| And someone up the back just told me. | |
| It's very hard to tell what the volume is here | |
| at the back. | |
| And you hear me fairly well. | |
| Okay. | |
| Thank you. | |
| And just make sure since I once started a lecture | |
| and got 10 minutes through it until someone told me | |
| they were in the maths department, weren't quite sure what | |
| neuroscience to do with that degree. | |
| We are here for brain and behaviour. | |
| Is that correct? | |
| Good start. | |
| Okay. | |
| Oh, I get a little bit slowly over the next | |
| couple of minutes. | |
| Just make sure if there's any other people who are | |
| coming in can come in. | |
| My name is Sam Coleman or Professor Sam Kaufman. | |
| I don't think I've met you yet. | |
| You may have seen me in the video. | |
| I'm not sure. | |
| I'm the head of Department of Experimental Psychology. | |
| I base is a better way along with you go. | |
| I'm the person you'll be seeing most in this course. | |
| That may or not may not be a good thing. | |
| I feel nervous today because this is the first letter | |
| I have given for about three years, so I apologise | |
| if I'm a little bit stumbling. | |
| I'll get back into the swing of it over the | |
| next few weeks, I hope. | |
| Please come in. | |
| So the aim of these two lectures today and on | |
| Friday is to give each of you make sure you're | |
| all up to about the same place and understanding a | |
| little bit about the cellular function of nerve cells and | |
| how their activity helps us to see the here, etc.. | |
| Can I just as a matter of starting point, can | |
| I ask who has done some form of biology before | |
| on neuroscience? | |
| Fantastic. | |
| Who has actually specifically done some form of neuroscience before? | |
| A few of you. | |
| So for some of you, this might be a little | |
| bit of old rope. | |
| For the next couple of lectures. | |
| I hope you'll be able to think about some things | |
| that you might not have thought about. | |
| For many of you, this might be the first introduction | |
| to neuroscience that you've had over these last couple of | |
| weeks, and I hope that you'll be able to get | |
| up to speed to where we want you to be, | |
| where we hope you'll be pretty quickly. | |
| Well, that is a really annoying door squeak, isn't it? | |
| Or just let people come in. | |
| She. | |
| I have a feeling this door is going to squeak | |
| for a while, so I'm going to have to kind | |
| of get started and try and talk over the squeak. | |
| I studied molecular biology when I was an undergraduate. | |
| Sometimes I go back and think things have changed a | |
| lot since I started. | |
| That was 25, 30 years ago. | |
| I practised as a neurophysiologist for most of my life. | |
| Sometimes it's a little bit hard for me to step | |
| back and understand what I do know and don't know | |
| what I should know and should not know. | |
| For these reasons, I'm very happy for you to interrupt | |
| and tell me you don't understand what I'm talking about, | |
| right? | |
| Sometimes it's difficult to pitch something that you know intimately | |
| to the right level. | |
| Okay, So please do interrupt. | |
| I hope that what I'm trying to do is trying | |
| in this lectures to try and keep some of the | |
| flavour of what we learn to do over the pandemic | |
| years. | |
| And and I'm going to try and be a bit | |
| more interactive towards the end of this lecture. | |
| Hopefully we'll get through in time and get through to | |
| it. | |
| I want to get I want to make sure you're | |
| all up to speed about the basic concepts. | |
| There's a lot of additional reading you could do to | |
| understand more detail. | |
| There are some fundamental things I think we need to | |
| understand about nerve cells, about brains, to understand how it | |
| is that our cognition is structured, to understand how it | |
| is that we think about things, to understand how it | |
| is that I see you when you see me. | |
| And that's the purpose of these two lectures. | |
| You might have seen this before. | |
| When I started out, as I said, training as a | |
| molecular biologist. | |
| My second year, I finally found a neurone and after | |
| about a year and a half of studying crab cycles | |
| and everything else, which I tell you, I'm not that | |
| interesting. | |
| This structure was something that really fascinated me. | |
| And this is a neurologist as a basic function of | |
| your brain, a very basic functional unit of your brain. | |
| And neurone has several defining characteristics. | |
| What I want to draw your attention to in this | |
| slide are the dendrites, these profusion of little tree like | |
| structures that come off the cell body or soma, the | |
| thermal self, which is where the DNA in the nucleus | |
| is, for example. | |
| And then the axon, which extends from the SOMA, a | |
| very specialised process and heads out towards the terminal boot. | |
| And this neurone has a bipolar kind of structure. | |
| It has inputs at the dendrites and outputs of the | |
| axon or nerve endings and the functions, the activity of | |
| these neurones, the computations that they perform which underlie all | |
| of what we do. | |
| So I'd like to start off with the central question | |
| Why do we actually have brains? | |
| When I try to ask myself this question, I come | |
| up with many different answers. | |
| And this is one I've said all along over the | |
