except that it's only open to |
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| 10:25 | side at a time. The best I can think about is one of |
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| 10:28 | rotating doors that you see at hotels at airports. You know what I'm |
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| 10:32 | about? You got your suitcase and walk right up to it and you're |
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| 10:36 | of like, okay, I've got get the timing right, and then |
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| 10:38 | like get in and you're like and you jump out on the other |
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| 10:42 | There's a point where if that stopped , you would neither be inside or |
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| 10:46 | and that's kind of how this It's like you go in and then |
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| 10:50 | it opens up your I mean, closed up on this side. Now |
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| 10:54 | not exposed to either side and then open up to the other side |
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| 10:57 | the same rules apply. I moved areas of high concentration to areas of |
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| 11:01 | concentration. Alright now, both of mechanisms that you're looking at here are |
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| 11:06 | to as passive diffusion. You're basically the mechanism to allow you move from |
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| 11:11 | area of high concentration in the area low concentration and you just have to |
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| 11:14 | which side has the higher the lower . Another type of career media diffusion |
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| 11:19 | referred to as active transport. We're look at this a little bit more |
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| 11:23 | probably in another slide. And the here is we're moving against our concentration |
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| 11:27 | , We're moving from low to high because it's called active, it means |
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| 11:32 | uses energy to do so, but go into more detail on the |
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| 11:35 | So it's on the next slide. you go. So here I'm using |
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| 11:43 | . I'm using a carrier when I'm with primary active transport. I'm using |
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| 11:49 | directly. All right. In other , think of it like a bubble |
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| 11:52 | machine. If I take a quarter stick the quarter in the bubble gum |
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| 11:55 | and turn the crank, I get gum out the quarter is the energy |
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| 11:59 | allow me to get my bubble gum . Alright, so that's kind of |
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| 12:03 | the primary active transport works. I my molecule, it binds and says |
|
| 12:08 | ready to go. And then as as energy is there, then that's |
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| 12:11 | be the thing that cranks the machinery allow you to move the thing |
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| 12:15 | Now, the reason we need energy this case is because we're moving something |
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| 12:19 | a direction that doesn't naturally want to . All right, think about this |
|
| 12:24 | I put um a bunch of ping balls into a closet and I opened |
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| 12:29 | door, which way the ping pong are gonna want to go, or |
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| 12:32 | gonna want to come out and roll , or they're gonna want to stay |
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| 12:34 | the closet, they're gonna want to out, and So, what you |
|
| 12:38 | here is a mechanism that kind of a little part of the door to |
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| 12:41 | something in. so it doesn't come out again. And what you're doing |
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| 12:44 | you're moving things where it doesn't want go when you move things in that |
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| 12:50 | , when you create that concentration and things in and creating more and more |
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| 12:55 | more of that same substance. What doing is you're creating potential energy, |
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| 13:00 | like lifting a ball and putting it a shelf. The ball wants to |
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| 13:04 | to the ground, but you had impart energy to move the ball up |
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| 13:08 | put it on the shelf, All you gotta do is bump the |
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| 13:11 | or tilt the shelf just a little and the ball is gonna come rolling |
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| 13:14 | the shelf, right? So primary transport is imparting energy and that energy |
|
| 13:21 | stored where you're putting that particle, I'm just gonna use again, here's |
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| 13:26 | concentration gradient. So there's a little , there's lots, so, by |
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| 13:30 | this in here and then over I've now put more particles where there's |
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| 13:34 | lots of particles and the particles want go this direction. Secondary active transport |
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| 13:41 | taking advantage of that gradient that you created. So the energy is expended |
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| 13:49 | , but now it's stored over here so here in secondary active transport, |
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| 13:55 | gonna use the stored energy to move else. Alright, so the example |
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| 14:01 | , I mean, I don't know I'm actually doing, No, I'm |
|
| 14:04 | using a direct one. So an here would be I have moved one |
|
| 14:11 | over here. Now this particle wants go back because that's the directions concentration |
|
| 14:16 | . It's not allowed to go back it brings something else along with |
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| 14:21 | All right. That's where the secondary transport. I'm using the energy that |
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| 14:24 | stored up by pumping things over here that's gonna naturally want to go |
|
| 14:29 | but it's not allowed to go back it brings something. Now I'm gonna |
|
| 14:34 | a really bad example. You ready the really bad example? Alright. |
|
| 14:38 | I told you, where did I to school? Do you guys remember |
|
| 14:40 | I went to college, Chilean New Orleans? New Orleans is a |
|
| 14:45 | city, especially if you go to there. All right. And my |
|
| 14:49 | , we like to have fun in . You guys apparently don't like to |
|
| 14:51 | fun. We have fun. and In New Orleans there is a |
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| 14:56 | about every three ft. All and around the campus especially there are |
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| 15:01 | and tons of bars and every night was a ladies night at one of |
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| 15:05 | bars. Now what they do is would charge a cover to get into |
|
| 15:09 | bar. Ladies could get in Um And guys wouldn't have to pay |
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| 15:14 | cover if they weren't brought went in a girl. Right? And so |
|
| 15:19 | idea was is like all right, want to go in and I want |
|
| 15:22 | going drinking, I want to meet . Girls want to get in, |
|
| 15:25 | don't want to pay for drinks. now we've got some sort of symbiotic |
|
| 15:29 | going on here, right? All gotta do is hang out outside the |
|
| 15:32 | say hey, if you let me in with you, I'll buy you |
|
| 15:35 | drink. And who who benefits both us. Right. And that's kind |
|
| 15:39 | what? Secondary active transport is. active transport. I've got molecules sitting |
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| 15:44 | here going, I want to get but I can't no one's letting me |
|
| 15:47 | . I don't want to pay the . And then we have a mechanism |
|
| 15:50 | allow us to move in. But we gotta do is bring another molecule |
|
| 15:53 | for the ride and say, if you come with me, I'll |
|
| 15:57 | you to where you need to And it's like, okay, |
|
| 16:00 | buy my drink and off you Terrible example, But can you visualize |
|
| 16:07 | ? Alright, we're gonna see some of this that you're in just a |
|
| 16:12 | , that you will not have to . But you're going to see that |
|
| 16:15 | are mechanisms all of these are mechanisms cells use to move molecules, particularly |
|
| 16:22 | back and forth across the membrane. , so with secondary active transport, |
|
| 16:27 | potential energy is being used to move against their own concentration gradient. All |
|
| 16:34 | now, these are the rules of . These are are summed up in |
|
| 16:40 | called fixed law of diffusion. you can go look up fixed law |
|
| 16:44 | you want to. In fact, you go on to uh Wikipedia and |
|
| 16:48 | up fixed law and see how he these. It's really kind of cool |
|
| 16:51 | he figured this stuff out in the 17 hundreds and he like created these |
|
| 16:55 | tubes, like as long as his and determined all these different things that |
|
| 17:00 | talking about here. But we're not go through the history. We just |
|
| 17:03 | to know what we need to All right. So, when we're |
|
| 17:06 | with the fusion across the membrane, , here's you can see I've got |
|
| 17:09 | concentration, there's low concentration. There's membrane. That's the part that allows |
|
| 17:14 | to pass through. There's some simple , size matters. All right. |
|
| 17:18 | bigger the salute, the harder it to move, the smaller the |
|
| 17:22 | the easier it is to move. way I think about this is um |
|
| 17:26 | have I don't have young kids but I used to have really, |
|
| 17:29 | young small kids and I take them have four of them, alright. |
|
| 17:33 | they're like gas molecules, they're always all sorts of different directions, |
|
| 17:37 | So, if I take them to sporting event, for example, um |
|
| 17:41 | kind of a big guy and when walking through a crowd, I bump |
|
| 17:44 | people, I have to say, me, and I have to kind |
|
| 17:46 | move sideways do this stuff. And of my kids do, they let |
|
| 17:49 | of my hands and they start zipping people's legs, right? And I |
|
| 17:53 | them in a crowd. So big hard to move when there's lots of |
|
| 17:58 | big things around, small things easy move around because they can zip between |
|
| 18:03 | . So the size of the salute when it comes to the radio |
|
| 18:06 | The smaller the salutes, the easier are to move. All right. |
|
| 18:10 | thing, membrane thickness. And this be pretty simple to understand if I |
|
| 18:14 | to move through something that's this you know, versus something that's that's |
|
| 18:18 | . It's gonna take less time to through it, right? So the |
|
| 18:21 | the thinner something is, the easier is to pass through It does that |
|
| 18:24 | of makes sense? Yeah. Okay, let me think about |
|
| 18:28 | Um Alright to get outside. we have this hallway, right? |
|
| 18:33 | , let's pretend the hallway is actually membrane, right? So, it |
|
| 18:38 | take longer to get from that door out to the other door to outside |
|
| 18:42 | it would if it was just a door, right? The thinner door |
|
| 18:46 | easier to pass through than the door the hallway in the door. |
|
| 18:50 | thickness matters, surface area matters. right. Um How many people do |
|
| 18:56 | think could fit through that these doors here? At the same time. |
|
| 19:01 | sounds good. I like four. . If we took one of those |
|
| 19:04 | away, how many could fit Two? Right, so the more |
|
| 19:09 | area we have, the easier it to pass people through that membrane. |
|
| 19:14 | , so more surface area, so just allowing more things to pass |
|
| 19:18 | You can think about the highway, you think about Highway 59 Highway 59 |
|
