| 00:01 | open. Alright, so here we , the day before the exam, |
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| 00:14 | all excited. Well I mean I'm my brain works in this class and |
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| 00:21 | class. This, you know, stuff in between. Doesn't matter. |
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| 00:24 | just like sleep, you know? , so remember we have an exam |
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| 00:29 | thursday that means we don't show up . Everything we cover today, everything |
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| 00:33 | supposed to cover today is gonna be the exam. Good news, muscles |
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| 00:37 | easy. You look at me like . All right there, easy and |
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| 00:43 | show you that they're easy. They're one time one semester my computer died |
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| 00:49 | I had to give the entire muscle off the top of my head, |
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| 00:54 | , We can draw it out and will take us 10 minutes. The |
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| 00:58 | that I spent an hour and a talking about is just me wasting |
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| 01:01 | is me using your time appropriately. . Before we get there though, |
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| 01:05 | just want to finish out with the . We were talking about different ways |
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| 01:08 | the brain is organized and the way information is sorted into the uh into |
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| 01:13 | structures of the brain. And this is more uh kind of an |
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| 01:18 | thing to let you understand that there a high degree of organization. And |
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| 01:21 | when we were talking about the I example, it maps to the retina |
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| 01:25 | what we didn't talk about is the other different layers that actually talk about |
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| 01:29 | and movement and all the other fun we kind of ignored that. We |
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| 01:33 | about how the body's map. there's , there's this amount of sensory quarter |
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| 01:37 | it maps your body to the specific of the post central gyrus and basically |
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| 01:42 | , okay if something is touching your , this is the part of the |
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| 01:45 | that's gonna be stimulated. When I something, we look at the motor |
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| 01:49 | of the brain that's actually the pre cortex and the pre motor cortex also |
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| 01:54 | in a very specific way. So can say if I want to move |
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| 01:58 | foot, I can go to this of the brain and that's the area |
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| 02:01 | that's being mapped with regard to the lobe and with sound it matches the |
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| 02:07 | of the cochlear so you've got high on one end and low notes on |
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| 02:10 | other end and those fibers are going into the temporal lobe. But what's |
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| 02:15 | about the way that we process sound also has to do with how our |
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| 02:20 | and how that sound reaches our So for example, we're probably all |
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| 02:26 | with that we hear stereoscopic lee, ? You guys just listen to one |
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| 02:32 | but when you're when you're listening no. And if you take one |
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| 02:36 | out, doesn't it sound weird. , because the way the sound engineers |
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| 02:40 | this is they're trying to make it like you're in the place where they're |
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| 02:44 | recording it, whether it be in concert hall or whether it be in |
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| 02:46 | studio and so they want to give a sense of being surrounded by the |
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| 02:50 | . So sound is coming at us all sorts of different directions. And |
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| 02:54 | way that our brain knows where it coming from is because the way that |
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| 02:58 | sound hits our ears and the last I told you on thursday I said |
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| 03:01 | at each other's ears and then many you cover up your ears really quickly |
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| 03:05 | you're like, I don't want you look at how weird my ears |
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| 03:07 | But you can see up here this what your looks like. It's |
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| 03:10 | And if you go and stay at here for long enough you're gonna |
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| 03:12 | yeah, it's really weird but it's to bounce sound in very specific ways |
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| 03:18 | that acoustic miatas are miatas so that sound hits the tim panic membrane in |
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| 03:23 | ways and in specific timing. So example, we actually detect where sound |
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| 03:30 | coming from because of two different Sound comes in the vertical plane? |
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| 03:34 | know, vertical plane is? that's up and down. So where |
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| 03:37 | we know where sound is coming from from the horizontal plane, where is |
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| 03:42 | coming from this side? Or is coming from that side? And so |
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| 03:44 | the vertical plane you only need one . Right? And so if that |
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| 03:49 | is coming from high or low it's bounce off the different parts of the |
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| 03:53 | in different ways. So that when reaches your ear you understand, oh |
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| 03:58 | it's come up high this is because bounced a certain way and if it |
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| 04:02 | low it arrives at my ear in different timing and it bounced a certain |
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| 04:06 | off those ear structures. Kind of . So that weird looking here, |
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| 04:12 | weird. Promise go look at it a bit Is allowing that to happen |
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| 04:18 | regard to the horizontal. Has to with the sound waves themselves and it |
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| 04:22 | two Ears. Okay, so here is showing you both high notes and |
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| 04:29 | notes. Alright, so high notes high frequency, right so that the |
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| 04:33 | waves are traveling very very close Low notes, you have very very |
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| 04:38 | wavelengths. So the sound waves are far apart. So when you have |
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| 04:44 | notes, what happens is when it one side. So if it's let's |
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| 04:47 | it's coming from like it's showing here the right side of your body, |
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| 04:50 | gonna hit both ears fairly close together the sound waves are just up |
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| 04:54 | up up moving very very quick. what's happening is is that it creates |
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| 04:58 | shadow and so that shadow is reflected how the left ear, if it's |
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| 05:04 | from the right hand side detects Alright, so it's not the exact |
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| 05:09 | sound that you're hearing on both sides I'm gonna show you how it does |
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| 05:12 | and then on the right side it its sweet time. So long waves |
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| 05:16 | hit one side and then the other with a delay between the two sides |
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| 05:20 | when that delay occurs, that's when knows oh it's coming from this side |
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| 05:24 | that side in this case would be right side to the left side. |
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| 05:27 | . But how this ultimately works has do with structures in the brain. |
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| 05:32 | right, So what we're looking at is the medial, superior Olivari |
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| 05:35 | If you have a superior Olivari that means you have an inferior one |
|
| 05:40 | well. And these are the these the structures of the brain stem that |
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| 05:44 | you to turn your head when you sounds, for example, when you |
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| 05:46 | the word hey and you turn you know, that's that's what the |
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| 05:50 | nucleus is responsible for. The other is responsible for site, you |
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| 05:55 | when you see something moving, you your head to watch it move. |
|
| 05:58 | . But what I want to point here is just the the amazing uh |
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| 06:04 | that we're looking at here. So structure you have, remember you have |
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| 06:08 | coakley on either side of the brain you're trying to detect which way the |