| last few years as limit brains around the body, this | |
| collection of organs, muscles, etc., to respond to its environment | |
| and to allow plastic control of the body so something | |
| we can adapt to changes in the environment or changes | |
| in the body itself. | |
| If you think about the simplest possible nerve cell circuit | |
| that we have in our bodies, for example, the reflex | |
| circuit that allows us to withdraw our hand rapidly from | |
| a hand that is a very simple circuit. | |
| There are two sign ups as to connections between neurones | |
| involved. | |
| There is a sensory neurones that goes from the periphery | |
| or from this case, the hand goes up the spinal | |
| cord. | |
| Little things and you're on there and then there's a | |
| motor neurone that goes from the spinal cord back to | |
| the muscles that control that hand in this case. | |
| That is the simplest possible neural circuit that we have | |
| in our body. | |
| It allows us to react very quickly to something that | |
| happened in the environment. | |
| In this case, touching something hot that might cause damage | |
| to our skin or other parts of our body. | |
| It is functioning very simple and really helpful. | |
| If we wanted then elaborated by, for example, reaching out | |
| and touching something. | |
| And for me, that's what the brain does. | |
| It's a centralised way to try and control these circuits | |
| and others like them that allow us to adaptively react | |
| to our environment and to plan and to do things | |
| that we couldn't simply do with a simple two neurone | |
| circuit. | |
| The neurones in the brain allow centralised and plastic control | |
| of the body, and a simple task in these two | |
| lectures is to try and understand how it is that | |
| those neurones allow that form of control to illustrate the | |
| complexity of the issue. | |
| This is a slide. | |
| This raises some of the brains in relative scales of | |
| the species that might be studied in neuroscience, including the | |
| bottom right there, the human brain, about one and a | |
| half kilos of stuff, about 86 billion nerve cells at | |
| the top left there have highlighted a couple of other | |
| animals that are often studied mouse and rat, both rodents. | |
| A mouse, for example, has a brain about half a | |
| gram in weight, and about 71 million cells do quite | |
| a lot, but a far cry from 86 billion. | |
| And then there are other animals like marmosets and macaques, | |
| both of whom are non-human primates, and have been important | |
| models in understanding human brain function. | |
| Now, our brain is substantially bigger than those of these | |
| studied species, mainly study species, but we shouldn't get too | |
| cocky if we look at the size of the brain | |
| of an African elephant, for example, it's much bigger than | |
| ours. | |
| Now I leave it up to you to decide whether | |
| an elephant is smarter than us or not, but I | |
| simply mean that size itself doesn't really matter. | |
| The complexity and function of these brains is all enough | |
| to allow the species to adapt and survive in their | |
| environments. | |
| Now emphasise that there are 8 billion nerve cells in | |
| the brain. | |
| Neurones. | |
| But that's about equal numbers of other types of cells. | |
| These are loosely cuentas glia. | |
| And I just want to explain to you why we're | |
| not going to be talk about and talking about glia | |
| for almost the entire rest of the course. | |
| They are about half the cells in the brain, and | |
| yet we're not going to be talking about them. | |
| Why is that? | |
| So this photo or this series of photos on the | |
| right here that some guy took several years ago now | |
| obtained by a technique called photon microscopy. | |
| We'll be talking about that a little bit next week | |
| in the methods section. | |
| What I've done here is find some cells in the | |
| brain with a substance that makes them appear black in | |
| the slide. | |
| And those cells are astrocytes, a form of glia, one | |
| of these non nerve cells in the brain. | |
| These images are a series of images taken a very | |
| narrow depth about two micrometres or 2000s of a millimetre | |
| apart. | |
| Down through the brain of actually, in this case, a | |
| living rat. | |
| And you can see these different black things here. | |
| Hopefully you can see my area up there. | |
| These black things here are these astrocytes and they have | |
| these lovely processes that connect neurones. | |
| Many of these white holes, the neurones and the blood | |
| vessels, some of these larger one of the blood vessels | |
| in the brain unstained in this preparation. | |
| And can see these lovely processes connecting all these neurones | |
| and blood vessels together. | |
| So those cells are there. | |
| These are just one form of the known neuronal cells, | |
| but we don't really study them. | |
| Now there are three basic types of cells we'll come | |
| across. | |
| One is the neurones, as I said, will get to | |
| them. | |
| Most of this course, these are what we call excitable | |
| cells. | |
| And hopefully by the end of this lecture you'll understand | |
| what I mean by excitable cells. | |
| Two other very common parts of cells in the brain | |
| of the microglia, which are effectively the immune system of | |
| the brain, very important. | |
| For example, there are many diseases which seem to be | |