| 19:22 | like six lanes over there in front Lakewood Church, right? So traffic |
|
| 19:26 | really, really easy. But if down closer to where 59 2 88 |
|
| 19:31 | of separate, you have two lanes there's always traffic even in the middle |
|
| 19:35 | the night, there's people backed up there's just two lanes, the amount |
|
| 19:39 | traffic can't pass through because there's not surface area. This is again the |
|
| 19:47 | , so the steeper the gradient. the more stuff you got, the |
|
| 19:50 | it's going to move, the more the gradient, the slower it's going |
|
| 19:54 | move temperature. We mentioned as as you increase temperature that implies, |
|
| 20:01 | or applies kinetic energy so that things going to move faster. And |
|
| 20:06 | the viscosity of the solution. So what we do is we talk about |
|
| 20:10 | alright. And so typically that's what solutions are primarily water but a solution |
|
| 20:14 | water plus stuff. And so you have other things in that solution. |
|
| 20:18 | so we're not gonna worry about it much, but in some cases you |
|
| 20:21 | have to go, oh there's more just what I'm dealing with here. |
|
| 20:24 | so this will slow things down. it easier to pour out water than |
|
| 20:28 | is to pour out honey? so honey has a lot of stuff |
|
| 20:32 | it. And so you can imagine to diffuse through honey would be harder |
|
| 20:35 | diffusing through water. Alright, and this charge just kind of shows |
|
| 20:40 | it's like what what how it It increases or decreases it. So |
|
| 20:47 | kind of shows you really more like going on and you can look at |
|
| 20:51 | top here and the top refers to if we only had one salute? |
|
| 20:55 | right now, it is just simply one substance that that we're interested |
|
| 21:00 | So the term flux refers to the of diffusion. So if you ever |
|
| 21:03 | flux, that's just saying, how are these molecules moving? So you |
|
| 21:07 | see here, I've got lots of . This membrane right here allows for |
|
| 21:11 | particles to pass through it. So permissible to this particle. And so |
|
| 21:15 | rate of diffusion or the flux, just going to be dependent upon that |
|
| 21:20 | gradient. And they're gonna keep moving what we have is we have the |
|
| 21:24 | of movement in one direction equal to rate of movement in the other |
|
| 21:28 | Now you'd say wait a second, less over there. So wouldn't they |
|
| 21:31 | go that way until everything stops And the truth is, molecules don't |
|
| 21:35 | moving right, I can have a over here trying to move against its |
|
| 21:40 | gradient. It's really hard for it do so. But you know, |
|
| 21:43 | it's bouncing off stuff it can do . And so what you're dealing with |
|
| 21:47 | molecules hitting each other until the rate them hitting each other is equal on |
|
| 21:51 | sides of that membrane. So there's that are going this way, some |
|
| 21:54 | are going that way and that rate the same and that's what we refer |
|
| 21:57 | as being equilibrium. Alright, so here we are out of equilibrium |
|
| 22:02 | we're out of equilibrium here, we in equilibrium. The rate of diffusion |
|
| 22:06 | here is faster than the rate of over there. Right. Because the |
|
| 22:10 | have changed until finally the rate of diffusion is equal in both directions. |
|
| 22:19 | , our bodies don't have one We have lots and lots and lots |
|
| 22:25 | salutes. Even in our first couple lectures we talked about there being different |
|
| 22:31 | concentrations of ions in these compartments. mentioned potassium, we mentioned sodium, |
|
| 22:36 | mentioned chlorine, we mentioned these cellular proteins, which are the four |
|
| 22:41 | . But those aren't the only ones got magnesium, you have phosphates. |
|
| 22:45 | tons of stuff in our bodies and have to consider each of those things |
|
| 22:50 | we're looking at some of these reactions some of these activities. And so |
|
| 22:54 | kind of shows you what's really kind going on. So, if you |
|
| 22:56 | imagine this over here is extra This over here is intra cellular cellular |
|
| 23:02 | I have two different molecules. Each has its own flux. So the |
|
| 23:07 | of flux in this direction for red pretty fast. The rate of flux |
|
| 23:10 | blue is really fast in that Right? And so they're just moving |
|
| 23:15 | each other, independence of each All right. And so, you |
|
| 23:20 | see still the rate of diffusion for just gonna look at blue here here |
|
| 23:25 | really fast. But here it's gonna slower because we've got some on this |
|
| 23:28 | . And eventually what's gonna happen is gonna reach equilibrium for blue and you |
|
| 23:33 | reach equilibrium also for red. And , what you see now is you |
|
| 23:38 | different equilibrium. This would refer to net flux. Alright, So two |
|
| 23:44 | flux is going in different directions. , flux number one flux number |
|
| 23:49 | And then by here we're now into for each of those independent flux. |
|
| 23:56 | I want you to think about for moment about your breathing when we breathe |
|
| 24:01 | and breathe out. Let's talk about in. Well, let's breathing in |
|
| 24:05 | breathing out. What are you breathing ? What's that oxygen? Close close |
|
| 24:15 | , that's what I'm looking for. . Not a tricky question, no |
|
| 24:19 | . But you're you're thinking it's okay, I'm so used to them |
|
| 24:21 | me such a specific question. it's air you're breathing. But what |
|
| 24:24 | your body want? And your first was correct. Oxygen. Right? |
|
| 24:29 | we breathe in and breathing out, dealing with multiple Items will be dealing |
|
| 24:34 | multiple molecules. All right. But only concerned with one for our |
|
| 24:39 | But still, when I breathe I'm breathing in 79% nitrogen. I'm |
|
| 24:44 | breathing in 20% oxygen and I'm breathing something my body wants to get rid |
|
| 24:49 | carbon dioxide plus a whole bunch of stuff. My body doesn't want. |
|
| 24:53 | right. The movement of air is representation of a process called bulk |
|
| 25:00 | bulk floats simply refers to entire solutions areas of solution. It's a mixture |
|
| 25:05 | a bunch of gasses. And basically we're doing is we're moving from an |
|
| 25:09 | of high pressure to an area of pressure. All right. So, |
|
| 25:13 | I breathe in I'm pulling in all of things. I'm moving from high |
|
| 25:17 | to low pressure. When I'm breathing , I'm creating high pressure in my |
|
| 25:21 | and I'm pushing out air again. has my air concentrations changed in that |
|
| 25:28 | . Go ahead and your head and yes, because I turned oxygen into |
|
| 25:33 | dioxide and I'm breathing out a little more carbon dioxide than I was breathing |
|
| 25:37 | , Alright, But I'm still breathing oxygen, right? And so bulk |
|
| 25:42 | simply refers to that movement. Think your blood in your blood. You |
|
| 25:48 | water and blood cells and molecules and molecules and even more molecules that we're |
|
| 25:54 | going to bother naming. And for , one of those molecules is glucose |
|
| 25:59 | that glucose is trying to get to cell so that it can be used |
|
| 26:02 | fuel, right? It's not gonna like, oh well I'm just gonna |
|
| 26:06 | the glucose. I'm sending everything along it along with the waste that those |
|
| 26:11 | produce. And so that is also example of bulk flow. So molecules |
|
| 26:18 | by rules that we've just described diffusion whatnot. But that's looking at an |
|
| 26:24 | molecule they also follow or rules that the whole solution itself. So when |
|
| 26:32 | breathing in we're breathing in a whole of things. Moving things again with |
|
| 26:37 | concentration gradient. But then when we're oxygen we're following the rules for that |
|
| 26:42 | molecule. We're moving carbon dioxide. following its own rules as well. |
|
| 26:47 | we gotta understand there's some complexities and molecules move. Alright now the good |
|
| 26:52 | is we're not going to deal with until A and P. Two. |
|
| 26:55 | understanding this concept is going to help understand respiration. The cardiovascular system and |
|
| 27:01 | renal system when they come up, , That's the fun part in the |
|
| 27:08 | . You get to use this in future. You'll get to use this |
|
| 27:11 | far. We're okay with stuff. three nods. And the people in |
|
| 27:16 | back falling asleep. I really, want to bring a silly string Class |
|
| 27:23 | Day. Just see if you guys up. Alright. So what we |
|
| 27:29 | have is we have a term that use when we talk about a |
|
| 27:33 | You've already heard me use this term this morning and it refers to |
|
| 27:38 | Alright. So what we do is say that membrane is permeable when it |
|
| 27:43 | a substance to pass through it. for example, our plasma membrane is |
|
| 27:49 | to oxygen. It's permissible to carbon . Alright, so that means there's |
|
| 27:54 | barrier here for those molecules. It even see the barrier just passes on |
|
| 28:00 | . So materials are going to move an area of high concentration to an |
|
| 28:03 | of low concentration, simply by following rules of diffusion or simple diffusion. |
|
| 28:09 | . We have other molecules like ethanol, water which are polar molecules |
|
| 28:15 | they shouldn't be present, prevented or shouldn't be allowed to pass through but |
|
| 28:19 | still permeable membranes still permissible to them some other sorts of chemical reasons we're |
|
| 28:25 | going to go into. If a is not allowed to pass through like |
|
| 28:31 | , glucose is too big and it's , it will not be able to |
|
| 28:35 | through. It just sits out here the water. It needs a mechanism |
|
| 28:37 | allow it through. So what we is that the membrane is impermeable. |
|
| 28:41 | the glucose or membranes are impermeable to . So, there has to be |
|
| 28:47 | sort of mechanism to allow them to through one of those uh facilitated transport |
|
| 28:52 | that we looked at. And then we look at a membrane itself, |
|
| 28:55 | we do is we say, it allows some things to pass through |
|
| 28:59 | other things it doesn't. So, means it has selectivity. It determines |
|
| 29:03 | gets to decide when things are going go through it. All right. |
|
| 29:08 | , a membrane is permeable to some like oxygen, carbon dioxide, but |
|
| 29:12 | impermeable to others. And then there's be times when we put channels through |
|
| 29:16 | allows for membranes or these materials to through. So, all the membranes |
|
| 29:21 | all ourselves cells are collectively selective. . They're selectively permeable. But when |
|
| 29:27 | looking at a substance, we can that membrane is permeable to blank. |
|
| 29:33 | that number collection kind of makes Alright. Alright. The dread |
|
| 29:40 | How many guys have learned about osmosis ? All right. If we didn't |
|
| 29:44 | about it. How many think you explain to somebody else clearly. So |
|
| 29:47 | they understood it and that you could a perfect score on the test on |
|
| 29:53 | . Yeah. See that's I don't . All right. Osmosis is one |
|
| 29:58 | those terms that everyone screws up. . I remember sitting in your seats |
|
| 30:04 | first time and not understanding. And I'm going to just memorize what they |
|
| 30:07 | me and I'm gonna vomit it back the exam. And I remember being |
|
| 30:10 | grad school going okay. I vaguely what osmosis is and I'm just gonna |
|
| 30:13 | like I know and stuff like It wasn't until I started teaching when |
|
| 30:17 | was like, oh this is the thing as why do people keep explaining |
|
| 30:20 | so poorly to me? All you ready for the easy explanation? |
|
| 30:25 | the chemist explanation. Because those are people that screw us up because what |
|
| 30:28 | chemist will tell you is like osmosis the movement of water to an area |
|
| 30:32 | higher concentration of solute. And all a sudden now you're like what |
|
| 30:37 | Because we've already learned a really, simple definition. We said what is |
|
| 30:42 | , diffusion is things moving from high , low concentration. But if I |
|
| 30:45 | osmosis is water moving to an area higher solute concentration all of a sudden |
|
| 30:49 | makes a lot of not sense. ? You said I'd use bad language |
|
| 30:55 | , right? The idea here is changing what you're focusing on. |
|
| 31:02 | and osmosis is simply water diffusion. you learn that it's water diffusion, |
|
| 31:10 | it just makes sense. Okay, there are physical rules that govern |
|
| 31:14 | There are chemical rules that govern And I'm gonna try to see if |
|
| 31:17 | makes sense to you by drawing this . Give you guys a little bit |
|
| 31:22 | light. Not at all help. right here I have a container with |
|
| 31:32 | membrane. Alright, if I put say 70% water here, and |
|
| 31:41 | I don't know 30% water there. way do you think the water? |
|
| 31:45 | this membrane is permeable to water? way is the water gonna go? |