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| 06:12 | is coming from. So each of have these neurons that travel and they're |
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| 06:17 | very long, what we refer to delay lines. And so you can |
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| 06:21 | that both sides, both Olivari nuclei innovated from both sides. So you |
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| 06:26 | a long fiber going in in a fiber going in and within those we |
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| 06:30 | a coincidence detector. Now a coincidence basically just says here's a point. |
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| 06:36 | if I receive a signal from both those, both of those neurons at |
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| 06:38 | same time, then I can detect side based on that delay. Because |
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| 06:43 | already calculated when the delay occurs, know which side the sound is coming |
|
| 06:47 | . So if they don't come at same time, I'm not detecting if |
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| 06:49 | don't come at the same time and you'll find a pair of matching pair |
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| 06:54 | says oh it's coming from this side from that direction or that direction or |
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| 06:58 | direction. All right now, this where we get to geek out a |
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| 07:01 | bit here because I can ask some you guys because I know some of |
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| 07:04 | guys actually play video games, And you guys have really really nice |
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| 07:09 | , right? And they have virtual sound in them, right? To |
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| 07:14 | speakers and virtual surround sound what they're . They're taking advantage of this and |
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| 07:18 | placing the sound to to mimic that sound is moving. And it's taking |
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| 07:24 | of these coincidence detectors to give you sense of oh I'm in the midst |
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| 07:28 | whatever the game is. Now you do this with a 5.1 speaker system |
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| 07:32 | 7.1 speaker system as well, but really kind of stands out when you're |
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| 07:35 | at two little speakers sitting on your . Alright, So that's what this |
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| 07:40 | trying to show you. Here's the lines and these are the coincidence |
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| 07:47 | So where I'm actually stimulating this this one this one kind of gives |
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| 07:51 | a sense of am I where am in the horizontal plane? So that's |
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| 07:56 | your brain knows which way sound is from, even though both ears are |
|
| 08:00 | hit? Yeah, I see the coming up, hmm. How does |
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| 08:08 | inferior curricula different? So, um that's a good question. So I'm |
|
| 08:14 | screw this up. I haven't thought it today, I haven't looked it |
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| 08:16 | . But inferior and superior one deals vision, one deals with with |
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| 08:21 | And I want to say inferior has do with vision, but I know |
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| 08:24 | I say that I'm guaranteed that it's to be wrong. Oh, the |
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| 08:29 | sauce. Right? So again, remember what we're doing with each of |
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| 08:35 | things is we're pre processing information before ever actually gets to the cortex so |
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| 08:39 | you can have a not so much understanding of what it is that you're |
|
| 08:43 | , but say direction and uh I'm just gonna go direction for right |
|
| 08:50 | , if that makes sense. The of understanding what it is coming from |
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| 08:54 | where it is coming from around you really what? So it's forcing your |
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| 08:57 | to turn is really what it actually . It's like, oh, |
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| 09:01 | it's coming from this direction. I too many of you guys walking around |
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| 09:04 | headphones. So my examples are not to be really, really good |
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| 09:08 | right? So stop wearing your headphones I can have better examples, but |
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| 09:12 | when you're in the street and that honks at you or when that friend |
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| 09:16 | your name or when someone says hey everyone turns around, right? So |
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| 09:20 | idea here is my turning of my is a function of hearing that sound |
|
| 09:25 | how about the duck? Right? ever hear duck? No, no |
|
| 09:30 | . You never duck, you do , right? But then what do |
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| 09:35 | do when you duck kind of look . So that's that's the idea. |
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| 09:41 | I think superior curriculum if I remember , eyesight in various sound. So |
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| 09:47 | right, so I want to just of just give you all that stuff |
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| 09:49 | to kind of give you that little of that understanding of this pre processing |
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| 09:53 | kind of taking place before it arrives in the cortex and what I wanna |
|
| 09:57 | now is I want to just spend is all about muscle other than what |
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| 10:00 | just talked about here. So when talk about muscle and almost 90% of |
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| 10:05 | textbook, whenever they talk about they're gonna spend the majority of the |
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| 10:09 | talking about skeletal muscle. So, did I tell you when you spend |
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| 10:12 | majority talking about skeletal muscle ignoring the two types not as important or there |
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| 10:19 | similar. Alright. So using skeletal as our as our our background or |
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| 10:26 | , we're gonna look at cardiac. we're gonna look at smooth. All |
|
| 10:30 | . And so first off, when talk about a muscle, right? |
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| 10:34 | you're when you like a named muscle your body, what you're looking at |
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| 10:37 | basically a series of muscle fibers that been wrapped together in connective tissue to |
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| 10:43 | a single function. And then if look at a larger muscle or like |
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| 10:47 | like your leg where you have like muscles in their multiple name muscles. |
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| 10:53 | you're looking at is a multiple structures are wrapped together again to perform similar |
|
| 11:01 | . All right. So, you named muscles. And then you have |
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| 11:05 | of muscles. And then if you downward, you'll see that within that |
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| 11:09 | muscle, you're gonna have bundles of and within those fibers or bundles, |
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| 11:13 | see the individual fibers themselves and each these levels. You're gonna have these |
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| 11:18 | surrounding connective tissue. And so the of the connective tissue is one to |
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| 11:22 | the individual fibers so that you can each individual fiber without stimulating the other |
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| 11:27 | . It's like putting insulation around the . If you take a whole bunch |
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| 11:30 | copper wires without any installation, you a signal down one of those copper |
|
| 11:35 | . It's gonna go to all the wires. Right. That makes |
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| 11:39 | So what do I do? I them all in plastic or rubber? |
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| 11:43 | . And so then now I've So when I send a signal down |
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| 11:46 | fiber, copper fire, none of other copper fibers are gonna be |
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| 11:51 | All right. So that's that's gonna the lowest level. And then I |
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| 11:54 | up into bundles. And so bundles multiple fibers that can be stimulated as |
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| 12:00 | group. But they're being stimulated independent each other. Alright. It'd be |
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| 12:05 | me pulling on a rope and I have enough strength. So, what |
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| 12:08 | I gonna do? I'm gonna recruit friends to help me pull the |
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| 12:13 | Alright. So we're each doing it , but we're doing the same |
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| 12:16 | And then I take bundles of And what I'm doing now is I'm |
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| 12:21 | greater strength so that I can accomplish the goal is of that particular |
|
| 12:25 | Alright. And so that's what this trying to show you. Alright, |
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| 12:30 | themselves are individual cells. So, talking about muscle fibers. That's where |
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| 12:35 | going fibers. Not the fibers They're wrapped in connective tissue separating themselves |
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| 12:40 | each of the individual fibers. But group is then wrapped together as a |