| basically a malfunction of the immune system of the brain | |
| of microglia. | |
| And then there's these other cells, astrocytes and other known | |
| example cells, for example, which connect these things together, which | |
| seem to provide the kind of super structure in which | |
| these nerve cells can survive and thrive. | |
| They also do other important things like maintaining what we | |
| call homeostasis. | |
| That is the amount of energy that you need for | |
| neurones to survive or the kinds of chemicals that they | |
| need to survive in the brain. | |
| The neurones are excitable and they can send signals over | |
| long distances. | |
| There is no cells capable of integrating and propagating signals | |
| very, very rapidly. | |
| An action potential which we spent a large amount of | |
| this lecture going takes about one millisecond or one thousandths | |
| of a second to occur. | |
| Those action potentials can travel sometimes up two metres down | |
| the axons neurone sends. | |
| These neurones have distinct zones as illustrated before for input | |
| the dendrites and output the axon terminals. | |
| That directional flow of input output allows them to do | |
| computations to take some summation of the inputs, compute and | |
| send a single output. | |
| Neurones also therefore formed these what were called hierarchal networks. | |
| Computations done at one stage of neural processing are then | |
| sent by the axons in the form of action potentials | |
| to the next stage of neurone processing. | |
| And we build up these successive representations, much like we | |
| do in computer models of the brain where we try | |
| to build. | |
| If you're familiar with kinds of nets that Google uses | |
| to do image recognition, for example, these are successive hierarchical | |
| representations of the image, and they're based actually on brain | |
| function, our understanding of the visual system in particular. | |
| On the other hand, astrocytes are not excitable cells, so | |
| they tend to have slow signals, their signals not formed | |
| in the order of one millisecond, but rather on the | |
| order of 3 to 5 seconds, slowly fluctuate much slower | |
| than we think. | |
| The normal perception of cognitive events or perception, you are | |
| able to type much faster than that. | |
| Astrocytes also connect to each other via various things called | |
| gap junctions. | |
| It's a little holes in the membrane between the way | |
| the membranes with true cells meet. | |
| Allows electrical current to flow through these membranes. | |
| So those astrocytes that you saw in those beautiful pictures | |
| from the rat cortex are actually one large network. | |
| We call this a synthetic network. | |
| And those that network, the activity, that network very slowly | |
| over time and space, again, incommensurate with what we think | |
| cognitive events are like, which are precise, rapid and very | |
| particular events. | |
| So for these reasons, we do not think the glia | |
| are important for the particular structure of cognition that you | |
| have. | |
| They are almost certainly very important for maintaining the neural | |
| signals. | |
| Failure in astrocytes and other forms of glia can lead | |
| to neural malfunction and disordered activity of neurones. | |
| But we don't think that the activity of those cells | |
| that are important for the kind of cognitive events that | |
| we experience. | |
| Instead, we think those are the job of the nerve | |
| cells, those 86 billion nerve cells in your brain, not | |
| the 86 billion other cells. | |
| I, as I've said, carry on. | |
| Euroclear clears word for glue. | |
| You can tell what the unanimous thought of them when | |
| they made up that name. | |
| I thought provide physical support that actually struck to the | |
| brain to remove debris and vacuum cleaners, basically provide immune | |
| function, work out when things go wrong. | |
| They also provide things called myelin while sheath, which we'll | |
| get to in the second, which help nerve cells communicate | |
| to each other. | |
| No particular cell types are called Oligodendrocytes. | |
| And they relative in the peripheral system out there and | |
| the arms are called formed cells also make myelin. | |
| Now, I've mentioned that astrocytes help maintain homeostasis, and I've | |
| shown you in those pictures that the blood vessels and | |
| the neurones are connected by these networks of astrocytes. | |
| And actually those astrocytes are doing two basic functions, at | |
| least one or two, but two that we need to | |
| think about. | |
| One is they actually help communicate energy levels or energy | |
| from the blood vessels, from the blood supply to those | |
| neurones, help those neurones work. | |
| And the second thing they do is actually signal to | |
| the local blood supply whether they need more energy or | |
| not. | |
| So if the local area of neurones is being very | |
| active, the energy supply like a fabulous. | |
| I think it's gone up. | |
| It didn't. | |
| See if you somewhat. | |
| Is this one working? | |
| So these astrocytes help communicate to the blood vessels that | |
| they need more energy. | |
| And when that happens, those blood vessels expand, they dilate, | |
| the blood flow to that area increases, and the energy | |
| to that local area increases supply. | |
| As important for understanding, for example, the bold signal with | |