|
| 31:49 | going to go to the right? very, very simple. Alright, |
|
| 31:52 | notice I have 70% water here when talk about the fusion, we talk |
|
| 31:56 | salute in water. And now what talking about, how does the water |
|
| 32:00 | If it's 70% water? What's 30% of Who knows saw you? |
|
| 32:07 | , It's just we don't care what is. It's something that means this |
|
| 32:12 | 70% of something. We don't know it is. But instead of focusing |
|
| 32:18 | this, just focus on this part there. Just focus on the |
|
| 32:23 | Because the question is asking when you're with osmosis, if you have a |
|
| 32:27 | permeable to water, which direction does water go? It moves to where |
|
| 32:32 | less water. That's pretty simple. rolls downhill. Something you've already |
|
| 32:39 | All right now the chemists get confusing they sit here and start focusing on |
|
| 32:45 | , you have a high water concentration here and you have a high solute |
|
| 32:49 | over there, Which way does the go? And all of a sudden |
|
| 32:53 | you have to do brain translation of that means. And really wherever you |
|
| 32:57 | high. So you just think that low water. Okay, And that's |
|
| 33:02 | the language of osmosis comes in. start dealing with that that conversion. |
|
| 33:08 | so you have to kind of do small translation in your brain to always |
|
| 33:12 | I've got to come back to the . All right. So osmosis is |
|
| 33:17 | movement of water through a selectively permeable selective to water. Alright, so |
|
| 33:25 | you can see this light purples. we decided was lilac. Yeah. |
|
| 33:33 | right. It's too early for It's blue. Okay. I |
|
| 33:40 | we can we can sit here for . I know it's like I don't |
|
| 33:44 | . All right, but that's supposed represent your water. If you look |
|
| 33:48 | the red dots represent your salutes. ? So, you already know by |
|
| 33:52 | looking at this. I can see a lot more water over here then |
|
| 33:55 | over there. So what do I to do is I need to move |
|
| 33:58 | in that direction. Now, if membrane was permissible to both the salute |
|
| 34:04 | the water, the water would move way, the salute would move the |
|
| 34:06 | direction. And you'd see equilibrium in cases. But this particular membrane is |
|
| 34:14 | to that salute. So water is to move to where there is less |
|
| 34:18 | so that it can reach equilibrium for . And that's why you get these |
|
| 34:21 | pictures right? Which is what your says. That doesn't make sense to |
|
| 34:26 | because it shouldn't climb that direction. , the way that water moves is |
|
| 34:31 | it can move through a membrane like plasma membrane. It's it's permissible to |
|
| 34:35 | membrane but it also has in that channels which we call aqua por ins |
|
| 34:42 | a fancy word water pours. So can move through the channels or it |
|
| 34:49 | go in between the fossil lipids because itsy bitsy and it breaks all the |
|
| 34:53 | that you try to learn as you're to learn about plaza membranes. |
|
| 34:58 | So that's what I was. Most . It's simply moving water down its |
|
| 35:03 | gradient. Now, the example I to use and we're gonna use hydrostatic |
|
| 35:09 | . We're gonna get to these two things. Alright. Hydrostatic pressure is |
|
| 35:12 | the pressure that a fluid exerts on things that are are pressed up against |
|
| 35:19 | . So we have water bottle, bottle, we have a Starbucks. |
|
| 35:23 | can see that there's fluid inside those where if you were to punch a |
|
| 35:27 | in the side of your little what would happen to the fluid inside |
|
| 35:32 | would try to go out. And because there's hydrostatic pressure, gravity has |
|
| 35:35 | effect on that. The water has itself and it's trying to escape so |
|
| 35:39 | it can be one molecule. Alright here, One molecule thick on the |
|
| 35:43 | , right? It's just trying to out as thin as it can |
|
| 35:46 | All right. But the force of containers are strong enough to overcome the |
|
| 35:52 | inside. But you can imagine if applied more and more fluid inside that |
|
| 35:56 | could get the bottle to burst. ? That would be the hydrostatic |
|
| 36:00 | So when you hear hydrostatic pressure, water. So hydrostatic pressure is simply |
|
| 36:05 | pressure inside of a fluid trying to that fluid to escape whatever containers it's |
|
| 36:13 | osmotic pressure is the opposing pressure. its a hydrostatic pressure, right? |
|
| 36:19 | a pressure that's outside that tries to osmosis. Alright, you guys know |
|
| 36:25 | a smart car is. Alright, many people can you fit in a |
|
| 36:29 | car? You're not trying. I ask. How many comfortably can you |
|
| 36:35 | in a smart car? How many ? How many people can you fit |
|
| 36:38 | a smart car? Let's say you one that's about right now. |
|
| 36:44 | so your college students, you got to go. You're all going out |
|
| 36:50 | right? Because no one studies at anymore. All right. And you |
|
| 36:53 | a smart card. You got eight that you want to go. So |
|
| 36:55 | take two people you put them in want to drive and you just start |
|
| 36:58 | people in there like cordwood. You're going one die and you're just |
|
| 37:02 | to push them in around person. six, you're gonna start feeling the |
|
| 37:07 | of that space is a little bit . And now the pressure inside is |
|
| 37:10 | much higher than it was when you one or two people in it. |
|
| 37:15 | you get person number seven, you pushing them in and that pressure is |
|
| 37:19 | to oppose that person coming in At # eight, you're gonna get that |
|
| 37:24 | pushed in and someone's gonna pop out other side, right? Because there's |
|
| 37:31 | so much space inside, that's like pressure. Every time a molecule moves |
|
| 37:38 | this side to that side, you've the hydrostatic pressure in this space, |
|
| 37:43 | ? That means the pressure over here drive a molecule in this direction has |
|
| 37:47 | be greater than the pressure on this . Every time I add another |
|
| 37:51 | you know, we're gonna keep but I'm increasing the pressure here and |
|
| 37:55 | , what's gonna happen, Let's say done it over time, eventually there's |
|
| 37:58 | be a molecule that goes in. then the pressure here says, |
|
| 38:01 | don't want you and it's gonna kick molecule out the other direction. And |
|
| 38:05 | the movement of water in this direction equal to the movement of water in |
|
| 38:09 | direction. Right, we reach a of equilibrium. Now you look at |
|
| 38:14 | again, your brain is looking at going, wait a second, this |
|
| 38:16 | taller than that one. Don't look that. Think in terms of number |
|
| 38:20 | molecules that you can't see here. ? And so the hydrostatic pressure that |
|
| 38:26 | the flow, or the movement of down that concentration gradient when that pressure |
|
| 38:33 | so high that it proposes it. found the osmotic pressure. Does that |
|
| 38:39 | of makes sense? I got one nodding the rest of your staring at |
|
| 38:43 | like I'm crazy. This is why like using that smart card example. |
|
| 38:52 | . Oh, can we osmosis the content is getting equal to? I |
|
| 39:02 | not. Alright, So the question , can we say that with osmotic |
|
| 39:06 | ? That's the water is getting the as the solute. It's not the |
|
| 39:11 | . It's it's literally you may not Water equilibrium. So here's 72, |
|
| 39:17 | ? You may not be able to that. Where what would be the |
|
| 39:21 | between 70 and 30 would be Right? It may be that the |
|
| 39:25 | on this side Only allows you to to 40% water on that side. |
|
| 39:30 | . So the pressure is what becomes at this point. All right. |
|
| 39:34 | not about the equilibrium of the number molecules. It's the pressure. All |
|
| 39:40 | . Yeah, that's a fair question again, your brain wants to |
|
| 39:43 | I like I like things nice and and equal and I want things to |
|
| 39:47 | pretty. I mean, right, it's not going to be that. |
|
| 39:52 | all you have to do is just about osmotic pressure is simply the resistant |
|
| 39:58 | that prevents water from moving into that . It's a hydrostatic pressure. So |
|
| 40:10 | probably asking, who cares? Why I need to know this stuff? |
|
| 40:13 | I'm now talking to the nurses the nurses in the room. All |
|
| 40:18 | patient comes and sees you or You particularly, you're just assigned to |
|
| 40:23 | , Right? And they're dehydrated and know, okay, well if this |
|
| 40:28 | is dehydrated, I need to give water, right? Because that's what |
|
| 40:35 | been taught. But we've already learned diffusion and we basically don't understand and |
|
| 40:40 | not gonna explain some principles of physiology you become dehydrated, the environment inside |
|
| 40:45 | cells try to match the environment outside cells. All right. So if |
|
| 40:50 | just understand that, just kind of your head like, okay, |
|
| 40:53 | If I give somebody pure water then I've done is now I've created an |
|
| 40:58 | gradient that favors water rushing into the so that the cells expand very very |
|
| 41:05 | and then what happens pop Because you've this at some point. Right? |
|
| 41:11 | way back in like 8th grade, learned about the blood cells. You |
|
| 41:14 | blood and water and they pop and you put salt, they shrink and |
|
| 41:19 | like that. Did you guys learn ? That's tennis city? And you |
|
| 41:23 | these terms hyper tonic isotonic and HIPPA . And again it's just prefix and |
|
| 41:29 | . That portion refers to the presence solute. Thank you again for screwing |
|
| 41:34 | up and make me learn one more . Right, tonic instead of dealing |
|
| 41:37 | the water. So when I look a solution, I'm asking, |
|
| 41:40 | it's water plus stuff. If I a hyper tonic solution, that means |
|
| 41:44 | stuff in the water is more than normally is. If I have an |
|
| 41:49 | solution, the stuff in the water what it should normally be. And |
|
| 41:55 | a hip a tonic solution is where stuff in the water is a lot |
|
| 41:58 | than it should be. Alright. used to just thinking in terms of |
|
| 42:02 | water back and forth, cause that's easy thing to do here. But |
|
| 42:06 | body, you know, if you your body, it has a certain |
|
| 42:11 | to it. And so what we'd is the number of salutes in your |
|
| 42:15 | is a specific value. So if take a solution that's isotonic, what |
|
| 42:20 | doing is we're not adding an extra or extra water in terms of |
|
| 42:26 | What we're doing is we're just adding more stuff and so we're increasing the |
|
| 42:29 | in your body. If I want move and oppose dehydration. For |
|
| 42:36 | what I wanna do is I want add in something that's not isotonic because |
|
| 42:40 | doesn't make you dehydrate less dehydrated. I wanna do is I want to |
|
| 42:43 | something that has more water but I want it to be just pure water |
|
| 42:48 | if I push in pure water water gonna rush into the cells and cause |
|
| 42:53 | to bust. So I'm going to something that's hip a tonic. In |
|
| 42:58 | words there's gonna be salute. But I'm doing is I'm slowing down. |
|
| 43:01 | other words, I don't have this slope. I'm making the slope a |
|
| 43:06 | less. All right. So if in nursing, you're not going to |
|
| 43:12 | about osmolarity. You're gonna be talking tennis. Itty. Alright. So |
|
| 43:18 | terms become important. Hyper tonic hyper tonic salute has more stuff. If |
|
| 43:25 | have more stuff that means you have water. All right. And it's |
|
| 43:31 | to a solution. So when you that solution in that means you have |
|
| 43:37 | penetrating salutes. Alright, that's hypersonic here's hyper higher penetrating salutes and less |
|
| 43:48 | isotonic. Anyone here ever used Visine is stuff your eyes when your eyes |
|
| 43:55 | all red and itchy. Yeah. , It's an isotonic solution. It's |
|
| 44:00 | saline solution or 0.9% saline solution. me when I dripped that stuff in |
|
| 44:07 | eyes, it has the same salutes terms of conservation. Not the same |
|
| 44:12 | salutes. The same concentration of salutes my tears have. And so it |
|
| 44:18 | in and goes refreshing. All Doesn't suck the water out of my |
|
| 44:24 | and it doesn't make water just drip over my face. That's isotonic same |
|
| 44:31 | equal non penetrating salutes or equal And lastly is the hip a tonic |
|
| 44:38 | low salutes high water. So when look at those words, think salute |
|
| 44:45 | then you have to do the conversion your brain for the water park. |
|
| 44:58 | we mentioned facilitated diffusion already. And I know I don't pause. |
|
| 45:04 | sir. Go ahead. This is you make me pause. Yeah. |
|
| 45:07 | gonna have to speak up really loud you. Mhm. I can sorry |
|
| 45:23 | speaking loudly. But the problem is there's a lot of space between you |
|
| 45:26 | there's lots of noise so with the it actually reflects back at you. |