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| 12:45 | . That's a fast ical. And fast calls are bundled together to create |
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| 12:49 | bellies, for example. All And so we have names for those |
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| 12:54 | levels. So the one that's around individual fiber is going to be called |
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| 12:58 | endo missy. Um Then we move the paramecium. That's the fast |
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| 13:02 | And then the surrounding one epic And then each of the individual muscles |
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| 13:08 | gonna be wrapped in deep fashion which just connective tissue. And then the |
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| 13:13 | groups of muscles that separate them like whole body muscles is separated from another |
|
| 13:19 | of fashion which is called superficial. this is where I get to ask |
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| 13:22 | question if anyone ever gun hunting An animal is where like one or |
|
| 13:27 | people are gonna raise their hands, ? And they're all like you're all |
|
| 13:30 | . Like. No. This is what we do we do that If |
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| 13:33 | never done that, have you ever to prepare a whole chicken? |
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| 13:38 | Okay. When you buy without plucking , right. But you go and |
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| 13:41 | get the chicken. And what do see underneath the skin you can see |
|
| 13:45 | the muscles are kind of already pre for you and connective tissue, |
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| 13:48 | And then um when you get gross and you actually get to start start |
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| 13:53 | cadavers, you'll actually get to start know playing with that stuff and actually |
|
| 13:58 | out muscles themselves. So what you're here is you're just looking at the |
|
| 14:02 | layers of connective tissue. That kind hold the whole thing together. |
|
| 14:05 | So, this is the most outermost tissue up there. That in a |
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| 14:10 | is the innermost connective tissue around each the individual cells that separate them from |
|
| 14:14 | other. Um I point out also bone is connected via a tendon. |
|
| 14:20 | , when you take this connective tissue bring it together, we're talking about |
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| 14:23 | Indonesian paramecium. And in these three layers, they come together at the |
|
| 14:28 | of a muscle and they create the and it's a tendon that's attached to |
|
| 14:32 | bone. So, when you contract muscle, what are you pulling on |
|
| 14:36 | ? And what's the tendon attached to pulling on the bone? Alright. |
|
| 14:41 | , to make my arm move. contracting a muscle which causes the tendon |
|
| 14:45 | stretch a little bit. But it pulls right? Cause tendons have a |
|
| 14:49 | bit of given them. Right. then that pulls on the bone and |
|
| 14:53 | moves the bone and that's what local is. Simply moving the bones in |
|
| 14:57 | to muscle contraction. All right. , I wanted you to be aware |
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| 15:02 | those of what we're talking about when talking about movement here. All |
|
| 15:07 | We got a diamond. An anatomy little bit. And the reason we |
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| 15:11 | into is just because one there's special that's used in muscles, Right? |
|
| 15:16 | number two, we're gonna be looking gonna be setting up a rube Goldberg |
|
| 15:20 | . You know what rube Goldberg Right? That's when you knocked the |
|
| 15:24 | and then at the end of it captured a tiger or something. |
|
| 15:28 | All these different little contraptions that go the way. So that's what this |
|
| 15:32 | . So the way that this makes easy is just think of the steps |
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| 15:36 | they're going along. So we're gonna at step eight and step B. |
|
| 15:39 | steps D. C. And then almost skipped over sea. Right? |
|
| 15:43 | then that's gonna be how a muscle of works. So we need to |
|
| 15:46 | the parts, right? If you're how a car works, you're gonna |
|
| 15:52 | up in the engine and you're gonna pointing out structures and you're gonna |
|
| 15:55 | what's that? That's a carburetor, does it do? It does this |
|
| 15:59 | then you're gonna name all the parts then you put them all together and |
|
| 16:02 | you know how the engine works. , physiology is a lot like working |
|
| 16:07 | cars. I don't know anything about . All right. First off the |
|
| 16:12 | membranes called ASarco lemma. See they're people. So they got to name |
|
| 16:16 | cells specially and so their parts get specially Sarko Lemma not plasma. Lemma |
|
| 16:22 | . Alright, the plasma the sight plasma is called ASarco plasma, sorry |
|
| 16:28 | plasm Gosh, I'm so tired. right now, is it different than |
|
| 16:34 | other cytoplasm. Not really, but are some unique things that kind of |
|
| 16:38 | out in it. First off there's are just fancy way of saying sort |
|
| 16:44 | glycogen Granules. So why would I to start glycogen Granules? A. |
|
| 16:50 | . P. Right. Do I to wait for sugar to be delivered |
|
| 16:54 | my muscles? Know if I'm being by a tiger? I want my |
|
| 16:57 | now and I just want to just right to the stores. Alright, |
|
| 17:02 | . Myoglobin is found inside these It binds up auction. It's a |
|
| 17:07 | to hemoglobin. So hemoglobin binds up in the blood. That's what helps |
|
| 17:11 | greater oxygen to our cells. Do want to wait for my lungs to |
|
| 17:15 | pumping more? No, I'm going have auction readily available to me so |
|
| 17:20 | can see already have the stuff ready do what I need to do. |
|
| 17:24 | right, lots of mitochondria. What have mitochondria A. T. |
|
| 17:28 | Alright, muscles use a lot of . T. P. I need |
|
| 17:32 | of mitochondria to make that a And lastly their multi nucleotide. Why |
|
| 17:36 | you think I'm multi nucleotide? This a trickier question. A lot of |
|
| 17:49 | , I mean that's that's a good . It's actually yeah. What do |
|
| 17:52 | think? Okay so so that's a and an egg thing. So they |
|
| 18:02 | so long but why are they so . Do the cells start off |
|
| 18:08 | No they don't start up big I'm you guys said no. So where |
|
| 18:12 | you think the big sell comes from of smaller cells. So why do |
|
| 18:17 | think they have many nuclei? Because these cells merged together and created a |
|
| 18:22 | very long cell. That's actually the region. Reason for that. |
|
| 18:27 | this is a developmental thing that's actually . So that's why I mean, |
|
| 18:32 | know, I'm not sitting there you don't know the answer. It's |
|
| 18:35 | of like this is kind of Right? I mean, there's a |
|
| 18:38 | places the body where we have these nuclear cells and really, it's a |
|
| 18:42 | of cells combining their their cytoplasm to a better response for whatever that is |
|
| 18:48 | they're doing. And this is one those cells. All right. |
|
| 18:52 | the one thing that's interesting or different these cells is they have what is |
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| 18:55 | a saarc Amir. A sarcoma is functional unit in a cell. All |
|
| 19:00 | . So, an individual cell can very long. It's as long as |
|
| 19:04 | muscle itself is. All right. the muscle fiber, right. Just |
|
| 19:10 | my bicep for example is attached here attaches down here. Right? So |
|
| 19:14 | would be the origin and the And then so the fibers that make |
|
| 19:19 | that bicep are the entire length of muscle itself, that name muscle. |
|
| 19:25 | , So within their it's about this and that means it's gonna have multiple |
|
| 19:32 | tiny Sakai mirrors within it. And of those sockeye mears represents the unit |
|
| 19:37 | we're looking at? So, there be 1000. I don't know how |
|
| 19:40 | there are in an individual state, there's thousands of them. And so |
|
| 19:44 | we're talking about the contract, I'll of a muscle. We're talking about |
|
| 19:47 | little itsy bitsy, teeny tiny unit which there are many of them right |
|
| 19:51 | to one another. All right. so, the defining uh structure of |
|
| 19:56 | sarcoma here. So, you can here is a This is actually the |
|
| 20:00 | fiber. All right. And you can see here these are mild |
|
| 20:04 | brill's And inside that mile five you can see there's a defining line |
|
| 20:09 | called a Z disc. What you're is you're looking at a bunch of |
|
| 20:12 | in a lattice from this angle. you look at something from that |
|
| 20:17 | it's flat, isn't it? But you turn it, you're gonna see |
|
| 20:20 | there's actual structure to it. All . And so, that's one Z |
|
| 20:25 | is this lattice work, and then travel a certain distance away and you'll |
|
| 20:28 | another Z disc. You travel a distance away. There'll be another one |
|
| 20:31 | another one and another one. each of these from Z. Dist |
|
| 20:35 | Z. Disc is a sarcoma. so when we're talking about the microscopic |
|
| 20:39 | that's going on. We're in that tiny space inside of a side of |
|
| 20:43 | larger cell. That's however long the that you're looking at. All |
|
| 20:50 | Now, when you contract, what gonna be doing is you're gonna be |
|
| 20:54 | the circle here. Alright, so that contract. I'll unit when you |
|
| 21:00 | . So, remember when you started life, how big were you? |
|
| 21:04 | a bit of your single cell, . You became a fetus and you |
|
| 21:07 | born. And how big were you you were born? That's really the |
|
| 21:10 | . I should have looked at you this big. All right. And |
|
| 21:13 | look how big you are. You're big. All right. It's |
|
| 21:20 | Looking at a little kid's hand relative your hand. All right. It's |
|
| 21:24 | this little tiny dot, right, speaking. So, when they grew |
|
| 21:29 | muscles grew and when their muscles what they did is they added sarcoma |
|
| 21:33 | the ends or within the structure of muscle. And so that's how they |
|
| 21:39 | . So a muscle increases in length adding those circum ears. So, |
|
| 21:44 | a growth thing. All right, , the sarcoma is a finite length |
|
| 21:53 | structures. Alright, so, we're to this side of the cartoon right |
|
| 21:58 | , within that structure we have in plasma critical um smooth and a plasma |
|
| 22:03 | um uh particularly. And it's been to store up calcium. And so |
|
| 22:08 | given it a special name. We it the psycho plasma particular um |
|
| 22:12 | the cytoplasmic particular um has this unique . So you can see here we've |
|
| 22:16 | it out and as you can it's fairly thin. The small cyst |
|