| the blood oxygen level dependent signal that you see in | |
| the AFM range. | |
| That is a change effectively in the blood flow to | |
| particular parts of the brain that is organised by those | |
| astrocytes in response to local neuronal activity. | |
| And you can show this by, for example, using this | |
| technique, like I said, called to photon microscopy to stimulate | |
| the little processes of those astrocytes surrounding blood vessels. | |
| When you do that, you see the blood vessels increase | |
| in diameter, allowing more blood, more nutrients to get to | |
| local area. | |
| So they help these astrocytes help brains maintain local energy | |
| homeostasis. | |
| The oligodendrocytes that I mentioned. | |
| These helped make the myelin sheets, these little fatty liberty | |
| things that surround the axons. | |
| And we'll get to the importance of that in a | |
| second. | |
| You can see them here. | |
| These myelin sheath, they are interrupted. | |
| They're not the entire acts neurone toppled by little slices | |
| of exposed membrane organised around here. | |
| And you can see that these oligodendrocytes make these little | |
| seeds. | |
| One oligodendrocyte may be making seeds for many different axons. | |
| Similarly, in this one person in the periphery. | |
| Important is low seats are very important, as we'll see | |
| in the second disorders of the root of many of | |
| the disruptive brain diseases that we know. | |
| For example, multiple sclerosis is a demyelination disease, removing the | |
| myelin from the axons. | |
| Why would that be important? | |
| We'll try to find that out in a couple of | |
| slides time. | |
| So I'm taking you through them the basic function of | |
| several of those non neuronal cells. | |
| Just to illustrate to you that they are important. | |
| There's a reason that 6 billion in the brain. | |
| I hope the photo to why we're not going to | |
| study them, why we think that the neurones which can | |
| provide these very rapid hierarchically organised signals are the ones | |
| that are important for the structure of thoughts, perception, cognition. | |
| And that is the last, I would say, almost certainly | |
| of glial cells in the next ten weeks. | |
| So I illustrated you before I sent it to you, | |
| by the way. | |
| Now, I'm going to interrupt these things into a little | |
| section that will become clearer if we go on. | |
| This might be a bit of time for us to | |
| understand whether or not it went to some issues with | |
| talked about so far. | |
| Are there any questions you'd like to resolved in the | |
| meantime off the back of your own? | |
| Sorry. | |
| You have to speak up a little bit is. | |
| Really happens here. | |
| Sorry. | |
| Let me just come up closer. | |
| And is. | |
| It's a very good question. | |
| I'm not going to go into it because there's actually | |
| several things wrong with that slide. | |
| And it does make me want to just make clear | |
| there are some small white lies I'm going to tell | |
| you over the next lecture. | |
| Bear with me. | |
| Including that one. | |
| Okay. | |
| Bear with me. | |
| It's to help us all understand the basic issue of | |
| energy supply, for example, not the particular aspects of the | |
| cycles that they go through. | |
| So I understand the question. | |
| I just don't want to try and make it too | |
| complicated at the moment. | |
| There are a couple of white lines here. | |
| I hope that neither of them make it problem. | |
| Why are they metabolising lactate, not glucose that was there? | |
| I think that was the question. | |
| There's an answer to that, but I think it's beyond | |
| what we need one after this typical lecture. | |
| Okay, I'll just move on to the next week, which | |
| is the neurones are excitable cells. | |
| So why is it important to understand new signal transmission? | |
| Maybe this is like, Well, duh, but I just want | |
| to try and convince you that it's actually an important | |
| thing. | |
| I've stated already that the function of the brain and | |
| the nervous system in general is to receive, transmit and | |
| process signals. | |
| This is what it does. | |
| So to understand how the brain works, we need to | |
| understand how it transmits processes. | |
| Those signals is no point otherwise. | |
| And if further, if we understood how the brain does | |
| this, this would allow us to do things like understand | |
| how little anaesthetics work. | |
| Who here has had a local anaesthetic before? | |
| Anyone. | |
| They wanna know what a local anaesthetic is. | |
| Little you might rap on something. | |
| Injections you've got. | |
| I have to get these things called basal cell carcinoma | |
| for my face every so often. | |
| I grew up in Australia. | |
| It's terrible. | |
| I get so many injections of local anaesthetic in my | |
| face. | |
| Hate me. | |
| Has anyone else had anaesthetic injections? | |
| What are they? | |
| What do they help? | |
| You do not feel pain or anything or anything. | |
| Is that where he said that or anything? | |
| Not feel anything? | |
| Exactly. | |
| Actually, it's a really strange sensation. | |
| And it's like a an absence of anything. | |
| Not actually a presence or some or lack of in | |
| something. | |
| And hopefully we'll understand why they work in a second. | |
| They hope this knowledge would also help us understand how | |
| anti-depressants work, how drugs affect the brain, how diseases like | |