|
| 45:29 | go ahead. Try one more Uh huh. If cells perform many |
|
| 45:38 | . So you got to think of like this in terms of why we |
|
| 45:42 | so many different cells is because each cell can only do a very very |
|
| 45:47 | part of the job if you want build. I'm just gonna use something |
|
| 45:51 | stupid example. If you want to a tower right? With legos, |
|
| 45:56 | could use to legos to do And then in your brain you'd say |
|
| 45:59 | a tower. But I would look and say that's just two bricks stuck |
|
| 46:03 | . If I want a tower I to use lots and lots of because |
|
| 46:06 | representation of a single brick doesn't really you that that full functionality of say |
|
| 46:14 | that what that brick brick represents. a terrible example. See this is |
|
| 46:18 | it's terrible for me to come up stuff on the fly. So let |
|
| 46:23 | be clear in terms of what you're . Are you asking why do we |
|
| 46:25 | so many cells in our body or there's so many different types of |
|
| 46:37 | Right. Yes. So why? ? Your question is why do if |
|
| 46:42 | have so many different functions? Why I have so many of the same |
|
| 46:46 | of sales doing the same thing? the amount of work that needs to |
|
| 46:50 | done, for example, can be by a single cell small cells. |
|
| 46:55 | , you're you're you're asking me to through a lot of things here regarding |
|
| 46:58 | here. Cell theory cells are very functional. The smaller they |
|
| 47:03 | And as they grow bigger in they become less and less efficient in |
|
| 47:06 | type of work that they do. that's why it becomes important to divide |
|
| 47:10 | . So, that's why you don't a lot of very large single cell |
|
| 47:13 | because at a certain point, they less efficient as they grow in |
|
| 47:18 | Alright. And you probably realize this the things that you do organizations become |
|
| 47:23 | efficient as they become bigger and bigger bigger. Right? It's a natural |
|
| 47:27 | . It actually occurs not just in , but in a whole bunch of |
|
| 47:31 | by a bunch of other areas. right. The second thing is in |
|
| 47:36 | of the actual things that they So if you look at, for |
|
| 47:39 | , a small, a small that's just a couple of different |
|
| 47:43 | It does it can do a couple things. But each of the sum |
|
| 47:46 | the parts of that that they do to grow in order to accommodate all |
|
| 47:50 | specialties that each of the individual cells . So for example, if you |
|
| 47:54 | a cell, I'm just making up that's responsible for producing glucose, it |
|
| 47:59 | to make enough glucose for all the to be functional. And then that |
|
| 48:03 | the things that it doesn't do, cells have to take over that |
|
| 48:07 | And so you're gonna have to as increase the number of things that are |
|
| 48:10 | different things. That means you have get more and more of those cells |
|
| 48:13 | do that type of job. So say now you have that one cell |
|
| 48:19 | make enough glucose for five cells. have to get a second cell to |
|
| 48:22 | enough glucose for the five cells. now you have to have another group |
|
| 48:25 | cells that make enough for to accommodate those cells that are making the |
|
| 48:31 | That kind of makes sense. Like increasing the workers to better |
|
| 48:40 | And so again, you can apply , you can kind of look at |
|
| 48:43 | how, you know, like a works or how um, you |
|
| 48:47 | organization works. It's like, you , I go and get a helper |
|
| 48:51 | help me do the job. They doing the job. And now it |
|
| 48:54 | me up to do something else. now there's not enough people to do |
|
| 48:57 | job that's going on over here. , I gotta hire somebody else. |
|
| 49:00 | so you can start seeing where the multiplication effect is. You become more |
|
| 49:06 | and better at doing something and you actually increase the efficiency of the one |
|
| 49:09 | . But you have to have more more support for those other cells that |
|
| 49:13 | doing that. That kind of answer question. All right. And that's |
|
| 49:19 | to get me off topic too. all right. I'll talk about anything |
|
| 49:24 | about forever. And I know you are dying to get out of |
|
| 49:28 | I do have an end point here I want to get to you before |
|
| 49:30 | stop. Alright. So, we about facilitated fusion and really what we're |
|
| 49:36 | about when we're doing that is we're about proteins that are found in the |
|
| 49:40 | membrane. Remember we said the plasma is lipids and proteins. And |
|
| 49:43 | the proteins, some of the proteins the membrane are transport proteins. They |
|
| 49:48 | molecules to pass back and forth. right. These transport proteins have both |
|
| 49:54 | open and closed figuration, just like doorway does. So, right |
|
| 49:57 | those doorways in a closed configuration. can't go through the door unless you |
|
| 50:02 | it. Thank you. All So, that's kind of how channel |
|
| 50:07 | work. Alright. It's going to how much you can transport. And |
|
| 50:11 | you're gonna do is with regard to channel protein when you open that door |
|
| 50:14 | gate. That's gonna allow for salutes move across that membrane down. Its |
|
| 50:21 | gradient carriers are a little bit As we said, they imply that |
|
| 50:26 | is something being moved directly or bound that protein. And so they're open |
|
| 50:33 | to one side. So, when bind it, that causes a change |
|
| 50:36 | the shape of the molecule so that switches over. Right? There's a |
|
| 50:40 | immediate uh an intermediate state where neither is open and then it opens up |
|
| 50:44 | the side and it releases that material on the other side. And then |
|
| 50:48 | we're using energy, we're moving things the concentration gradient. When we're not |
|
| 50:52 | energy, you're moving with the concentration . Now focusing on the channels for |
|
| 50:58 | moment, what we're looking at here that there are different types of channels |
|
| 51:03 | can be opened by different types of lack of a better term. Right |
|
| 51:08 | , they're called gated channels and I know why they said gated channels versus |
|
| 51:13 | doors or whatever. I mean, just language but you can think of |
|
| 51:17 | in terms of a door. So we have some doors that require |
|
| 51:22 | . Like a physical key. We other doors that can have like a |
|
| 51:26 | , right? We have other doors have that little like at the bathroom |
|
| 51:30 | you wash your hands and you don't to touch horrible things, you've got |
|
| 51:33 | little foot thing that you can pull door open with. You have doors |
|
| 51:36 | handles. You got different types of have different ways of opening them. |
|
| 51:40 | all agree with you on that. . And so that's kind of what |
|
| 51:42 | channels are. Is there are different of opening different types of channels. |
|
| 51:47 | it's only this one mechanism. We to these mechanisms as modalities. |
|
| 51:51 | So, for example, the easy to think about is ligand gated ligand |
|
| 51:56 | a molecule that binds another molecule. ? So, if you say ligand |
|
| 52:00 | channel, it's a molecule that binds channel and serves as a physical key |
|
| 52:04 | open the channel. That's an easy . And so when we can all |
|
| 52:09 | but we have some other ones. , for example, you can have |
|
| 52:12 | thermally gated channel which is not shown here when the temperature changes, that |
|
| 52:16 | the molecule change shape, which causes gate to open a mechanically gated |
|
| 52:21 | There's manipulations of the plasma membrane. the plasma membrane gets manipulated, causes |
|
| 52:26 | channel to be manipulated, it causes to open up another one. And |
|
| 52:31 | is what we're going to spend quite bit of time with is the voltage |
|
| 52:34 | channel. Alright. And we spend lot of time with it because that's |
|
| 52:37 | nervous system and muscles voltage gated channels charges associated with them. And so |
|
| 52:43 | the charges around that channel change, causes that channel to open or |
|
| 52:51 | All right. So that's the voltage channel. And so the term we |
|
| 52:54 | when when the the charges change. called the membrane potential. And we're |
|
| 52:59 | get to that a little bit So, when you see that word |
|
| 53:01 | freak out, it's just potential refers potential energy which refers to the presence |
|
| 53:05 | ions. So there's these different types channels that have different types of mechanisms |
|
| 53:11 | open and close them. And when open and close the channel, you |
|
| 53:15 | or decrease the permeability of the So, if I have a closed |
|
| 53:20 | , that membrane is impermeable to whatever substance is that that channel allows to |
|
| 53:25 | through. But when I open it your membrane is permeable to. |
|
| 53:27 | Does that kind of makes sense? . Primary active transport is that type |
|
| 53:34 | carrier where we're moving to things against soil. You're using energy. |
|
| 53:42 | In this case, what we're gonna . We're using the example of the |
|
| 53:46 | common type of pump that we find the body, which is the type |
|
| 53:50 | primary active transport, the sodium 80 pes pump. sodium potassium are |
|
| 53:56 | moved. And it's using energy as pump to drive this this thing. |
|
| 54:02 | a real simple mechanism. And what gonna do is it's gonna change. |
|
| 54:06 | how he said the extra and intracellular are different. It's this pump that's |
|
| 54:10 | for it. You see what happens you can imagine imagine an environment where |
|
| 54:14 | the exercise and the intracellular fluids are same. And I have this |
|
| 54:19 | I have this pump. What I'm do is I'm gonna pump sodium out |
|
| 54:23 | the cell and I'm gonna exchange it potassium from the outside of the |
|
| 54:27 | So what I'm doing is I'm pumping into the cell, pumping sodium outside |
|
| 54:32 | cell. I'm doing this at the of 180 p. And that's kind |
|
| 54:36 | what's going on here saying, look , this is the inside of the |
|
| 54:39 | . I'm taking sodium naturally wants to to it. It doesn't want to |
|
| 54:43 | out of the cell. It just to bind to this. And when |
|
| 54:45 | binds, that creates an attraction for T. P. To bind to |
|
| 54:50 | . When the ATP binds and these molecules bind, it releases the energy |
|
| 54:54 | changes the shape of the carrier when get to the other side, you |
|
| 54:59 | longer have binding sites. Alright, binding sites basically no longer like binding |
|
| 55:04 | to sodium. And so they do you gotta go out and it's like |
|
| 55:07 | right, well, I have no . And then it just follows the |
|
| 55:10 | of diffusion. Just kind of moves from where it was bound up. |
|
| 55:13 | , there's more sodium out here And so it doesn't want to go |
|
| 55:16 | direction, but it has no Right? It's like that's the way |
|
| 55:19 | gotta go. Just go And so what it does at the same |
|
| 55:24 | What you do is you create potassium sites, potassium look binding sites and |
|
| 55:28 | goes and binds to it. And when the to bind the two potassium |
|
| 55:33 | , the sodium are gone, then changes shape and goes back to the |
|
| 55:36 | original shape and then to potassium are and so, what you've done now |
|
| 55:42 | you've moved ions against the gradient and created to environments where you now have |
|
| 55:49 | of sodium, sodium wants to come in the cell, but there's no |
|
| 55:52 | for it to do. So, got lots of potassium inside the cell |
|
| 55:55 | it wants to go out, but has no mechanism to do. |
|
| 55:58 | you now have stored up potential energy it's this potential energy that this mechanism |
|
| 56:03 | us to have or that that that this mechanism creates that we can then |
|
| 56:10 | to do some really, really cool in cells. All right. |
|
| 56:15 | it basically is acting like a The cell acts like a battery in |
|
| 56:18 | way by storing up energy. pumps don't just exist exist like |
|
| 56:24 | I mean, this is the primary , but there's lots of them we |
|
| 56:28 | like proton pumps. And so here , you're going to use a |
|
| 56:31 | P. Right? I have lots protons down here and I don't want |
|
| 56:36 | here, I want them out Right, you can think of this |
|
| 56:38 | like the license zone. This is inside of the cell over here, |
|
| 56:41 | inside the life zone. So what wanna do, I wanna put a |
|
| 56:44 | of protons inside the license zone. what I'll do is just keep pumping |
|
| 56:48 | a TP to pump protons into the zone. And I created a little |
|
| 56:53 | vesicles full of protons, very very . So pumps are a common mechanism |
|
| 56:59 | move molecules against their gradients at the of energy. Here's that example of |
|
| 57:07 | active transport. Alright, so over this side is my sodium 80 pes |
|
| 57:15 | . Alright, so what do we ? We pump sodium out there, |