| 22:20 | like they do. But then when get to the end of that psycho |
|
| 22:23 | particular, it bulges out. And this bulge is referred to as a |
|
| 22:27 | cistern E. So this is where predominant portion of the calcium is going |
|
| 22:32 | be stored up because there's just more . And then right next to that |
|
| 22:36 | end that terminal cistern E. In . Uh moving along the length of |
|
| 22:42 | , the structures are what are called T tubules or the transverse tubules. |
|
| 22:46 | , transverse tubules is simply a tube opens up to the surface of the |
|
| 22:51 | and then travels through the cell and up onto the other side. It's |
|
| 22:55 | tunnel, alright. And so it basically bringing the surface deep to the |
|
| 23:04 | . That kind of makes sense. right. So, I think we |
|
| 23:08 | a picture here. I'm gonna show little bit in about two slides. |
|
| 23:12 | right. So, what I want to think about this little structure |
|
| 23:14 | This transverse tubules is a tube that's up to the external surface and brings |
|
| 23:20 | external surface down deep through the Kind of like a hole in a |
|
| 23:25 | , right? Or like a straw surface deep two, and then opens |
|
| 23:30 | on the other side. Alright, , that's what it kind of looks |
|
| 23:33 | . And you can see here structurally blue represents the t tubules, yellow |
|
| 23:38 | the cytoplasmic articular, the bulge to at the end of the cycle plasma |
|
| 23:42 | , right next to the t Is that uh terminal cistern? |
|
| 23:48 | So what we're gonna do is we're walk through all these structures and what |
|
| 23:52 | doing when we stimulate the cell. . And then we're gonna pause and |
|
| 23:57 | we're gonna go and talk about a more things. All right, so |
|
| 24:00 | we are. This is a Alright. What we're looking at is |
|
| 24:05 | motor in plate, see the special . It gets a special name because |
|
| 24:09 | is the interaction between a neuron and muscle fiber. So the post synaptic |
|
| 24:14 | is actually referred to as the motor in play. What you have is |
|
| 24:18 | have tons and tons and tons of receptors. And then you have a |
|
| 24:23 | bunch of vesicles just lined up full acetylcholine. And so when an action |
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| 24:28 | travels down that axon down to the terminal, it causes the opening of |
|
| 24:34 | or opening of these calcium channels, calcium comes in, causes the vesicles |
|
| 24:38 | be released, releases all the acetylcholine the motor in place or into the |
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| 24:43 | cleft to the motor in plate that binds up to those channels and cause |
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| 24:48 | those channels to open. And what's about this is that here we're not |
|
| 24:53 | an E. P. S. . Down in our post synaptic cell |
|
| 24:56 | , what we're getting is we're releasing much acetylcholine that the the greater potential |
|
| 25:02 | produced here has a magnitude so large it results in an action potential. |
|
| 25:07 | for every action potential in that motor you get an action potential down here |
|
| 25:12 | your in your muscle cell kinda All right. So you can imagine |
|
| 25:17 | getting a greater potential that reaches threshold an action potential. The potential begins |
|
| 25:21 | along the surface of the cell and nothing new that we've learned here. |
|
| 25:26 | . The difference being that we just a muscle cell instead of a neuron |
|
| 25:29 | this side. Right? So you see we refer to as the in |
|
| 25:33 | potential. So E. P. becomes an action potential along it travels |
|
| 25:37 | the length of the cell and on surface of the cell. So here |
|
| 25:40 | is traveling along the surface of the and it comes across you can see |
|
| 25:45 | would just keep on going. But also has these t tubules and what's |
|
| 25:50 | tubules, it's just surface moving closer the inside of the self. And |
|
| 25:53 | those action potentials continue on down through inside of these t tubules and they'll |
|
| 25:59 | keep going to the other side. here is where we're gonna encounter something |
|
| 26:05 | . All right so in the t we have a series of channels. |
|
| 26:11 | or not channels we have a series of receptors are called D. |
|
| 26:15 | P receptors. And these D. . P receptors are closely associated with |
|
| 26:20 | type of receptor called or iodine Alright. And so the D. |
|
| 26:24 | . P receptors in their iodine receptors gonna go to a better picture I |
|
| 26:29 | . Okay here we go. So have the D. H. P |
|
| 26:33 | and here's the ride on receptors notice on the terminal sister knee and what |
|
| 26:37 | is is as as an action potential down it causes the opening of these |
|
| 26:41 | . H. P receptors which are or attached to the right and receptors |
|
| 26:45 | basically pull those open and that causes release of the calcium into that |
|
| 26:52 | And so when an action potential occurs we're seeing is a massive rush of |
|
| 26:57 | from these sarko plasma critical um into cytoplasm or the sarko plasm of the |
|
| 27:06 | so far. You with me so one action potential or actual causes release |
|
| 27:12 | acetylcholine. Acetylcholine causes opening of those , causes an ep ep ep ep |
|
| 27:18 | big enough that it causes another action . Action potential travels along the length |
|
| 27:22 | goes into the T. To be down through the T. To be |
|
| 27:25 | causes the opening of the D. . P receptors. D. |
|
| 27:28 | P receptors are associated with the right receptors right Iron receptors open up calcium |
|
| 27:33 | out of the of the terminal sister , out into the cytoplasm so so |
|
| 27:39 | it's just a whole bunch of calcium a whole bunch of different places in |
|
| 27:42 | to an action potential so far. good. All right. Yeah, |
|
| 27:53 | Yeah. So so what we're doing is we're parsing words. Alright, |
|
| 27:58 | this is like moving from like freshman two now to the junior level. |
|
| 28:03 | it's just saying the portion of the , plasma particular um that is engaged |
|
| 28:09 | holding the calcium. So it's the structure, It's just the region. |
|
| 28:13 | . So putting in the context of room, you're sitting in the middle |
|
| 28:17 | the room on the aisle side, you? But you're still in the |
|
| 28:21 | . So we're just adding another word to make you feel smarter than the |
|
| 28:27 | . Yeah. Oh you're jumping ahead the game. Hold that, hold |
|
| 28:38 | thought. If I don't answer the and a couple slides then say you |
|
| 28:42 | answer the question, a couple of and be mad at me and I |
|
| 28:47 | answer it. What's that? Because we need to understand is that circle |
|
| 28:57 | and this is what this is all ? So first off, you've probably |
|
| 29:01 | a slide like this at some point your academic career where you have to |
|
| 29:04 | muscle. Do you all have to muscle at some point? I |
|
| 29:07 | bands, bands, bands Yeah, looking at a couple of people and |
|
| 29:12 | like and I have never seen this in my life. All right, |
|
| 29:15 | remember we have Z lines. So I'm gonna start here with the |
|
| 29:18 | line. So you can see the line is clearly delineated right there. |
|
| 29:23 | that's why they picked that and they that soccer. Now, remember these |
|
| 29:27 | scientists who are looking at this and knowing what the hell they're looking at |
|
| 29:29 | they see are light and dark And so what they're doing is they're |
|
| 29:32 | , oh look, here's a dark . Then we got a light line |
|
| 29:35 | we have a dark line that we kind of a light line. Then |
|
| 29:37 | have a dark line that we have kind of a light line, looks |
|
| 29:39 | that one. And then oh it repeats itself in the opposite |
|
| 29:43 | All right. And so that's why define this. They could have picked |
|
| 29:46 | of these things to start the point definition. Alright, But they happen |
|
| 29:51 | pick right here. So, you see on either side of that Z |
|
| 29:55 | , what we have is the eye . The band represents the thin filaments |
|
| 30:01 | the maya filaments, the structure the of the side of skeleton of the |
|
| 30:07 | fiber. We'll get to what that in just seconds. So, that's |
|
| 30:10 | filament. Alright. This this The a band is from where this |
|
| 30:15 | band begins. And even though you some light stuff in there, It's |
|
| 30:19 | it ends on the other side. , So there's stuff that's going on |
|
| 30:22 | the center of the a band. the a band is that thing and |
|
| 30:26 | represents the thick filaments. Alright. then within the context of that thick |
|
| 30:31 | , we have this kind of lighter , even though there's a dark one |
|
| 30:34 | the inside of that, that little region is referred to as the |
|
| 30:38 | Band. All right now the a really what it is is the overlap |
|
| 30:45 | thick and thin filaments. So what have here is you have a thin |
|
| 30:49 | . Then you have thick and thin and this little H. Band right |
|
| 30:52 | represents where there's just thick filaments. then the M. Line is like |
|
| 30:57 | Z. Line, it's where the filaments are attached. So the |
|
| 31:00 | Line represents the point where the thin are attached. The so that's the |
|
| 31:05 | band is the thin filaments and the filaments keep extending onward and they go |
|
| 31:09 | the a band. A band is the thick filaments are overlapping with the |
|
| 31:13 | filaments. And then that little Band represents where thick filaments are. |
|
| 31:18 | then we repeat on the opposite side the in line. Now, just |
|
| 31:21 | make this easy so that you can , we're gonna pull up to |
|
| 31:25 | you can stand up again and since furiously writing, I'm gonna pull you |
|
| 31:28 | and make you do stuff too stand side by side in the center, |
|
| 31:33 | straight into the light. Don't go the light. Alright. Stick your |
|
| 31:39 | straight out. So you're gonna be in line. See he's an |
|
| 31:43 | Line. Doesn't look like an in to you, yep. So look |
|
| 31:48 | you know what those are? Those that's thick filaments, right? Thick |
|
| 31:55 | . She is a Z. Alright now there would be another line |
|
| 32:01 | the other side. Right? So the line. Stick up your |
|
| 32:06 | Look at that. She has thin . Look at this. Alright, |
|
| 32:13 | you see are they overlapping? So have a Z line from here to |
|
| 32:18 | . That would be the I. . That's half an eyeball and the |
|
| 32:21 | half would be over on that There's an eye band. What would |
|
| 32:24 | be? That would be a the . Continues on that direction. But |
|
| 32:28 | it stopped for sport short period, a little interruption. That would be |
|
| 32:34 | . M H A I. Thanks. You see how easy that |
|
| 32:42 | , you have a visual of that . Okay, you're gonna be called |
|
| 32:47 | again in just a moment. so just be ready to be in |
|
| 32:51 | and the line again, you're like thanks. All right now here you |
|
| 32:55 | see that representation of what's going on and there's a lot more than what's |