| multiple sclerosis and Alzheimer's disease damage the brain, and why | |
| they cause the symptoms they do, as well as these | |
| aspects of cognition. | |
| I want to make clear to you that I think | |
| that understanding how nerve cells processing was actually at the | |
| core of all of brain and behaviour, all of psychology, | |
| for example, because without that understanding it's very difficult to | |
| know what it is we are trying to explain. | |
| So this is going to be a bit of another | |
| white lie, but just bear with me about this again, | |
| helps us understand, I hope, the kind of signals we'll | |
| be talking about. | |
| So in the old days, by the old days, I | |
| mean probably starting the beginning of last century. | |
| This is how most of neurophysiology, the physiology of nerve | |
| cells was conducted. | |
| A large squid would be captured. | |
| It's giant Exxon, which is huge, much larger than any | |
| of your icons, is excised and put into a bath | |
| of saltwater seawater. | |
| A couple of fine glass electrodes are pooled on some | |
| machine which can pull them. | |
| These electrodes have small tips filled again with another salty | |
| solution. | |
| And we generally take two of those electrodes or at | |
| least one of those bathymetry and something else like a | |
| piece of wire. | |
| We put the wire in the salt bath and put | |
| the electrode into the axon and you can record the | |
| difference in electrical potential between these two things. | |
| And that's what's recorded on something like a little camera. | |
| So this photometry is recording the difference between the inside | |
| and the outside of the cell. | |
| In this case, the axon of that cell. | |
| That whole time, too, was very much like a light | |
| lotus when you attach it to the both ends of | |
| the battery. | |
| Potential difference of process to enter the battery causes current | |
| flow and the like per well. | |
| So we're going to do something similar to that with | |
| electrical device. | |
| This is the only bit of chemistry you need to | |
| know. | |
| From my perspective. | |
| I don't. | |
| Who here knows what an island is? | |
| We all remember back to those dark organic chemistry days, | |
| but some little bit like ions, atoms and molecules that | |
| have lost or gained one or more electrons. | |
| So an iron is positively charged. | |
| What we call the cation is one that's lost an | |
| electron, for example, a sodium atom. | |
| And a sodium has this one little poor electron wandering | |
| around on this outer shell. | |
| If it loses that electron, it becomes positively charged with | |
| electrons themselves and negatively charged it lose. | |
| The electron becomes positively charged, and we denote this item | |
| now as having an A plus plus relative charge. | |
| Similarly, if a atom gained electron would become negatively charged | |
| if the sample chloride gains electron becomes negatively charged. | |
| We do know that with a little minus sign. | |
| The substances we call salts, combinations of these positively and | |
| negatively charged molecules ions. | |
| So, for example, table salt, the stuff that we eat | |
| is a combination of sodium chloride. | |
| When you put into water, those two ions can dissipate | |
| and move around freely. | |
| Coming in sodium, potassium chloride minus. | |
| And the body is basically 80% water. | |
| So you can imagine the pool of ions floating around | |
| in there, including the brain. | |
| Okay. | |
| The next bit of that is, I think, over chemistry. | |
| We're going to have to know. | |
| The next bit is just to try and get you | |
| through some terminology that we're going to use as well. | |
| Way to think about cells. | |
| I sometimes find that we talk about self and then | |
| don't really think about what they are. | |
| So this is a sale, or at least if I | |
| had a blackboard, I would put it that this is | |
| a cell. | |
| What's distinctive about this thing? | |
| Anyone with a. | |
| Tell me. | |
| Or the. | |
| Wants to think about that. | |
| It's a regular. | |
| Thing. | |
| Regular. | |
| They will ignore that for the moment. | |
| What else is there? | |
| It's not so long. | |
| It's got a cell wall or a membrane. | |
| Exactly. | |
| It's got an inside and outside. | |
| It's basically a bag of stuff. | |
| Right. | |
| That membrane or cell wall, whatever you want to call | |
| it, which is a bunch of fats. | |
| Sometimes phospholipid is a little formula bag in which you | |
| stick stuff. | |
| And those phospholipids are really tightly bound and don't allow | |
| things to move across the membrane fairly impermeable to a | |
| lot of the things you think are important. | |
| So this bag means there's an intra or within cell | |
| and extra or outside cell space, three different spaces for | |
| two different things. | |
| And inside the cell is what we're kind of concerned | |
| about. | |
| Although to understand what's happening inside the cell, we have | |
| kind of also understand what's happening outside the shell. | |
| It's that's itself just a bag of spice. | |
| A bag of stuff includes the nucleus, includes, you know, | |
| the DNA and gene stuff and proteins and things like | |
| that. | |
| But in the end, it's a bag, this bag formed | |
| by cell membrane. | |
| The next thing is the science. | |
| A little bit of chemistry are not all in the | |
| same place. | |