|
| 57:18 | put potassium in here, we're doing at the cost of 1 80 |
|
| 57:23 | So I've got lots of sodium in and it wants to come back inside |
|
| 57:25 | cell but it didn't have a mechanism do so so it's hanging outside the |
|
| 57:29 | going, how do I get back the bar? And then glucose comes |
|
| 57:33 | saying you know what I really want go in there but I can't there's |
|
| 57:36 | much glucose. So um hey why we make a deal? I'll go |
|
| 57:43 | and I'll bring you along and then way we can both go in |
|
| 57:47 | you can go where you want to and I can go where I want |
|
| 57:50 | go. But even though I'm not and you're not allowed, this mechanism |
|
| 57:54 | me. So sodium binds glucose binds both of them bind. We use |
|
| 58:00 | energy that that power to move glucose the cell. Alright, you're |
|
| 58:05 | So what? Yeah, that's the of unit porter. Yeah. And |
|
| 58:11 | gonna look at it on the next slides. The two slides of |
|
| 58:14 | We don't need to memorize. All . What? This is showing you |
|
| 58:20 | is how we move things without actually energy. Alright. Energy is something |
|
| 58:27 | we cherish as a cell, so don't want to waste it. And |
|
| 58:31 | represents energy stored, right? I if I break down glucose do I |
|
| 58:36 | energy out of it? The answer yes. Right? Remember if I |
|
| 58:39 | just glide colleges, I get 4 P. And then if I go |
|
| 58:42 | the whole process through all the different , I get 34 to 38 80 |
|
| 58:47 | . So, I don't want to energy to move energy. You |
|
| 58:51 | That's that's wasteful. Right? this is a mechanism for me to |
|
| 58:57 | energy without having to spend it. ? I moved three and sodium is |
|
| 59:04 | there at the cost of 1 80 . And I can move a whole |
|
| 59:08 | of things. This isn't the only of sim porter that exists, |
|
| 59:13 | This isn't the only type of secondary transport. If things move in the |
|
| 59:17 | direction, That's a sim porter when move in the opposite direction. So |
|
| 59:22 | is going out, potassium is going . That's anti porter. It doesn't |
|
| 59:26 | if it's active or or secondary Just describes the direction molecules are |
|
| 59:33 | Now, I'm just gonna show you slides and then you guys can go |
|
| 59:36 | a break real quick. All And I show you these slides. |
|
| 59:41 | do not memorize these things. But I want to show this to |
|
| 59:45 | because if you understand the generic right? I understand what primary |
|
| 59:53 | I understand it was secondary active. understand what a sim porter is or |
|
| 59:57 | anti porter or unit ports or multi , what those are descriptive. And |
|
| 60:03 | body uses these types of mechanisms over over and over again for very specific |
|
| 60:12 | in very specific or unique ways. ? So, the artist here is |
|
| 60:17 | to show you, you know, what a pump looks like, |
|
| 60:19 | So here's your sodium potassium pump. look, we have calcium hydrogen |
|
| 60:25 | We have a calcium pump here. , this is called circa You don't |
|
| 60:29 | to know that. Right? And we have is we have these multiple |
|
| 60:35 | that are conserved. There's that hydrogen . And so once you learn how |
|
| 60:39 | pump works. Once you know how works every time you see it. |
|
| 60:43 | kinda makes sense. Similarly, I the wrong direction. Similar. Here's |
|
| 60:48 | channel. Look at all these There's your potassium channel, there's a |
|
| 60:51 | channel voltage gated channel, there's a gated calcium channel. Over on this |
|
| 60:55 | channel channel, here's a channel, a channel everywhere. The channel |
|
| 60:59 | Right? Once you learn how to works, you always know how it |
|
| 61:03 | . Now. You're just looking at . Oh this is the calcium |
|
| 61:06 | Oh this is the potassium channel. just to let you know there are |
|
| 61:11 | plus sodium channels in the body. , goody, good news. You |
|
| 61:17 | have to know. Right then you like transporters. Right? So here |
|
| 61:23 | have sodium moving saying amino acid sodium glucose. So they're calling it a |
|
| 61:28 | . Co transporter. So, if understood this, you already understand co |
|
| 61:36 | . Alright. I have one thing wants to go in. One |
|
| 61:39 | The other thing wants to go and moving with its concentration, ones moving |
|
| 61:42 | its concentration and so that's how we those across. And so we'll see |
|
| 61:47 | over and over again. There's one an anti support system but it's called |
|
| 61:51 | exchanger. It's a co transport Anti report. All right, Look |
|
| 61:58 | this one is a fun one. called N. K C. |
|
| 62:02 | But again, not having to know you can look at and say, |
|
| 62:05 | look, I'm moving a sodium and into chlorine and it's using the exact |
|
| 62:09 | mechanisms. It's moving one thing against gradient and a couple of things with |
|
| 62:15 | gradient it's able to do that because understand or you're able to understand because |
|
| 62:21 | that. Here's an exchanger, other . All sorts of different. Here's |
|
| 62:26 | co transporter, both things being pumped . And this is the stuff that |
|
| 62:33 | going to see over and over again the body and allows the cells to |
|
| 62:36 | the unique things that they do. we're gonna stop here for a |
|
| 62:43 | I spent a lot of time talking stuff like that Saturate for a |
|
| 62:47 | Why don't you guys go to the , get back here by 10, |
|
| 62:51 | and let's see what we can finish . Mm. Alright, So what |
|
| 63:02 | gonna do is we're gonna just continue with this movement of materials. Some |
|
| 63:08 | in the body are too big for are too big for carriers. |
|
| 63:13 | when we're talking about carriers and we're really talking about very very small |
|
| 63:16 | . All right. But if you're about, for example, hormone or |
|
| 63:21 | sort of cida kind if you've never the word side of kind of type |
|
| 63:25 | signaling molecule, big things can't be back and forth through channels. You |
|
| 63:30 | something bigger to do that. And where these vesicles come in. So |
|
| 63:34 | you think about the inner membrane remember we talked about that we went |
|
| 63:37 | nucleus to E r er to golgi to um vesicles vesicles to to something |
|
| 63:45 | we refer to the plasma membrane vesicles one of the ways that we move |
|
| 63:50 | out of the cell. It's also way that we bring things into |
|
| 63:54 | And so when we talk about vesicular there's some terminology that we use. |
|
| 63:58 | when we are secreted something or removing we call that exocet. Oh sis |
|
| 64:04 | right. And so this will be example. Here's our vest ical you |
|
| 64:07 | see we've got some sort of particles it that we want to secrete from |
|
| 64:10 | cell. And so it merges with plasma membrane through those snares that we |
|
| 64:14 | about. And then what you're gonna is you're going to release that material |
|
| 64:19 | you get that material merged or that membrane and that vesicles merge together. |
|
| 64:24 | right now this does require energy. anyone watch the little video with the |
|
| 64:29 | the um the google Yeah. For . The google video. Youtube. |
|
| 64:36 | . Um And you saw like they you exocet, oh sis they showed |
|
| 64:41 | the transport of vesicles. Um And can imagine each and every one of |
|
| 64:47 | things, those movements of steps that with the membrane. Each cost |
|
| 64:51 | And that's when we say a teepee energy is required for this endo psychosis |
|
| 64:58 | just the reverse. And of course no picture for me to show |
|
| 65:01 | But the idea here is that you're to have some that's still exocet Oh |
|
| 65:06 | sorry, come on. There we . There's an acidosis acidosis is just |
|
| 65:13 | opposite. The idea is that you the membrane and there's something that allows |
|
| 65:18 | to either bind to or selectively collect even non selectively collect materials from the |
|
| 65:25 | cellular fluid. Now there's lots of types of endo psychosis. And depending |
|
| 65:29 | which type of book you look they have define things differently. And |
|
| 65:33 | what I've tried to do here is these broad categories or use these broad |
|
| 65:37 | . The first one is Figo psychosis we we kind of looked at that |
|
| 65:40 | we're looking at the license zone because picture showed a macrophage. And what's |
|
| 65:44 | about Figo psychosis is that psychosis requires plasma membrane to be extended away from |
|
| 65:51 | cell and is around the thing that actually trying to consume, right and |
|
| 65:55 | I'm using that language of eating Because so what you're doing is you're |
|
| 66:00 | you're like, oh here's the I'm like okay, here it |
|
| 66:02 | And what I'm gonna do is I it and then I extend my plasma |
|
| 66:07 | and it wraps around it and it the thing I'm trying to eat inside |
|
| 66:12 | vesicles and then that vehicle can be with the license. So typically this |
|
| 66:17 | gonna be very large material, you , relative to the cells. So |
|
| 66:21 | can be parts of cells. I like lots of pieces in the whole |
|
| 66:25 | , that sort of thing very early they recognized and I say they being |
|
| 66:31 | recognize another mechanism of indiscriminate absorption and what it is. Is that the |
|
| 66:37 | membrane in dense itself. So instead reaching out what it does is it |
|
| 66:41 | or imagine eights and then closes in creates a vesicles kind of like this |
|
| 66:46 | kind of pulls down and then and whatever happened to be trapped in there |
|
| 66:50 | now going to be used by the and that's kind of it's indiscriminate. |
|
| 66:54 | nothing that it's looking for specifically. just kind of grabbing in whatever is |
|
| 66:58 | the exercise of fluid trapping it and using whatever whatever it captured. So |
|
| 67:04 | had cell eating. So we're just call that one cell drinking. That's |
|
| 67:07 | the name came from pinot psychosis. right. But there's another kind of |
|
| 67:13 | there's actually a couple more which we're going to go into. But another |
|
| 67:17 | words now, it's more specific and what you have is in your uh |
|
| 67:22 | your member you're gonna have a series receptors right? They're gonna be sitting |
|
| 67:25 | on the surface and when they get they're being bound by something specific. |
|
| 67:30 | that receptor recognizes only one kind of . And when you bind those those |
|
| 67:35 | those receptors congregate to a region that protein associated with it's usually called a |
|
| 67:42 | coated pit and I don't know if I don't have it labeled there so |
|
| 67:45 | molecule is clattering and so when enough these receptors that have been bound by |
|
| 67:50 | remember we said what ligand is it's non specific term meaning a molecule that |
|
| 67:55 | another one. So when you have ligand bound up to receptor and they've |
|
| 68:00 | with these clattering in this specific area the whole thing pinches off and you've |
|
| 68:06 | captured up whatever it was specifically that looking for. Alright so whenever you |
|
| 68:11 | receptor think specific I'm looking for something and what's interesting is once it pinches |
|
| 68:19 | then what you can do is you actually recycle the receptors, send them |
|
| 68:22 | up through the process of exito sis out the things that you bound up |
|
| 68:26 | then you know do whatever it is you're going to do to it. |
|
| 68:31 | what we have here is we have couple of different mechanisms in which ways |
|
| 68:34 | ways in which materials are moved inside outside the cell. You can kind |
|
| 68:39 | see how this kind of went with last stuff but we kind of just |
|
| 68:42 | of set it off to the side we have diffusion right? We have |
|
| 68:47 | of transport through channels and carriers and carriers can be pumps right we can |
|
| 68:53 | things with their concentration gradient or against concentration gradient depending on the availability of |
|
| 69:00 | and then we can move big things well as small things. And so |
|
| 69:04 | these different types of mechanisms that allow cells to move things back and forth |
|
| 69:09 | and out of the cell. Now really easy to think about cells just |
|
| 69:14 | of sitting around and doing nothing and working independently and just kind of doing |
|
| 69:17 | thing. But the truth is the are very very talkative, They are |
|
| 69:23 | upon each other to know when and to do things. And so what |
|
| 69:27 | have is we have this process called signaling. It's just a field of |
|
| 69:33 | describes or term that describes how cells to each other. Now there's how |
|
| 69:40 | talk and to whom they talk depends the cells and where they're located and |
|
| 69:45 | their targets are. But so what can say is look they're gonna be |
|
| 69:48 | if they're close to each other, fast do I need to do |
|