|
| 33:01 | being shown here. But I just to point out a couple of |
|
| 33:05 | Alright, when a contraction takes place muscle doesn't stay in this contracted state |
|
| 33:10 | it relaxes, it springs back to original shape, doesn't it? So |
|
| 33:14 | a spring like molecule in there that it to spring back. That molecule |
|
| 33:20 | going to be titan. All Not to be confused with another molecule |
|
| 33:26 | titan. Alright. And it actually you can see here the little blue |
|
| 33:31 | things that's even in the spring shape remind you. That's what it does |
|
| 33:33 | what it is. It's associated to very end of that a band. |
|
| 33:37 | it's basically holding on to the end the thick filament. So when I |
|
| 33:41 | I squeeze tighten down so it's not a spring. And when I |
|
| 33:45 | what happens it's brings back out So it's serving as a spring to |
|
| 33:50 | us back into our original shape of sort here we also have a R |
|
| 33:56 | tenant tenant is found on the end the bands. And it's what attaches |
|
| 34:03 | um thin filaments to the Z. . And the last molecule is nebula |
|
| 34:09 | and is also found attached to the and it sits and goes right down |
|
| 34:13 | center of that thin filament. And it does is it makes sure that |
|
| 34:18 | thin filament is heading straight outward and sag down or sad or point |
|
| 34:25 | And what this does is it increases interaction between the thick and the thin |
|
| 34:30 | so that you can get a contraction that circle mirror right? So you |
|
| 34:35 | how when their arms they were like of doing conquered stuff. What you |
|
| 34:39 | is you want fibers that are gonna parallel to one another so that they |
|
| 34:42 | interact with one another. And what is actually trying to show you is |
|
| 34:45 | you took a cross section, this what the thin filaments would look |
|
| 34:49 | This is what the thick filaments would like. And then together you can |
|
| 34:52 | that if they're arranged in such a . So that for every thick filament |
|
| 34:56 | have six thin filaments or you can the opposite for every thin filament you |
|
| 35:01 | a couple of thick filaments around or thick filaments. And so what you're |
|
| 35:05 | is you're having multiple interactions within these mild fiber pills. All right through |
|
| 35:12 | side of skeletal elements. Yes sir ma'am? Sorry. Well we haven't |
|
| 35:20 | that yet. So just thick and . Or which one is thick. |
|
| 35:23 | , so the a band right It's this right here. So it's |
|
| 35:30 | it's where the band begins, it with the H. And then it |
|
| 35:35 | at the M. And then you a new one. H. All |
|
| 35:37 | way to a. So everything in here is a thick filament, |
|
| 35:44 | That's where you'll see the overlap of thin filament. So I by itself |
|
| 35:48 | thin H. By itself is thick . Is thick and thin crossing over |
|
| 35:52 | other. H. Is thick. ? So there you go. There's |
|
| 35:56 | thick filament right there? Okay. right. So what are these thick |
|
| 36:00 | thin filaments. Alright. And I part of the answer over there, |
|
| 36:13 | . You keep getting ahead of the both of y'all? Yeah. |
|
| 36:16 | The answer is yes. All And we're gonna I was gonna demonstrate |
|
| 36:19 | up here I guess I don't have anymore. No. No. They're |
|
| 36:22 | you know you guys please show Sorry. But yes, that's that's |
|
| 36:25 | . In with regard to a sock a contraction. We're gonna see the |
|
| 36:29 | . And the H. Band shrinking . Still coming back to your question |
|
| 36:34 | . But we got to understand what thick and thin filament is. |
|
| 36:37 | thin filaments have three parts and actually than that because your opponent actually has |
|
| 36:43 | parts to it. But we're gonna to keep this really really basic. |
|
| 36:46 | . So first off the thing we're interested, it's acting all right. |
|
| 36:50 | learned about thin filaments being acting? . Acting is the portion that actually |
|
| 36:55 | in the contraction. It interacts with thick filaments, the myosin heads of |
|
| 37:00 | miocene in the thick filaments. So it functionally binds to because it |
|
| 37:06 | that functional site or that active site bind the miocene problem is. You |
|
| 37:10 | want to always by the Mayas and want to protect it? You only |
|
| 37:12 | to buy the medicine when you want create a contraction. So it has |
|
| 37:16 | portion to it called trophy mason with name like triple Medicine. Do you |
|
| 37:19 | it's related to medicine? Probably And it is. And so what |
|
| 37:24 | does is it sits and hovers and mildly attracted to that mice and binding |
|
| 37:30 | . And so what it does is covers that mice and binding site. |
|
| 37:35 | you can see it here, this tiny pink band that goes back and |
|
| 37:39 | . I think that's pink. You , that kind of surrounded basically sitting |
|
| 37:43 | covering up all the mice and binding . So it's in the way you |
|
| 37:47 | interact with it if you're Miocene, though you might be ready to. |
|
| 37:51 | the only way that you can interact this thin filament with the act then |
|
| 37:55 | if you move the trump out of way and that's what proponents job |
|
| 37:59 | Troponin is bound up to the triple . It's bound up to the acting |
|
| 38:05 | kind of serves kind of as a a as a link to hold it |
|
| 38:09 | place. But holding the trophy Miocene place. And then the third part |
|
| 38:13 | up calcium. Now you might start , oh, maybe I understand now |
|
| 38:17 | I'm releasing calcium right? Because if binds up calcium and it's helping to |
|
| 38:22 | the trope of Miocene in place, if I had calcium, it's gonna |
|
| 38:25 | it out of the way. So acting becomes free. And the answer |
|
| 38:28 | that's what it's gonna do. But get back to that. Hate trying |
|
| 38:32 | tell you the story before the story there. All right. So let's |
|
| 38:36 | to the thick filament, thick filaments like golf clubs that someone got really |
|
| 38:39 | angry about. Right? They wrapped shafts together. And really that's what |
|
| 38:46 | is. Just basically these really really bodies with these heads. And there's |
|
| 38:50 | there's a hinge portion that allows the to actually move. And so you |
|
| 38:54 | kind of think remember the picture that that boxer from the 1860s like |
|
| 38:58 | you know? And he's like this how he boxes. That's what the |
|
| 39:04 | heads do they move because of these portions. Now, that hinge portion |
|
| 39:09 | what what separates attitude? It's basically heavy chain is what so you got |
|
| 39:13 | light chain of the heavy chain. heavy chain is where you have the |
|
| 39:17 | binding site. So you can see here, that would be the heavy |
|
| 39:20 | . All right, that's where the site is gonna be located. It |
|
| 39:23 | has an A. T. A. Site whenever I have an |
|
| 39:26 | . T. P. A What am I trying to do? |
|
| 39:29 | to release energy from a T. . So here you can see, |
|
| 39:34 | I'm probably going to be using energy move that head around. All |
|
| 39:39 | Um We also have the light chain which we'll get to in just a |
|
| 39:43 | . Um But in essence what its is is to help stabilize the structure |
|
| 39:49 | it's gonna be um It's gonna be primarily in the other cell types. |
|
| 39:55 | right. So, what I want to focus on is the head and |
|
| 39:58 | how they're all wrapped up together. get a whole bunch of these |
|
| 40:02 | They're always paired up together as a a pair. And then you take |
|
| 40:05 | pears and then you just start creating bundles. And so each of those |
|
| 40:11 | and heads are gonna be working independently each other. But they're all those |
|
| 40:14 | heads are working on the same acting . It'd be like being able to |
|
| 40:18 | to or or hold on to a . Right? If I grab the |
|
| 40:21 | with one hand and let go and on a spring. What's it gonna |
|
| 40:24 | ? It's gonna keep going back. , what I can do now is |
|
| 40:27 | can grab and pull the acting like with the two heads. But remember |
|
| 40:33 | got lots of these heads that are with all these different acting molecules. |
|
| 40:38 | right. Let's see if we're back the story. Yes. Alright. |
|
| 40:42 | , when we think of a muscle , we usually think of energy and |
|
| 40:45 | think of a T. P. is not what's causing the contraction. |
|
| 40:49 | thing that causes the contraction is the of the calcium. So, let's |
|
| 40:53 | back to where we started acts potential the in the motor neuron causes release |
|
| 40:57 | acetylcholine. Acetylcholine binds to those channels causes sodium. Come in we'll get |
|
| 41:03 | E. P. P. P. P. Results in an |
|
| 41:05 | potential in the muscle cell. The along the muscle cell travels along goes |
|
| 41:09 | through the T. Tubules activates the . H. P. Receptor which |
|
| 41:12 | activates the right brain receptor which causes release of the calcium into the |
|
| 41:16 | Where is the calcium gonna buy troponin the thin filament And when it binds |
|
| 41:25 | that troponin, what it does is causes a change in the shape of |
|
| 41:29 | troponin molecule which causes the triple miocene be pulled out of the way, |
|
| 41:34 | the acting on the acting that myosin site. Now that head of miocene |
|
| 41:40 | already in position, it's ready to right all you gotta do just move |
|
| 41:45 | out of the way So by moving out of the way. Boom you're |
|
| 41:48 | able to bind when the mice in act and bind. What do you |
|
| 41:53 | happens? Power stroke. That's the thing and that's the next step. |
|
| 41:59 | you need that interaction to occur So the calcium allows for the binding |
|
| 42:04 | take place so that the power stroke take place. Power stroke is just |
|
| 42:10 | fancy word for saying Madison, pulling the acting. All right now this |
|
| 42:14 | where A T. P. Becomes . All right so all we're doing |
|
| 42:19 | my son is the one we're just looking at one head. But you |
|
| 42:23 | imagine I got those two heads doing same thing and an opposition. One's |
|
| 42:27 | one is not there. The other buying the other one releases. All |
|
| 42:31 | . And so, what I want to look at here is where that |
|
| 42:33 | T. P. Is Alright. do we see the A. |
|
| 42:37 | P. Come in right here. is a TPS job? It's to |
|
| 42:42 | the head from the from the So, really what we want to |
|
| 42:48 | is let's pretend this is our starting , right? Instead of this being |
|
| 42:52 | starting point. So, here we in that normal state. A |
|
| 42:55 | P. Is bound to myosin when T. P binds to myosin, |
|
| 43:00 | A. T. P. A that 80 P releases the energy and |
|
| 43:05 | that head to get into the cocked . All right. So, the |
|
| 43:09 | you can think about is here's my . Then I'm over here. I |
|
| 43:12 | interact. But what happens is the . T. P. Comes along |
|
| 43:15 | me and gets me ready to All right. So, now all |
|
| 43:20 | gotta do is be able to interact it. But because I've got trouble |
|