| So, for example, throw mines which are described mainly outside | |
| the neurones in the extracellular space. | |
| Potassium, which is tonight confusingly with this K is mainly | |
| inside the cell. | |
| And calcium, which has two parts because it's lost to | |
| electrons, is also mainly outside the cell. | |
| Or the negative ions or anions. | |
| There's two different types we're concerned with generally. | |
| One is chloride, which is kind of an extra electron | |
| that's mainly outside the cell, and the other are proteins | |
| themselves. | |
| That's stuff that makes up our cellular machinery also usually | |
| in charge, and that's mainly inside the cell to do | |
| with the cell. | |
| So if we look at the cells or a few | |
| cells here, we would see that there are some anions | |
| and potassium ions within the cell. | |
| And then there's a bunch of calcium chloride and sodium | |
| floating around outside of. | |
| And so these different locations, special locations that these islands | |
| are really important because basically there's a gradient between the | |
| inside on the outside of the cells for the concentration | |
| of those ions. | |
| More potassium inside, more sodium outside. | |
| Those gradients of concentration set up. | |
| What are cold set up are the basis of the | |
| electrical potentials that we see in nerve cells. | |
| Now, if we go back to how we measure the | |
| activity of nerve cells of the electorate inside and outside | |
| of the cell. | |
| We find that actually, generally speaking, in fact, almost always | |
| these nerve cells are what we call negatively charged. | |
| They have a resting membrane potential that is in the | |
| absence of anything else of about -70 millivolts. | |
| Minus 70,000th of a vote. | |
| They don't seem like much, but it's a lot. | |
| It's enough. | |
| That negative potential. | |
| The difference between the insight into so and so the | |
| space is the basis for all of new single use | |
| signalling. | |
| And this the statement here is this show is polarised | |
| and it doesn't have the same inside and outside. | |
| So if the potential difference gets smaller, i.e. goes towards | |
| zero, so it gets to 60, we say the will | |
| be polarised, less polarisation. | |
| If it gets more polarised, it gets further way from | |
| zero, like the -80 with a hyper polarised, more polarisation. | |
| So this resting membrane potential, which I've argued, which I | |
| will argue is the basis of all our brain function, | |
| is actually the largest single sink of energy in the | |
| body. | |
| Most of the energy that your brain uses in your | |
| brain uses most the energy in your body towards keeping | |
| this resting resting memory potential at about -70 millivolts. | |
| So again, if we put the electrode from outside into | |
| the axon that we were seeing before, you see the | |
| potential go from 0 to 60 miles, 70 millivolts. | |
| The difference between the inside and the outside of the | |
| cell. | |
| As I explained, to try to explain, I encourage you | |
| to read about this. | |
| Way too many books on this many articles. | |
| You can have a thank you in much clearer way | |
| than I'm trying to do it now. | |
| This potential the rest of member States was a result | |
| of the difference in the ionic concentrations. | |
| So for example, sodium is more common outside the sodium | |
| inside itself. | |
| Potassium is more common inside the cells phone outside the | |
| cell. | |
| And the fact that that membrane so membrane, the fact | |
| that this is a cell is largely permeable to a | |
| lot of these ions. | |
| By impermeable I mean that those ions cannot easily cross. | |
| If I could easily cross half the sodium, we're going | |
| to be the inside of the outside the cell. | |
| And if there was no difference between the inside the | |
| outside. | |
| So the concentration of those ions, there would be no | |
| membrane potential. | |
| So the fact that this membrane, this bag is largely | |
| impermeable to ions is what allows the cell to set | |
| up this potential difference between the inside and outside the | |
| resting membrane potential. | |
| And then what you need is little things in those | |
| membranes, little holes, little pores that you can open and | |
| close to allow ions to flex across. | |
| Once you've made this bag, you then have to put | |
| new pinpricks in it and have it be controllable or | |
| something. | |
| And once you got those three things, the ability to | |
| control the flux lines across the membrane and this difference | |
| between the similar concentration and extracellular content of those items, | |
| you can make a cell. | |
| And they can help us so communicate. | |
| There is a little pump movie which has a on | |
| on the middle side, which I like to look at, | |
| which has an interesting take on this. | |
| I encourage you to look out when I say this. | |
| I mean what I was about for it. | |
| So I've already said the potential requires energy and is | |
| actually responsible most of the brain's energy consumption. | |
| And the reason for that is that there is this | |
| one particular set of proteins sitting in the cell membrane | |
| called the sodium potassium pump. | |
| So I described that there's a difference in interstellar concentration | |
| of ions that doesn't just arrive by chance. | |
| These loop pumps sitting in the membrane, exchanging, constantly changing. | |