| 69:51 | Where's my target cell gonna be? all have big influences on how and |
|
| 69:57 | or how what mechanism gonna use to Now the most common form of |
|
| 70:04 | His chemical communication. Right? So I can do is I release a |
|
| 70:09 | through the process of excise exocet. sis and then you pick it up |
|
| 70:13 | receptor and that tells you what to . Alright. So this is by |
|
| 70:18 | the most common but some cells that connected to each other can use electrical |
|
| 70:25 | . In other words, they can ions. So when I move ions |
|
| 70:29 | and forth across the membrane, I'm the charge across that membrane which is |
|
| 70:35 | electrical change. And I can use movement of ions as a signaling mechanism |
|
| 70:41 | myself. But I can also use signaling mechanism to cells that I'm connected |
|
| 70:47 | . Alright, so chemicals the most electrical is the next most common or |
|
| 70:54 | other type I should say. And going to focus in primarily on the |
|
| 70:58 | and when we get into the nervous , we're gonna talk a lot about |
|
| 71:01 | electrical mechanism. All right. So that in mind let's take a look |
|
| 71:08 | at the different types of chemical When you go grocery shopping. Do |
|
| 71:12 | write yourself notes? Do you make a list? Okay. Not all |
|
| 71:16 | time, but sometimes. Right. . That's what autocrats signaling is. |
|
| 71:20 | basically talking to yourself. If you you study when you study, do |
|
| 71:24 | talk to yourself? You know, had a friend in high school, |
|
| 71:29 | talked to herself and she didn't know . I mean she would just talk |
|
| 71:32 | you're like yeah, so what she I mean verbal talk to herself, |
|
| 71:38 | kind of what autocad and signaling Right, basically what you do is |
|
| 71:40 | secrete uh some sort of chemical message it's capable of binding receptors on your |
|
| 71:45 | cell. And you'd say well why I ever need to do that? |
|
| 71:50 | , remember negative feedback mechanisms you may turning off a system that you're actually |
|
| 71:56 | . So you may be regulating how of this protein you're using by determining |
|
| 72:00 | much is able to bind up to receptors. That would be an example |
|
| 72:04 | where you might see it. But essence autocrat signaling is when you talk |
|
| 72:07 | yourself as a cell, Okay. all these cases that we're gonna be |
|
| 72:13 | at, you need to have the receptor for the message that you're |
|
| 72:18 | Alright, so that's just that's a rule when it comes to sales talking |
|
| 72:22 | each other. All right. Perricone is sending out a signal. |
|
| 72:30 | So here again you're releasing the signal you're talking to cells nearby. I'm |
|
| 72:37 | that word nearby. Next to nearby there's another term for next to. |
|
| 72:44 | . So what you can see again we have a bunch of nearby |
|
| 72:47 | right? And we have cells that receptors on both types but notice these |
|
| 72:54 | that are for the for this, know, just like we have over |
|
| 72:57 | these receptors recognize the signal. These do not. So this cell is |
|
| 73:04 | talking to this population of cells, have to have the right receptor for |
|
| 73:09 | signal in order for you to respond that don't have the right receptor aren't |
|
| 73:14 | and they keep doing whatever it is they're supposed to be doing all |
|
| 73:17 | So what you're doing is you're communicating to whom needs to be communicated to |
|
| 73:23 | you're dealing with cream. But the are nearby. This example right here |
|
| 73:28 | a neuron neurons release a chemical that going to then go out into a |
|
| 73:35 | space and to bind to receptors that close to or nearby that original |
|
| 73:42 | Alright. This is kind of it's synaptic signaling. Alright. And so |
|
| 73:47 | just a type of perricone signaling. type of peregrine signaling that we've that |
|
| 73:53 | kind of set apart is called These are the next two signaling. |
|
| 73:58 | it's more like this than it is this. Here, what we have |
|
| 74:03 | just a Quran signaling is I can a chemical message and it can go |
|
| 74:07 | the cell that is next to me I can be attached to that |
|
| 74:11 | So here it is two cells that next to each other. When this |
|
| 74:16 | puts this particular receptor on its it's able to connect to that receptors |
|
| 74:20 | the receptor on that cell. And this cell is telling that cell what |
|
| 74:24 | do, it's kind of like velcro have to have the right parts in |
|
| 74:28 | to interact with each other. This how immune cells talk to each |
|
| 74:32 | right? You have immune cells just through your body and they bump into |
|
| 74:36 | other all the time. But if have the right receptor and the right |
|
| 74:39 | in that come together and that tells immune cell you go and kill that |
|
| 74:44 | over there. Typically we were called type of direct contact. These these |
|
| 74:52 | of receptors are called cell adhesion molecules cams. Yeah, yeah. Process |
|
| 75:00 | to cell recognition. This type of right here which is a type of |
|
| 75:05 | a current signaling which takes advantage of junctions, which we'll talk in just |
|
| 75:08 | moment the two cells are connected to other and so their cytoplasm are open |
|
| 75:13 | each other. And so what you do is you can produce a chemical |
|
| 75:18 | that then flows into the next cell tells that cell what to do and |
|
| 75:21 | versa. This is a type of that not only uses molecule signaling molecules |
|
| 75:29 | also uses ions. And this is cells electrically communicate with each other. |
|
| 75:36 | . So I can have ions here they can move down their concentration gradient |
|
| 75:40 | I can change how much ion is one cell next to the other. |
|
| 75:45 | is your heart functions is through this of mechanism right there. Endocrine signaling |
|
| 75:54 | our long distance signaling. Alright, , when we think about hormones, |
|
| 75:59 | is what hormones do. All So, we have a chemical message |
|
| 76:03 | produced in one cell that goes into bloodstream travels through the body and arrives |
|
| 76:08 | in all sorts of different places and places you'll have cells that have no |
|
| 76:13 | . So the hormone isn't doing anything gets picked up back in the blood |
|
| 76:16 | keeps going. But in other places will arrive and there's gonna be cells |
|
| 76:20 | have the right receptors. Okay, give you a simple one. Um |
|
| 76:26 | way that when when when we're monitoring much water is in our body, |
|
| 76:31 | place that does that is in the . Alright. And what it |
|
| 76:35 | it releases a chemical that then travels a body and goes to our adrenal |
|
| 76:39 | and determines whether or not we need produce a hormone there that then acts |
|
| 76:43 | the kidney. Alright. So you see there's three different locations here and |
|
| 76:48 | we have are different hormones. One the brain to the adrenal gland, |
|
| 76:51 | from the adrenal gland of the that's quite a distance moving between those |
|
| 76:56 | points. The only cells that can are the ones with the right |
|
| 77:03 | Alright, so in all of these of chemical signaling, the chemical and |
|
| 77:07 | receptor matter if I release chemical It can only bind to receptor |
|
| 77:14 | They can't bind to receptor B. , when we do this we have |
|
| 77:19 | type of long this signaling, we these things hormones, hormones vary in |
|
| 77:23 | and type and stuff and we're gonna into that a little bit later. |
|
| 77:27 | for example you can have hormones that proteins or you can have hormones that |
|
| 77:30 | lipids and we looked at the lipids we when we threw up the |
|
| 77:34 | we had a picture of all the types of hormones that are steroids. |
|
| 77:39 | . But those aren't the only hormones exist in the body. Now, |
|
| 77:46 | we're gonna do is we're gonna dive little bit deeper into the molecular biology |
|
| 77:51 | receptor responses of this type of chemical . All right. And we're just |
|
| 77:56 | of dipping our toe in. so, this big word right |
|
| 78:00 | metabolic tropic meta bow refers to metabolic there's metabolism involved. Tropic means |
|
| 78:09 | So, I'm doing a type of through a metabolic pathway. And really |
|
| 78:14 | way this has worked. It's really basic. And this is how |
|
| 78:17 | lot of hormones work is I have receptor on the surface of the cell |
|
| 78:22 | receptor binds to some sort of signaling that's called reception. That's going to |
|
| 78:27 | the receptor that then activates a molecule activates a molecule, which activates a |
|
| 78:32 | , which might be you don't know many molecules are in this pathway. |
|
| 78:35 | matter. This is called transaction. you've done is you've turned an outside |
|
| 78:42 | into an inside signal. You've transducer message and that's where the word comes |
|
| 78:48 | , changed it from one type to other internal text or external to |
|
| 78:53 | And then, over the course of transaction you're creating some sort of molecule |
|
| 78:59 | becomes an activator or what we refer as an effect er because it causes |
|
| 79:03 | effect and it creates a cellular All right. And this is a |
|
| 79:08 | generic way to think about how chemically chemical messages work. I bind the |
|
| 79:15 | . I change the message from the of the inside and I make something |
|
| 79:19 | happen inside the cell alright? And I make something new happen inside the |
|
| 79:24 | I can either activate things. We think in terms of always activating, |
|
| 79:28 | can activate something but I can also something. Right? Like I can |
|
| 79:34 | in this room and I can turn the lights or I can come in |
|
| 79:38 | room and I can turn off the . It just depends on what the |
|
| 79:42 | is responsible for. All right. I can change the activity of the |
|
| 79:47 | or I can create new transcription factors behave like a transcription factor or activator |
|
| 79:53 | activate one. And I can change genes are being turned or being turned |
|
| 79:57 | . In either case, what I've is I've changed the activity of the |
|
| 80:00 | either what's already present or what's not and making something new appear or |
|
| 80:07 | Now this is a very common type transaction cascade. Again, it's very |
|
| 80:12 | , notice we don't have any names any molecule but you can see it |
|
| 80:15 | , here's my receptor, here's my in my ligand binds a receptor that |
|
| 80:19 | the receptor that takes one molecule and it to become phosphor elated when you |
|
| 80:25 | the word phosphor relation. What I'm is I'm giving energy to that molecule |
|
| 80:29 | do something new. I've turned it or I've turned it off. All |
|
| 80:33 | . And so now in this particular we're just saying we're activating this molecule |
|
| 80:38 | activates this molecule, which activates this so on and so on all the |
|
| 80:41 | down the line. So this is example of transaction that's occurring. |
|
| 80:47 | If you're like me when I sat your seat, you're going well, |
|
| 80:49 | seems like a waste of time and . Why would I why would I |
|
| 80:52 | a whole series of steps when I just flip the switch. All |
|
| 80:57 | Is that the question you're asking? nod your head. Yeah, of |
|
| 81:00 | . That is exactly the question I because this molecule isn't only activating that |
|
| 81:07 | , it's activating other molecules and it's other molecules off. So what you're |
|
| 81:11 | is not only are you working in pathway, but you're working in multiple |
|
| 81:15 | and at the same time this one may activate 10 of those molecules and |
|
| 81:22 | one of these molecules might activate 10 those molecules and each of these molecules |
|
| 81:26 | activate 10 of those molecules. And can see what we've done here is |
|
| 81:30 | taken one signal and I've amplified it a massive signal. So I've got |
|
| 81:35 | that's doing a lot of work for very, very small. So it's |
|
| 81:40 | amplification process as well so that ultimately cellular response is big to a |
|
| 81:46 | very small signal up there at the . Now, every time I activate |
|
| 81:55 | I have to enact or inactivate right? Because otherwise it's just gonna |
|
| 81:59 | going forever. Right? And so have mechanisms that allow us to do |
|
| 82:04 | . And these are just an example a molecular switch. Again, you |
|
| 82:08 | need to know these things right but this is just showing you here's |
|
| 82:11 | protein that's in active here. It active. So I have something that |
|
| 82:17 | it from the inactive form to the form. But then for everything that |
|
| 82:21 | it, I have to have something in activates it and this is how |
|
| 82:23 | regulate and control which systems are on off. So for example, has |
|
| 82:29 | father ever told you after you turn the light in the room as you |
|
| 82:33 | the room, turn off the damn . Did they use that word? |