| 43:23 | in the way I can't interact, comes along, moves it out of |
|
| 43:26 | way. Now I can interact when interact with the act. And what |
|
| 43:30 | I do? I pull And that's this is showing. All right. |
|
| 43:34 | mean the cock state I'm able to . So I pull. And what's |
|
| 43:40 | happen is I'm going to release the phosphate. Right? And then there's |
|
| 43:46 | power stroke. And now after the stroke I'm no longer attracted to the |
|
| 43:51 | . So the ADP is released and need to get a teepee once again |
|
| 43:56 | come in to cause me to release going on. So 80 peacocks |
|
| 44:03 | Once I interact I pull I have release the A. D. |
|
| 44:08 | A. T. P. Comes releases me. I do the |
|
| 44:11 | T. P. S. I'm cocked. I'm ready to go |
|
| 44:16 | . And how do I remember How do I remember the role of |
|
| 44:19 | . T. P. What is of the characteristics of a cadaver after |
|
| 44:24 | died? What is the state that goes into stiffens up? Which has |
|
| 44:29 | special name, rigor mortis. Why does rigor mortis even occur? |
|
| 44:34 | , it's a function of the two that we just looked at. All |
|
| 44:38 | , When your cells are no longer . Alright, so when you're |
|
| 44:45 | nothing is driving the activity of the . Right. But they still have |
|
| 44:49 | teepee and then still have calcium in . But nothing is driving the |
|
| 44:53 | And so what happens is the first is all the calcium gets released from |
|
| 44:57 | cycle Plaza particular goes down to the . So, your cells are flooded |
|
| 45:00 | calcium. Well they're flooded with That's gonna cause the trouble troponin to |
|
| 45:05 | out of the way so that my can interact. You still have a |
|
| 45:09 | in yourselves. What's the A. . P. Gonna do? It's |
|
| 45:11 | allow you to create a series of until you run out of A. |
|
| 45:14 | . P. And then what have done is you've created a sustained contraction |
|
| 45:19 | now you are in rigor mortis. . And then after a little while |
|
| 45:24 | sell, start breaking down and that's you go back into that relaxed state |
|
| 45:28 | your now rotting you. Okay? what does a. t. |
|
| 45:33 | two allows me to break the bond that my muscle is no longer in |
|
| 45:39 | contraction. Right now I'm sustaining the because I'm using the two heads. |
|
| 45:46 | if no calcium is there and A . P. Is present, that's |
|
| 45:50 | break the bond, that's gonna allow to take place. That can make |
|
| 45:54 | . Yeah. Yes. Right so triple the way I remember it |
|
| 46:03 | Triple medicine is related to medicine so mildly attracted to the myosin binding site |
|
| 46:09 | acting. So Troponin pulls the triple out of the way. Right, |
|
| 46:15 | like the chaperone, it's not letting couple get together, you stay apart |
|
| 46:20 | what it's doing, if that makes . Alright. So the power stroke |
|
| 46:27 | because a tee pee breaks the bond then going through the process of processing |
|
| 46:33 | a teepee that allows for the power to occur, that's what's going on |
|
| 46:40 | here at this stage. So how we relax? The muscle take to |
|
| 46:47 | and call me in the morning? one knows what selma is. See |
|
| 46:51 | guys are such a good generation. a muscle relaxant. It's a prescription |
|
| 46:56 | relaxing that was heavily abused in the and 90s. Hmm. Yeah. |
|
| 47:06 | have a friend who's a rarely really attorney now. Um That's what what |
|
| 47:10 | thing was in college. Yeah. . Yeah. Alright. So how |
|
| 47:20 | you relax? Well, simply put are the two things that that result |
|
| 47:25 | a contraction calcium and A T. . So if I get rid of |
|
| 47:31 | calcium, will I have a So what will that cause basically I |
|
| 47:36 | be able to get the contraction. I'm now creating the state for real |
|
| 47:39 | to take place and then if I a T. P. That's gonna |
|
| 47:43 | the bond. So now the muscles back into their original shape. All |
|
| 47:47 | , So what moves the calcium is pump called circa. Alright, circa |
|
| 47:55 | found on the Circle Plaza particular. always on And so you're always using |
|
| 48:03 | TP to pump calcium back out of environment when you have an action potential |
|
| 48:09 | causes the opening of those ride on more calcium leaves and gets pumped back |
|
| 48:13 | . That's why you get the state the state of that calcium influx. |
|
| 48:17 | when there's no calcium or sorry when no action potential, calcium is no |
|
| 48:21 | being released. And so now the is able to do all the hard |
|
| 48:25 | of moving the calcium back out and that muscle goes into that relaxed |
|
| 48:29 | Alright so the key thing here is plays the major role of allowing the |
|
| 48:36 | to occur because it's allowing the mice the action and the acting to |
|
| 48:41 | Okay it's not the A. P. A. T. P |
|
| 48:44 | the bond between the two as long A T. P. Is not |
|
| 48:47 | . You're gonna have a sustained All right so far that makes |
|
| 48:57 | Okay. No it doesn't. Well walk through the whole thing if it |
|
| 49:02 | make sense. Let's walk through the thing. Step one action potential through |
|
| 49:05 | motor neuron step to release of acetylcholine the synaptic cleft under the motor in |
|
| 49:10 | . Get an E. P. . At the motor inn plate that |
|
| 49:12 | in an action potential on a muscle action potential travels along the surface of |
|
| 49:16 | cell. Goes down through the T , binds to an active or not |
|
| 49:20 | to but opens up channels which are D. H. P. Receptors |
|
| 49:24 | are associated with the ride in receptors causes calcium to e flux out of |
|
| 49:27 | cycle plasma particular um into the Right lots of lots of calcium binds |
|
| 49:35 | the opponent moves out of the Makes the myosin binding site available and |
|
| 49:40 | . My son is already in position its act and binding site to be |
|
| 49:44 | to interact with that as long as a teepee available. What we're gonna |
|
| 49:47 | is we're gonna get the power We'll be able to break reset power |
|
| 49:52 | and just keep that to maintain or contractions when I stop releasing calcium. |
|
| 50:00 | other words when there's no action potential gets put back into the circle plasma |
|
| 50:05 | I'm no longer able to interact. so the muscle goes back into its |
|
| 50:09 | state because the A. T. . Allows you to break that |
|
| 50:14 | That makes more sense. I know went fast but see there's a picture |
|
| 50:17 | it and you can see in three I could have explained the whole thing |
|
| 50:23 | by looking at this one picture. you would all like I don't understand |
|
| 50:26 | cartoon. What's this strange looking thing here. Right and that's what I |
|
| 50:30 | to avoid. Is the strange looking . Yes sir sir. Just no |
|
| 50:37 | calcium is being removed circa is the the means by which calcium is being |
|
| 50:42 | . It's always on even in the of of pumping or releasing calcium out |
|
| 50:47 | the cytoplasm. It's just it's a a pump that's slower than opening up |
|
| 50:51 | the right and receptors. Right so what all this just tells you and |
|
| 50:56 | just follow follow along. Right here's motor in place. You can see |
|
| 50:59 | D. H. P. That be the right iron receptor. And |
|
| 51:03 | this is showing what happens when calcium released. So one picture is all |
|
| 51:07 | need. You can draw it out you draw it out it makes 20 |
|
| 51:10 | more sense. Yeah, circa No there are So what's happening is circa |
|
| 51:19 | is simply always on. So if if I'm just gonna make up a |
|
| 51:23 | let's say the ratio is 4 to . So if I'm having four calcium |
|
| 51:27 | while one calcium being pumped back Obviously the calcium going out is favored |
|
| 51:32 | when I shut those right iron Now what I'm doing is I'm pumping |
|
| 51:37 | back at a greater rate. So why it's working. I still haven't |
|
| 51:43 | to it yet. I'm going to I don't get to it I will |
|
| 51:46 | stop and say all right. How we get bigger and stronger? All |
|
| 51:49 | . So first off, there are types of contractions. They're what I |
|
| 51:52 | isotonic contractions. And isometric contractions. with with regard isotonic there's gonna be |
|
| 51:58 | types of isotonic contractions when you're changing muscle length. Alright so usually I |
|
| 52:04 | some sort of prop that I can with. I guess I'll just use |
|
| 52:07 | bag. All right. So So I've got all the floppy |
|
| 52:16 | Alright so here I am with my , if I am lifting this up |
|
| 52:21 | curling it. What's my bicep Getting longer or shorter? And it's |
|
| 52:25 | shorter. Good. Alright so when put the bag back down is the |
|
| 52:29 | changing shape again? It's getting what , shortest thing? The same |
|
| 52:33 | Alright, so you just witnessed two types of isotonic contractions. A contraction |
|
| 52:38 | makes the muscles shorter. That's concentric when the contraction that is allowing the |
|
| 52:44 | to become longer, that's called Alright, now the other type is |
|
| 52:50 | isometric contraction. Now isometric is where increasing and I should have said in |
|
| 52:56 | isotonic you're not increasing the uh the that you're producing, the forces being |
|
| 53:03 | . So in other words, the of this does not ever change, |
|
| 53:08 | it? In the in the course me lifting up and putting it back |
|
| 53:11 | again. Right. So I only to create enough force to overcome the |
|
| 53:16 | of the bag. So once I that force to overcome the load, |
|
| 53:20 | maintaining that force to be able to that odd item. Right. |
|
| 53:27 | So what is that? Like So I'm creating enough force to generate |
|
| 53:31 | overcome £5 and I can move the or I can set the £5 |
|
| 53:37 | I'm still moving the £5. So the load and the force that I'm |
|
| 53:43 | with an isometric contraction, the length change. But the force I'm |
|
| 53:49 | the tension in that muscle is Alright, so there's never really a |
|
| 53:54 | way to show this. Um So just gonna go up against this wall |
|
| 53:58 | closer so you'll just have to bear me. Alright, so here I |
|
| 54:02 | , I'm pushing up against the right? You can see my |
|
| 54:05 | Look at that and look at that muscle right there, right? So |
|
| 54:09 | can see I'm not putting a lot tension into that muscle to push that |
|
| 54:12 | , but can I produce enough tension knock that wall down? Come |
|
| 54:17 | have a little faith. No, cannot. This this wall isn't. |
|
| 54:21 | , So I can apply force, force, apply force, apply |
|
| 54:25 | And no matter how much tension I into my arm, the muscles not |
|
| 54:30 | its length. Right? So, want to try this yourself? You |
|
| 54:35 | do it in your chair, You got one arm, you got |
|
| 54:37 | arm them again against each other, ? And now produce a little bit |
|
| 54:41 | force. You can do it with . All right. Just a little |
|
| 54:44 | You don't have to push art? I mean, can you feel that |
|
| 54:47 | creating a little bit of tension? ? Put more attention and more and |
|