| 330 miles took them out, bringing through potassium mines, putting | |
| in. | |
| Thereby setting up these concentration gradients across the cell membrane. | |
| This little thing. | |
| This little thing uses adenosine triphosphate, which is the body's | |
| major source of energy. | |
| And it's consistently reactive. | |
| It's always growing. | |
| And that's why the rest of my body was sitting | |
| at 1780 volts. | |
| If it fails, you die. | |
| Having this resting membrane potential allows you to then form | |
| action potential. | |
| This slide looks a little bit complicated. | |
| Very straightforward. | |
| So let's go through if you haven't seen this before, | |
| but it is really straightforward. | |
| We've discussed there's a resting membrane potential about -70 millivolts. | |
| And I've discussed that. | |
| That's not very. | |
| Imagine that there is a little input within you on | |
| the cause of that resting membrane potential to deviate a | |
| little bit. | |
| Go towards zero depolarise. | |
| This little. | |
| Sometimes I just love it. | |
| Yeah, because sometimes it is a critical point that mine | |
| is 6365 millivolts. | |
| At which. | |
| What are called voltage gating. | |
| Gated sodium channels are opened. | |
| Now that voltage gated means a particular voltage potential difference. | |
| At which these channels are open. | |
| Otherwise, they closed the when they closed the bags to | |
| the bag with the bag suddenly permeable to throw mines. | |
| Over 30 mines have been sitting outside for sale. | |
| You open this lock. | |
| Suddenly they can go into the cell. | |
| You have a bunch of positively charged demands and flexing | |
| to sell very rapidly. | |
| There are thousands of these channels in the membrane. | |
| Millions of. | |
| All these 30 mines really rapidly rush into the cell, | |
| overwhelming everything else, all that positive charge that comes with | |
| them depolarise it even further. | |
| So you can see here, which is route threshold, a | |
| threshold is open these channels that allows the sodium to | |
| come in and suddenly the cell's potential difference changes dramatically. | |
| It goes back to there and often overshoots because if | |
| too many of these 30 mines come in. | |
| At some point in time, those towns can close again. | |
| Oh, that's not. | |
| Then stuff allows the to return back to resting potential, | |
| in particular the influx of potassium ions. | |
| Also the active action of that 30% pump. | |
| So you have this low threshold offer which is exceeded. | |
| You have this massive in your arms and then a | |
| relaxation back to the basic steady state. | |
| And that is an actual potential. | |
| That's all it is. | |
| Basically, it's transient in Russia, 30 miles. | |
| It's just been get switched on. | |
| Very simple. | |
| But incredibly important because this is what we mean by | |
| this has been excitable. | |
| So if you can and you can make them. | |
| Produce listings. | |
| Does anyone know what the other major example? | |
| Selling bodies. | |
| My muscle cells. | |
| Yeah, muscle cells. | |
| So muscle cells contract because of a very similar flux | |
| of ions based on calcium in this case. | |
| So that movement of muscles, which I've never had, actually | |
| the filaments all work together, driven by this transient change | |
| in the calcium and potential calcium fox. | |
| The brain cells are very much like that, except faster | |
| and different ions. | |
| And different connections. | |
| Clearly they don't move. | |
| I mean, there's a lot of differences between. | |
| By the way, those voltage sodium channels will be blocked | |
| by something called tetrodotoxin or ctcs, often abbreviated because no | |
| one can actually save it for the toxin. | |
| I have to practice for 5 minutes before coming. | |
| You say Dax's neurotoxins about 1000 times more potent than | |
| cyanide. | |
| It blocks those voltage settings. | |
| Of course, if you block this into account for maximum | |
| potential, if you can't perform actual controls, you can't move | |
| your muscles, including your diaphragm. | |
| You can't breathe. | |
| You know. | |
| So that's why Fuku or Pufferfish has been prepared so | |
| carefully, because actually those fish are large source of so. | |
| If you prepare them incorrectly, you'll consume a little bit | |
| of that. | |
| And that's enough to stop your breathing and make it | |
| on. | |
| Blocking the voltage gate to certain terminals is also how | |
| local anaesthetics were very similar. | |
| They stop. | |
| Therefore the sensations from that part of your body. | |
| We have an injection in your arm, for example. | |
| You feel strange absence of sensation as from there, because | |
| the sensory neurones which rely on these certain channels are | |
| not sending the signals anymore. | |
| Now, this what? | |
| Angular? | |
| Slightly different. | |
| So painkillers generally, a lot of painkillers are based on | |
| morphine analogues. | |
| And morphine analogues. | |
| Opioid receptors for morphine, as we've discussed, actually makes it | |
| terrific targets opioid receptors that opioid receptors are really important | |
| to controlling breathing, but they're not actually important in the | |
| regulation of. | |
| As a generation. | |
| Yeah. | |
| Yeah. | |
| What? | |
| Isn't it? | |
| Yeah, well, technology is much more powerful than any local | |
| anaesthetic. | |
| Use The local anaesthetic has been designed to kind of | |