|
| 82:38 | I say that a lot in my , right. I got four |
|
| 82:42 | they're constantly going into rooms. It's so bad. My wife is now |
|
| 82:46 | yelling at the kids, right? they're not young. I mean we're |
|
| 82:50 | , I got a sophomore in high , I mean he should know better |
|
| 82:52 | my daughter who was also sophomore, should know better, Right? But |
|
| 82:56 | idea is that you turn things on you're done with the process You turn |
|
| 83:01 | back off and this is how we all these processes. So, for |
|
| 83:07 | , if I keep activating this up , this thing will keep going. |
|
| 83:12 | if I only activate this once it naturally turn itself off because we have |
|
| 83:17 | like this in play that turned the back off automatically. That kinda makes |
|
| 83:27 | . So meta tropic has pathways has transaction. All right. So you |
|
| 83:33 | just think metabolic pathway. There's lots molecules involved. The other type is |
|
| 83:40 | a tropic again, tropic means to something on or off. Ion means |
|
| 83:44 | using an ion to do. So here what I'm doing is I have |
|
| 83:48 | receptor that may have a Liggan or gate or whatever it is. But |
|
| 83:52 | I'm doing is I'm opening up a and that channel allows ions to flow |
|
| 83:57 | and when ions flow that's current. when I have current I have electrical |
|
| 84:02 | , I'm changing the electrical activity of cell. All right, these types |
|
| 84:08 | responses are very quick and they're very lived. Because what I'm gonna do |
|
| 84:12 | I'm gonna open the channel and I'm close it back up when the ligand |
|
| 84:15 | opens when the ligand is let go destroyed. It closes back up. |
|
| 84:19 | I get a very very quick If you go back to a meta |
|
| 84:23 | thing, this turns on this which on this which turns on this which |
|
| 84:27 | on this which turns on this. you see how it takes a lot |
|
| 84:29 | time for it to happen? Then we have this weird one. |
|
| 84:39 | is what I was studying when I in grad school. Partly not not |
|
| 84:43 | but partly steroids and lipid signaling lipids, lipid based signaling molecules do |
|
| 84:53 | like water. And so what they're , what they've done or what they |
|
| 84:57 | to sell uses them for is they them as a mechanism to turn on |
|
| 85:02 | off genes. All right. So have receptors but the receptors I don't |
|
| 85:07 | to I mean their job is to on genes. All right. So |
|
| 85:12 | are what we call transcription factor. so when there is no steroid, |
|
| 85:17 | transcription factors or nuclear receptors hang out in the cytoplasm and the nucleus. |
|
| 85:23 | . But once they get bound up get transported into the nucleus of the |
|
| 85:28 | and they bind these regions in front the promoter. Remember what we said |
|
| 85:31 | promoters were? That's the start of gene. And that promoter when when |
|
| 85:37 | these nuclear receptors come in and bind hormone response elements. What they do |
|
| 85:42 | they turn on or they turn off expression of the gene. Alright, |
|
| 85:46 | steroids use this unique sort of mechanism change the activity of the cell at |
|
| 85:53 | gene level now, back up here a second. Everything in this pathway |
|
| 86:00 | exists. You guys see all the in the pathway. See all the |
|
| 86:03 | colors and stuff. So you can . I said this was really fast |
|
| 86:09 | it's basically ions moving back and This is slower than the ions, |
|
| 86:14 | it's fast because everything is already It's like lining up dominos. Once |
|
| 86:18 | press the first domino, all the dominoes fall when I'm dealing with nuclear |
|
| 86:25 | . What I'm doing is I'm making new proteins. The process from going |
|
| 86:29 | to a gene to making a protein time Now the example I'd like to |
|
| 86:34 | is a real simple one in this . How do I turn on and |
|
| 86:37 | ? The lights gotta switch right over . All right. So, you |
|
| 86:41 | imagine a meta tropic pathway is like . All I got to do is |
|
| 86:44 | over to press the switch and all lights go off. There's a mechanism |
|
| 86:47 | connects all the lights to the When you're dealing with nuclear receptors. |
|
| 86:52 | you're doing is saying, yeah, want to turn the lights on or |
|
| 86:55 | . But what I need to do I need to build the lights and |
|
| 86:57 | need to build the switch in order make it happen so I can make |
|
| 87:02 | happen. But it's going to take for it to happen. But once |
|
| 87:07 | done it it's gonna be around for while. That kind of makes |
|
| 87:13 | All right. So there is a in the response because what we're doing |
|
| 87:18 | we're changing gene expression. But once changed gene expression, it's gonna be |
|
| 87:23 | for a while long lived. The ones are not long lived. They're |
|
| 87:29 | very quick and they're very very short . Alright. I'm gonna pause there |
|
| 87:36 | a second. Any questions about Because I'm really kind of just dipping |
|
| 87:39 | toes into some very very complex physiological . And you're kind of sitting there |
|
| 87:45 | and going, oh crap, what I need to know about that? |
|
| 87:47 | see the look. Not my first . Are you okay with those those |
|
| 87:52 | ways of signaling mechanisms of signaling. can stare too. Those three. |
|
| 88:09 | , that's it. Okay. We're then you trust her. Okay. |
|
| 88:16 | right. Back to a little bit anatomy. Alright. Again, we're |
|
| 88:21 | dealing with the cell friday is tissue after friday is test day. That's |
|
| 88:28 | . Right? That's when you get take the test and then go to |
|
| 88:32 | . Then you get to celebrate that took the test, skip lab. |
|
| 88:36 | they get really upset about that. right. And then what we do |
|
| 88:40 | go into the organ systems. So we're gonna start here. |
|
| 88:46 | we're gonna finish up with the Alright. And really what we wanna |
|
| 88:49 | is we want to look at how are connected to each other because they |
|
| 88:52 | they don't work by themselves. And this little picture here shows you the |
|
| 88:55 | common types of junctions of the most way in which cells are attached to |
|
| 89:01 | another. The first type is the OEM. And really what the Dismas |
|
| 89:05 | is is like molecular velcro. All , you hear me use that term |
|
| 89:09 | and over again. But the idea is basically I have a bunch of |
|
| 89:13 | molecules on one cell, a bunch other adhesion molecules that recognize them on |
|
| 89:17 | cell. You have a whole bunch proteins that hold those adhesion molecules in |
|
| 89:21 | . And then what you do is gonna take a bunch of intermediate filaments |
|
| 89:23 | attach them to those adhesion molecules. then those two cells can then be |
|
| 89:28 | to each other. So that when pull on one of those intermediate |
|
| 89:33 | I'm pulling on this entire structure which is attached to the other cell which |
|
| 89:38 | on the other cell which pulls on intermediate filaments. And what I've done |
|
| 89:41 | is I've dispersed force. And so now holding cells close to each other |
|
| 89:47 | context so that when I affect oneself another, how I can ensure that |
|
| 89:53 | remain mechanically stable between each other go to the indian burn the reason your |
|
| 90:00 | doesn't go falling off your body is cells are connected by these types of |
|
| 90:06 | alright, They resist tension and they due stress or distribute stress by taking |
|
| 90:12 | force and sending it through all these into another cell which are connected to |
|
| 90:18 | cells which are connected to other And it kind of looks like |
|
| 90:21 | This is a really, really, bad drawing because cells are not connected |
|
| 90:25 | way. You can imagine cells are closer together. But this is trying |
|
| 90:28 | show you that connection between the desmond . If I pull on this cell |
|
| 90:33 | here, that forces distributed to this , which distributes the force to all |
|
| 90:37 | other cells around it. And the all move in unison and with reduced |
|
| 90:48 | . Yes, the hemi Dismas. is the half Dismas. Oh, |
|
| 90:52 | right. We're going to learn a bit later that epithelium sits primarily on |
|
| 90:58 | of connective tissue. Alright, that's of the ways that we see |
|
| 91:03 | How do those two things which are the same, stick to each other |
|
| 91:06 | they use things like hemi Dismas So, again, here's that |
|
| 91:10 | Here's those intermediate filaments. Here's those . And then you can see right |
|
| 91:14 | here, this would be connective And what these cams do is they |
|
| 91:20 | fibers in the connective tissue that they're of binding to. Again, you |
|
| 91:25 | not need to know specific names. do not memorize the specific names of |
|
| 91:30 | . But the idea here is they themselves to other molecules in the connective |
|
| 91:35 | . And this allows this epithelium to on a unique tissue and not be |
|
| 91:41 | off of it. Right? If were to create a little cut in |
|
| 91:45 | skin and try to pull and pull skin away from your connective tissue, |
|
| 91:48 | would take a lot of work You can do it. That's how |
|
| 91:51 | skin animals. And that's where you leather and all sorts of fun |
|
| 91:55 | But it's not an easy thing to . All right, So hemi |
|
| 92:00 | OEMs are half Dismas. OEMs they cells in epithelium to connective tissue. |
|
| 92:06 | what we're going to learn about the membrane when we get to the |
|
| 92:12 | Mhm. Don't memorize those or inte . When I was in college and |
|
| 92:22 | his junctions junctions apparently didn't exist. someone discovered them. And now you |
|
| 92:27 | have to memorize it when you see word adherence junctions, what do you |
|
| 92:33 | at here? So basically junction that two cells to stick together. They're |
|
| 92:38 | hemi Desmond zones. They just use proteins. All right. They don't |
|
| 92:43 | have that plaque. But again, you have is you have intermediate |
|
| 92:48 | you have uh molecules to which everything bound you take these cat these are |
|
| 92:53 | cat hearings are a type of cell molecule and they basically take them and |
|
| 92:57 | bind to cells together. And now adhered to one another. All |
|
| 93:03 | They're just structurally different. Right? he made Dismas um is sell to |
|
| 93:14 | tissue Desmond's. Oh must sell to at heron's junctions. Cell to cell |
|
| 93:20 | structurally different. And then we have tight junction which isn't or could be |
|
| 93:29 | it might not be. So you're learn about leaky tight junctions. You'll |
|
| 93:32 | about tight tight junctions and so forth . What you have to have a |
|
| 93:35 | of proteins that are kind of like bags. Right? Think about a |
|
| 93:40 | bag and sealing the little zip Right. And what you can do |
|
| 93:43 | you can imagine I can't go into bag and I can't go out of |
|
| 93:46 | bag because of that. That's basically is a series of proteins on one |
|
| 93:50 | and a series of proteins on the cell. And they basically are adjacent |
|
| 93:54 | one another and they linked to each and they create a barrier so that |
|
| 93:57 | environment on this side of the cell different than the environment on that side |
|
| 94:01 | the cell. It prevents things from in between the two cells and it |
|
| 94:05 | a unique space on either side. we talked a little bit. I |
|
| 94:10 | I said once you may not have it. I said that with epithelium |
|
| 94:13 | have polarity. Remember that when I that. And so that polarity is |
|
| 94:19 | because of this type of tight Oh I have a picture there. |
|
| 94:25 | it even easier to see. So there's the typical side, this is |
|
| 94:30 | basal lateral side over here. This they're showing you the intestine. They're |
|
| 94:35 | look there's stuff up there. Things leak in between the cells because those |
|
| 94:39 | junctions create a barrier between that environment this environment. All right. So |
|
| 94:47 | something wants to get over here, has to go through the south. |
|
| 94:51 | you don't have a tight junction then can leak through. So tight junctions |
|
| 94:57 | barriers Between walls of cells and two environments. There's just something else that |
|
| 95:05 | does and that's it's kind of unique that you see how it's kind of |
|
| 95:10 | pink in here. You see that pink that's there to show you that |
|
| 95:15 | goes all the way around the but also internal to the cell. |
|
| 95:19 | actually materials there. So, the side of the cell over here is |
|
| 95:26 | from the basal lateral side. So chemical reactions that are occurring on this |
|
| 95:30 | are different than that one because those junctions also create division within the |
|
| 95:37 | I'm not gonna ask you about It's kind of interesting when you think |
|
| 95:41 | if you have an apricot and basil how do they know which side is |