| 54:52 | and just keep pushing and pushing and to make your arms move. But |
|
| 54:57 | they're moving in opposite directions are pretty . They're not gonna move anywhere. |
|
| 55:00 | what you just did was an isometric . The muscle did not change its |
|
| 55:05 | , but the amount of tension you did All right. It wasn't enough |
|
| 55:11 | move the load if you've ever gone weights and try to lift something that |
|
| 55:15 | too heavy for you. You like, Oh look, here's a |
|
| 55:19 | weight. You know, you're not the load but you created a whole |
|
| 55:24 | of tension trying to do so. , so those are the two types |
|
| 55:28 | contractions. Now, everything we've described to this point has to do with |
|
| 55:36 | little tiny socks here, with the of the contraction portion. Alright, |
|
| 55:39 | looking at the full length when you at a contraction. Remember that when |
|
| 55:43 | talking about the power stroke and We're talking about a sarcoma here and |
|
| 55:47 | circle here represents a single fiber not a fiber. A single |
|
| 55:51 | Right? And there's lots of socks that one fiber. But look at |
|
| 55:56 | muscle. Your muscle is lots of wrapped into fast calls, lots of |
|
| 56:00 | cools wrapped into a muscle. And when you talk about a contraction inside |
|
| 56:06 | , inside that soccer mayor, we that a twitch. Now don't confuse |
|
| 56:10 | twitch in a sock. Amir as twitch like that. That's that's something |
|
| 56:16 | different. Alright. It's something that's with a volt meter. Right? |
|
| 56:23 | you but you're not gonna see it . All right. And so any |
|
| 56:27 | of signal, any sort of action causes the sock'em ear to contract and |
|
| 56:32 | . That would be a twitch. that's not enough to move anything. |
|
| 56:37 | fiber. Can't do a job. need multiple fibers and you need to |
|
| 56:42 | a sustained contraction. So, what can do is you can do |
|
| 56:47 | All right. Now, the hard to think about here is that action |
|
| 56:51 | are not the same things as All right. And action potential is |
|
| 56:55 | signal to cause the contraction. Remember we saw the action potential travel |
|
| 57:00 | the surface of the cell and then cell released the calcium. And it |
|
| 57:05 | the cell to contract as well to action acting in the my the my |
|
| 57:11 | interacting. All right. So, you look at these up at the |
|
| 57:16 | , the little red arrows represent where action potential is. The green graph |
|
| 57:23 | the contraction. They're independent of each in terms of measure. And you |
|
| 57:28 | see here this is what a twitch look like. Right? There is |
|
| 57:31 | potential. You get a little tiny , Get another one. Doesn't do |
|
| 57:36 | . You can get them a little closer together. And that's that temporal |
|
| 57:40 | kind of like what we saw when were trying to deal with magnitude and |
|
| 57:43 | action potential. So you get a of action potential in a row and |
|
| 57:47 | growing on each other. And so get kind of this, this kind |
|
| 57:50 | twitchy activity. It's still not enough actually create a sustained contraction. But |
|
| 57:57 | you get a whole bunch of action together and they're really, really |
|
| 58:01 | what you'll do is you'll get a contraction that's being maintained. That's that's |
|
| 58:06 | sustaining, right? This is what referred to as tetanus. Alright, |
|
| 58:13 | is what allows your muscles to do they do. They're creating that tension |
|
| 58:18 | cause movement and each of the individual , like I said, they're not |
|
| 58:22 | enough to do anything. So twitch really not doing anything but tetanus in |
|
| 58:27 | single fiber can't do anything. What need to do is you need to |
|
| 58:29 | multiple fibers working in concert to get to happen. That kind of makes |
|
| 58:36 | . If I'm pulling on a I can't move it by myself. |
|
| 58:39 | I get me and my buddies we can pull cannons out of the |
|
| 58:43 | if we need to. That's actually tug of war actually really was strength |
|
| 58:48 | cannons out of the mud. All , and that's what we're looking at |
|
| 58:52 | we're looking at tetanus. How do remember what tetanus is? What happens |
|
| 58:55 | you step on a rusty nail in parking lot? You get lockjaw. |
|
| 59:01 | right. That's tetanus, right? do they call it tetanus because of |
|
| 59:07 | the lockjaw. That's the ideology. how it appears. It causes a |
|
| 59:12 | contraction in the jaw muscles. I know why? Don't ask me |
|
| 59:16 | but that's where it comes from. was gonna take a sip but apparently |
|
| 59:22 | . Alright. We're almost getting to answer. Motor units. A motor |
|
| 59:29 | represents the neuron and the fibers. innovating. Alright. Motor units have |
|
| 59:36 | sizes depending upon the activity that they're for. All right. So, |
|
| 59:42 | example, in this little cartoon you see here is a single axon and |
|
| 59:46 | has 123 collaterals. And it's innovating fibers. So this motor unit is |
|
| 59:54 | axon plus those three fibers. And the activity that this one can produce |
|
| 60:00 | the amount of tension that those three by themselves could produce. Different motor |
|
| 60:07 | can be of varying sizes. If doing very fine activity. What you'd |
|
| 60:12 | is you'd have a couple of fibers neuron. What's an example of fine |
|
| 60:18 | ? Fine motor activity. Writing. That's the easiest one to think about |
|
| 60:23 | writing, right? It's having really degree of control so that you can |
|
| 60:27 | all that beautiful calligraphy that you're Right? Or the chicken scratch in |
|
| 60:33 | case. All right. If I'm with course activity, what would be |
|
| 60:38 | example of course activity, lifting Walking, right. What is |
|
| 60:44 | We've already talked about this. Walking not falling. Right? I lift |
|
| 60:48 | my look, right? I that's course activity. And so what |
|
| 60:54 | I doing? I have a single going down to hundreds of fibers to |
|
| 60:58 | contract so that you can lift up clunky leg, relax it fall |
|
| 61:04 | All right, So that is how motor units work. And so when |
|
| 61:11 | talking about an activity. So, example, if I wanted to curl |
|
| 61:15 | , do you think that weighs a ? No. Right. So I |
|
| 61:19 | put it in my hand and I do a curl of this house and |
|
| 61:22 | could see that I would probably not . I don't need a lot of |
|
| 61:26 | units to cause that curl, But I can add weight to |
|
| 61:30 | I'm gonna put my phone in my . So now I've doubled the |
|
| 61:33 | So I may need more motor units be able to do that activity. |
|
| 61:39 | then we can get to bigger and things, you know, sometimes there's |
|
| 61:43 | chair in here and I'll curl the . Right? But this obviously weighs |
|
| 61:47 | than those two little things, Right. So, it's the same |
|
| 61:52 | , the same muscle groups. But recruiting more and more motor units. |
|
| 62:01 | ? Um So, that's actually on different slide, but in essence, |
|
| 62:07 | in order to create a movement and increase the tension, I'm going to |
|
| 62:12 | in more and more fibers. more motor units to to accomplish the |
|
| 62:18 | . Yeah. Oh my goodness. . All right. So let's hope |
|
| 63:06 | don't know how much we've we've missed . Yeah, I don't know, |
|
| 63:12 | oh well the good news, how , how many years I've been teaching |
|
| 63:16 | ? 16. How many lectures have recorded? About 30. So if |
|
| 63:21 | missed this one you can go and to an old one. It's not |
|
| 63:24 | good as this one though. So the other thing is is that |
|
| 63:32 | the motor units themselves are never gonna clustered. Right? So what you |
|
| 63:36 | do is you want to spread your units around the muscle itself so that |
|
| 63:40 | you create a contraction, you're actually a contraction in the same direction. |
|
| 63:46 | ? So just think of my I don't want all my motor units |
|
| 63:49 | one side so that when I create contraction pull this way you want it |
|
| 63:53 | that it creates that one movement that trying to accomplish. So these are |
|
| 63:57 | distributed and there's many of them so they can have an additive effect on |
|
| 64:03 | activity that you're trying to accomplish. know I'm gonna forget those. All |
|
| 64:11 | . I'm gonna answer your question now I don't know if I have a |
|
| 64:15 | for this just 15 minutes. Good . One of these days. I'm |
|
| 64:22 | gonna come in here. You tell what I'm supposed to say and then |
|
| 64:25 | just get it done and then I'll add to it at the end of |
|
| 64:27 | . Alright with regard to getting What you don't do is you don't |
|
| 64:33 | more sarcasm. Here's what you do you add more mild fibers to the |
|
| 64:37 | here. Alright so remember how we that cross section. Right? So |
|
| 64:42 | about when you when you work out your muscles do they go? Which |
|
| 64:46 | did they go this direction or they this direction? They go this |
|
| 64:49 | So what you're doing is you're taking little tiny muscle fiber, that cell |
|
| 64:53 | what you're doing is you're jamming in and more mild fibers so that that |
|
| 64:56 | goes like that. Then you add more and more of those fibers. |
|
| 65:01 | many fibers doing many of my fiber and that's why your muscles get all |
|
| 65:04 | and bulgy. So it's adding mild not acting fiber rules. Alright. |
|
| 65:11 | both white and dark meat, You guys like white meat and |
|
| 65:15 | We're getting close to thanksgiving. We I mean two months. But I |
|
| 65:18 | you should be making plans at this right? Each of your muscles, |
|
| 65:21 | have both fast and slow versus oxygen like elliptic in terms of their |
|
| 65:27 | And really this just tells you there you see fast versus slow. This |
|
| 65:30 | talking about how quick their twitch activity . Fast fibers are gonna twitch |
|
| 65:35 | Slow fibers are gonna twitch slowly. ? And so fast ones are going |
|
| 65:39 | um create these strong contractions. Slow are gonna be sustained contractions when you're |
|
| 65:47 | with oxidative versus glock elliptic? It's telling you what sort of pathway you |
|
| 65:51 | dependent on oxidative phosphor relation. Or you dependent on glycol icis? |
|
| 65:56 | So if you're like Alice is how A. T. P. Are |
|
| 65:59 | gonna use roughly to? Right? gonna you're gonna make to write oxygen |
|
| 66:04 | elation roughly? 32, 34, . Whichever number you happened to land |
|
| 66:09 | the time that they were teaching Right. And so. Right. |
|
| 66:14 | mean, there's gonna be more. ? And so you can imagine I |
|
| 66:19 | fibers that are gonna be dependent upon those steps to make energy which allows |
|
| 66:25 | to sustain activity for longer periods of . So, I become I'm basically |
|
| 66:31 | resistant, whereas if I'm uh dependent glycol assists, I can fatigue fairly |
|
| 66:37 | . All right. And so we three fibers that are based upon those |
|
| 66:41 | of characteristics and that's what these are oxidative fast oxidation fast, like |
|
| 66:45 | Alright, So, you can imagine I am glycol it, I'm gonna |
|
| 66:50 | um very little myoglobin because I'm just gonna need it. Right? Because |
|
| 66:55 | don't have oxygen phosphor relation where these myoglobin. Um These are the least |
|
| 67:01 | . And there, you know, can see red muscle while they read |
|
| 67:04 | myoglobin. Myoglobin has the pigment that up oxygen. That's why they're |
|
| 67:10 | So, I don't know, breasts, that's in chickens and |
|
| 67:17 | That's what you look like. So all mixed. That's a big old |
|
| 67:23 | . Don't memorize the chart. Just of gives you a sense of the |
|
| 67:28 | . Cardiac muscle not very different from , skeletal muscles. That's why we |
|
| 67:33 | have one slide structurally. When you at skeletal muscle, there long strands |
|
| 67:38 | long as the muscle cells. Cardiac are very, very short and they |
|
| 67:41 | connected in the end and they actually . So, you can see |
|
| 67:44 | like this cell right here, you see it has multiple branches to |
|
| 67:48 | T tubules are a little bit Um, they actually form die ads |
|
| 67:53 | of triads. So, the Circle in particular doesn't have the feet the |
|
| 67:57 | way. So that's why they're die um smaller circle plans were particularly because |
|
| 68:02 | are dependent upon the calcium outside the , not just calcium inside the |
|
| 68:06 | All right. And lots of lots mitochondria because yeah, also they're interconnected |
|
| 68:12 | one another. Be a gap So that when you contract one |
|
| 68:16 | you're gonna be contracting all the All right. So, the potential |
|
| 68:20 | from cell to cell to cell. , we're gonna talk about cardiac |
|
| 68:24 | After the test, when we go the cardiovascular system, we're gonna see |
|
| 68:28 | all this stuff adds up. But just some slight differences, but behaviorally |
|
| 68:33 | , very similar similar to the skeletal . This is just showing you |
|
| 68:38 | Oh yeah, calcium. It's calcium the same thing. Just coming from |
|
| 68:41 | outside the cell. So when I to pump it out what I use |
|
| 68:45 | on the surface of the cells. muscle is the weird one. All |
|
| 68:51 | . So what we have here is have cells that are arranged in Cincy |
|
| 68:57 | . Since issue being cells that are with other cells. We can fall |
|
| 69:01 | one of two categories. It's either be multi unit or single unit. |
|
| 69:04 | I saw one person to email me question about this. And so I |
|
| 69:08 | answer because I wanted to just answer when you're dealing with multi unit, |
|
| 69:12 | you have here are individual cells that innovated individually. So you can see |
|
| 69:18 | I have many units. That's why called multi unit. When you're dealing |
|
| 69:22 | single units you have multiple cells innovated one neuron. And really it's not |
|
| 69:29 | even innovated. What what you can here is that the motor fiber basically |
|
| 69:35 | above and over the cells and it along its length instead of a synaptic |
|
| 69:41 | . It has a series of bulges very costly. And it's from these |
|
| 69:44 | costs that releases a neurotransmitter. And kind of washes over the cell. |
|
| 69:49 | that's what it's kind of trying to you is like look see there's very |
|
| 69:52 | along the length, right along there that's what allows it to release the |
|
| 69:57 | . So this acts as a unit single unit. Hence the single unit |
|
| 70:02 | smooth muscle. So multi unit has units individual cells acting independently single unit |
|
| 70:09 | as one group within the single You can have self excitable cells. |
|
| 70:14 | will see those in cardiac as But I didn't want to deal with |
|
| 70:16 | right now. So these actually are that are deep polarizing at a regular |
|
| 70:21 | and then they can cause independent of of the nervous system to cause the |
|
| 70:27 | sense Isham to de polarize into This is what this is trying to |
|
| 70:33 | you is like see here we've got potentials and then if I get up |
|
| 70:37 | threshold I get a series of action which will result in contraction. This |
|
| 70:40 | another type where you're like I'm slowly polarizing. Reach threshold to get an |
|
| 70:46 | potential, slowly polarizing. So these just two different types of mechanisms showing |
|
| 70:51 | you can have self excitable cells resulting action potentials independent of the central nervous |
|
| 71:00 | . Just another picture. So how I doing now? nine minutes. |
|
| 71:07 | see. And how many slides I like three. four. Oh my |
|
| 71:11 | ! I better stop talking then. good lord. They just like multiply |
|
| 71:16 | rabbits. Alright, structurally. very different. Right. No, |
|
| 71:23 | . Here's the same proteins that are Z lines are found in the smooth |
|
| 71:28 | but they create a different structure called a dense body. And so you |
|
| 71:33 | see here it kind of looks like you if you've ever been watched enough |
|
| 71:37 | or if you've cooked enough, you how to bind up meat. You |
|
| 71:40 | like a ham. That's kind of this is like. So you can |
|
| 71:44 | it's basically a bunch of cross fibers create this lattice work and each of |
|
| 71:49 | points of crossing. That's where those bodies are. So, when a |
|
| 71:53 | occurs, you're pulling towards the dense , Right? But if you're basically |
|
| 71:57 | lattice, that means you're pulling them four different directions. So you can |
|
| 72:01 | what happens when that smooth muscle It looks like a hand. That's |
|
| 72:04 | of squeeze through. All right here, we're going to use a |
|
| 72:10 | system. We have thick filaments, have thin filaments. There's no |
|
| 72:13 | If I have no troponin, that I'm not really pulling things out of |
|
| 72:16 | way the same way. All I have intermediate filaments that kind of |
|
| 72:20 | structure here. Now there are two here that inhibit the activity of mice |
|
| 72:27 | cal opponent and Desmond. And what job is is in essence is to |
|
| 72:34 | the the the activity of the interaction the medicine and the acting. All |
|
| 72:39 | , So, that's that's really what do. So, we don't need |
|
| 72:42 | troponin. We have these other molecules . And what I want to show |
|
| 72:47 | here is I think. Let me double check. Yeah. Okay, |
|
| 72:51 | this is just trying to show you in essence we're still using calcium. |
|
| 72:57 | , so calcium is flowing out and is getting into this area but instead |
|
| 73:02 | the calcium binding to Troponin which doesn't , it has to be doing something |
|
| 73:07 | and that's something different that it does it works through a signaling cascade. |
|
| 73:13 | uses cal module in So remember good can imagine it popped up a couple |
|
| 73:18 | days ago. Alright, so here is, calcium binds to and activates |
|
| 73:21 | module in. What cal Madeline does three different things. First off it |
|
| 73:26 | up to the light chain or not like binds up to a light |
|
| 73:29 | kindness. And so remember we said the hinge portion has a light |
|
| 73:33 | So what we're doing is we're activating keenness that activates that region. |
|
| 73:40 | so that's the first thing that binds and activates mice and light chain myosin |
|
| 73:45 | chain kina activates myosin light chain basically increases a TPS activity. So what |
|
| 73:51 | a TPS do in skeletal muscle? the A. T. P. |
|
| 73:56 | that we could get the head to and create the contraction. So calcium |
|
| 74:03 | a contraction through this pathway. It activates a cow model in kenya as |
|
| 74:09 | which phosphor relates are cal opponent. did cal opponent do? Sorry, |
|
| 74:14 | back to slides it's an inhibitor. what we're doing is we're blocking the |
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| 74:21 | were inhibiting the inhibitor. Right. so when I have two negatives that |
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| 74:25 | in a positive and everything is hunky and the system moves forward. And |
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| 74:29 | other thing it does is it actually to and inhibits cal opponent in and |
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| 74:32 | itself. So calcium does a lot these cells. And instead of going |
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| 74:40 | that troponin pathway where you have all machinery in place, we're going through |
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| 74:45 | cascade that's independent and this is why a weird one. Right? All |
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| 74:51 | same things happen calcium gets released. still get a muscle contraction. It's |
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| 74:55 | the steps in the middle that are . Right? So here calcium isn't |
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| 75:00 | to proponent inviting the cal margin which myosin light chain which activates the |
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| 75:06 | T. P. A. Which causes the contraction. All |
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| 75:10 | It's blocking the inhibitor. And I that's what all this is trying to |
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| 75:14 | is just show you the differences between three things. Was that the last |
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| 75:19 | ? See I told you I could it done. Yeah. Thank |
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| 75:23 | Yeah, you should see there are when I talk like a million |
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| 75:26 | All right, before he goes running of here. I mean are there |
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| 75:29 | questions about this? And I saw hands. Yeah. Okay. About |
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| 75:37 | the calibration. Did we start that ? Damn it. Alright. So |
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| 75:41 | regard to the calibration, I thought changed the date because usually what we |
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| 75:46 | is it's like we have like a to get the paper done. But |
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| 75:49 | some reason I don't know how when looked at the calendar, we had |
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| 75:52 | three weeks so I'm gonna move that . So if you read that paper |
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| 75:55 | the calibration, just hold on to thoughts, we'll come back to it |
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| 75:59 | the test. I don't want I didn't want you to deal with |
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| 76:01 | before the test, but apparently my is in other places, so. |
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| 76:08 | ? Oh yeah. Just no Vegas no Vegas. Uh Hold on. |
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| 76:17 | got his in |
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