|
| 95:45 | it's because the tight junctions make it . All right. Stop multiple. |
|
| 95:57 | . Yes. So different environments will , you can have Desmond zone. |
|
| 96:02 | going into the test because this is area that I did my studies right |
|
| 96:06 | way the germ cells are made or find themselves in between epithelial cells and |
|
| 96:13 | you'll do is you can look in and you can see there are tight |
|
| 96:15 | , adhere injunctions, Dez Mazzone's hemi , OEMs attaching the epithelial cells and |
|
| 96:21 | there are junctions that actually break and . So they have all these things |
|
| 96:26 | as well as gap junctions so that can have communication with the cells that |
|
| 96:29 | next to. So it's not uncommon see multiple things. And I think |
|
| 96:34 | kind of how they discovered adherents are because eventually what we do is we |
|
| 96:38 | antibodies and stuff that we can use tag molecules and say this is what |
|
| 96:41 | is. And they were tagging So can see a Desmond zone here. |
|
| 96:45 | why is it not lighting up? that's when they realized, oh, |
|
| 96:48 | different molecules there. Here's the gap . Gap junctions allow two cells that |
|
| 96:56 | connected to each other to communicate So here this is one cell, |
|
| 97:01 | the other cell, a series of creates the gap junction. These are |
|
| 97:05 | connections, that's the group of proteins so they create a gap or poor |
|
| 97:10 | can open and close. And so allows the materials in this cell to |
|
| 97:15 | exposed to the materials in that So, if I have ions for |
|
| 97:19 | , they can be allowed to move through between the two cells. They |
|
| 97:23 | have to go out of the cell come back in a different way. |
|
| 97:26 | basically sharing cytoplasm. All right, the molecules have to be very very |
|
| 97:34 | to do. So now outside of cells we talked about there being |
|
| 97:44 | And so there's this guy coke So you can see here's our glycoprotein |
|
| 97:48 | are being shown in this picture. the truth is is that when you |
|
| 97:53 | at these cells, they're not just naked to the to the environment around |
|
| 97:59 | . There's all sorts of proteins. like we talked about there being a |
|
| 98:02 | of skeleton on the inside, there's of this network of proteins and other |
|
| 98:07 | that sit on the outside of the . Alright, even on the a |
|
| 98:10 | side. And again, if you watch that video um that I |
|
| 98:14 | you're gonna see, you're gonna see matrix because those little receptors that that |
|
| 98:19 | cell is trying to make in that video, they kind of pop up |
|
| 98:22 | you can see there's these wires and proteins that kind of you know, |
|
| 98:27 | fibers, not wires but fibers sitting above them and they kind of poke |
|
| 98:31 | of them so that they can be contact this network of proteins that's found |
|
| 98:38 | the cell is referred to as the cellular matrix. Alright, there's all |
|
| 98:43 | of stuff. There's collagen and other as well as some sugars. You |
|
| 98:48 | like this is a protein sugar, called google icon and you get things |
|
| 98:53 | glycoprotein like hands, you don't need worry about them but there's all these |
|
| 98:56 | types of molecules that sit out there these are secreted by the cell to |
|
| 99:01 | an environment that both prevent and promotes . So you have to have the |
|
| 99:08 | sort of connection to be able to cells. It also helps to have |
|
| 99:14 | environment which you can anchor cells. on the basal lateral side this extra |
|
| 99:18 | matrix is there to help create something you can grab onto. And so |
|
| 99:23 | allows for the different cells to connect each other and other and also you |
|
| 99:28 | see that there's like molecules like this allow you to signal with the |
|
| 99:33 | So you're gonna see this term come over and over again. The extra |
|
| 99:37 | matrix, extra cellular matrix. Just that the cells aren't just sitting there |
|
| 99:42 | , they actually have all sorts of sticking out from them that allows them |
|
| 99:45 | interact with their environment and that is extra cellular matrix. Okay, last |
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| 99:53 | bit here that I want to deal is cell cycle. How much do |
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| 99:59 | got here? Okay, it's just simple um This isn't like an intro |
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| 100:06 | class where you have to learn every solitary step in phase and how to |
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| 100:10 | them and stuff. I just need to understand that cells are capable of |
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| 100:14 | . And when they're doing that they're they're when they're going through replication and |
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| 100:18 | they're creating new copies new clones of . And then they can go through |
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| 100:22 | periods of not division or they can they can be my topic. In |
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| 100:27 | words they're going through division and then reach a point of maturity where they |
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| 100:31 | stop doing that. All right. so the cell cycle represents this period |
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| 100:38 | replication and so you can see it . There's two phases. We have |
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| 100:41 | period that's metabolic. So that's your period. That would be you know |
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| 100:46 | of how you're preparing for division and there's this period of division called the |
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| 100:51 | topic phase. So you've heard of , that's what that refers to. |
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| 100:55 | those steps Okay. All right. of course during the inter phase you |
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| 101:00 | basically go step out and say okay done. I'm not doing I'm not |
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| 101:03 | of the cycle anymore. I've been . And I set out off to |
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| 101:06 | side that's kind of what I have on this side is just kind of |
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| 101:09 | what are the phases metabolic phases referred as G one that's the first growth |
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| 101:15 | and every cell has a different length terms of how long it lasts. |
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| 101:19 | if you're still in the process of more cells or new cells there's a |
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| 101:23 | called the S. Phase where you copy the DNA make you you replicate |
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| 101:29 | duplicate your D. N. So that you can divide later in |
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| 101:32 | mid topic phase. That's what the . Phase here. So this is |
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| 101:36 | kind of a growth phase. I'm I'm getting ready to make new |
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| 101:39 | N. A. I. Go make my new D. N. |
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| 101:41 | . And then I go through this phase for division. Which means I |
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| 101:46 | check to make sure I've gone through checklist to make sure everything's okay right |
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| 101:51 | you go on a trip. Do go through a checklist? Did I |
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| 101:54 | the doors and I packed enough Do I take sunscreen? Do I |
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| 101:58 | my ticket? That sort of Right so that's kind of the same |
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| 102:01 | that goes on here. There's a of checklists that the cell goes through |
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| 102:05 | it says have I done everything correctly in order for me to go here |
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| 102:09 | once I enter this if anything's busted get to die. And so it |
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| 102:15 | to make sure that that doesn't All right. You also have that |
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| 102:22 | . G. Not phase. That's that zero is G. Not and |
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| 102:25 | that's the one where it just kind hangs out and says I'm done I'm |
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| 102:28 | gonna do the thing that I've been to do. All right So I |
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| 102:32 | the checkpoints. Um there's one here the G. One and then there's |
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| 102:37 | couple in the G. Two. And again just understanding that I'm I'm |
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| 102:42 | checkpoints to make sure that I'm able progress in the next phase is |
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| 102:46 | It's kind of like lack of better like graduating from high school and graduating |
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| 102:51 | college right? There's a checkpoint that have you done all the work you're |
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| 102:56 | to do? You have? Okay you go. So mitosis is the |
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| 103:03 | of the nuclear material. Psychokinesis is division of the cellular material. Okay |
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| 103:13 | there are four phases. You don't to recognize what these things that are |
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| 103:19 | in these phases. I'm not gonna you that. It's just mean alright |
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| 103:22 | just under I mean at some point life you learn it MAC pro fes |
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| 103:25 | face to face to face. Did guys learn that one point? Did |
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| 103:29 | have to look at the picture of cell and draw the little stages at |
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| 103:31 | point? Yeah. So just understand I'm doing here is I've already replicated |
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| 103:36 | D. N. A. During interphase. In pro phase. What |
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| 103:39 | doing is I'm organizing that D. . A. So that I can |
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| 103:42 | it Between the two daughter cells. right so it's the latter two phases |
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| 103:49 | that DNA is being pulled apart and ultimately being reorganized. And then psychokinesis |
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| 103:55 | simply saying look I've separated at the of the D. N. |
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| 104:00 | And now what I'm gonna do is gonna split the material of the |
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| 104:04 | So I have two identical copies of cells that are now clones of each |
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| 104:10 | we call them daughters. And then capable of doing what the parental cell |
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| 104:14 | doing. Initially we tired. I can keep going. I'm not |
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| 104:27 | . Alright so that's where we're gonna today when we come back. Unless |
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| 104:31 | really go like off the reservation it's be a pretty short lecture. I |
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| 104:37 | know if it's it's probably gonna be little bit more than ours. We |
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| 104:39 | not break. But historically going through different types of tissues is pretty |
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| 104:45 | So you guys have a great I will see that's tomorrow. |
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| 104:53 | You guys have a great day. you tomorrow. Have a wonderful |
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| 104:57 | Don't burst into flame. Bye bye |
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