| only work in that slight place. | |
| Referred to a toxin. | |
| Generally speaking, it's consumed and therefore systemically, rather than just | |
| being consumed. | |
| At some point it's very apparent. | |
| Yes, you shouldn't treat like McCain or other local anaesthetics, | |
| like they're being perfectly designed to actually overcome these issues. | |
| They just work in a kind of similar way. | |
| Local versus. | |
| Yeah. | |
| What? | |
| They get cleared out and diluted effectively by the system. | |
| Any other questions? | |
| The. | |
| Just take time. | |
| Okay. | |
| I was going to do this interactive thing, which I | |
| think I've got to wait till next lecture because this | |
| is reminding me how long lectures actually take action potentials | |
| move along that move to the sciences and that little | |
| action potential. | |
| They've been describing all that process, initialisation that takes place | |
| in a place called the Action Hillock. | |
| This is the bit where the action beach itself, on | |
| a blue and a V-shaped thing will be incredibly special | |
| specialised be the membrane. | |
| Recent work by some colleagues in the Netherlands have shown | |
| that the density of the sodium channels is only 37 | |
| channels in the axon hill. | |
| It is ten 100 fold greater than anywhere else in | |
| the neurone. | |
| They really important for generating the action potential. | |
| But once the action generated, why is it? | |
| How does it work? | |
| You've got this accent, which is maybe a metre long. | |
| You've got this little bit of membrane potential happening, this | |
| little bit of membrane just where the accent meets the | |
| sun. | |
| For neurones, a signal that explains how to leave the | |
| Soma and get to the end of the axon. | |
| And it does that by a very simple process, which | |
| is basically regeneration. | |
| So if you get an affinity for forming this little | |
| bit of the membrane here. | |
| In the neighbouring little bit of membrane has a little | |
| bit of a deflection. | |
| Depolarisation. | |
| And then that starts the cycle of the action potential | |
| again. | |
| That neighbouring bit of membrane that happens here and and | |
| happens here, it's turning off. | |
| It happens here. | |
| It happens to propagates down the axon. | |
| If you think about it carefully, can imagine it can | |
| happen both ways. | |
| That is actually the case, actually potentially can go from | |
| not only into the action, but also the dendrite. | |
| It's a very deconstructive that's on the table. | |
| That means that that's the way we think the signal | |
| progresses. | |
| Little regenerating action potential. | |
| Somehow manages to depolarise this little bit of membrane and | |
| move along that membrane. | |
| What an amazing thing that we evolved. | |
| Now, if you just left it to his own device | |
| to travel down that piece of membrane, probably through about | |
| a metre a second, some general speed for a potential | |
| move down a bit of an. | |
| And insulated membrane. | |
| That's a bit slow. | |
| One second. | |
| You know something? | |
| Hit me. | |
| Like. | |
| So a lot of the major axons in the body | |
| and some of the direct forms in the brain are | |
| in chief. | |
| Myelin with myelin is basically just like wrapping insulating tape | |
| around the acronym. | |
| Stop the actual potential for really from generating at that | |
| point and instead allows maximum potential from this position to | |
| jump across the next note of review. | |
| And so instead of just slowly moving along, it takes | |
| massive, long strides down the axon. | |
| It can speed up transmission tenfold, at least. | |
| Yeah. | |
| Is it likely that people like the signal won't reach | |
| from one? | |
| Like some of the others. | |
| So that's the danger, right? | |
| The mine was too long. | |
| So the question was, isn't there a danger that the | |
| little depolarisation here doesn't reach the next note? | |
| I think of what you are. | |
| And so clearly that's a danger. | |
| So that bit of myelin can't be too long. | |
| Yeah, there has to be critical distance between the two | |
| nodes above which we just to the actual would not | |
| propagate. | |
| At the moment. | |
| She's really important in speeding up production in Europe. | |
| Okay. | |
| I'm going to have to move along. | |
| So we'll just keep by the way, at the end, | |
| later. | |
| I think we're meant to leave this door and I | |
| will wait out there if you have additional questions for | |
| me so that people can come in once we're doing | |
| now. | |
| This is how I think an action potentially works. | |
| Music, all the dinosaurs. | |
| I think anyone ever tried to do this at home. | |
| Right. | |
| Good old school. | |
| Yes. | |
| Okay. | |
| Now, why am I using this analogy? | |
| I made the point before because it was quite impressive | |
| one. | |
| I like to think of that can pretend to be | |
| an asleep and then it gets to some point and | |
| triggers the ball ball moving towards the pocket. | |
| Right. | |
| By the way, this keeps going. | |
| I think this entire video is actually. | |
| What's that. | |
| Is the ball you're. | |
| Tracking? | |
| Yeah. | |
| We'll get there in a second. | |
| So the ball. | |
| The ball, Yes. | |
| Is a basically neurotransmitter. | |
| The pocket is supposed to be cleft. | |
| Let's see if we can understand those statements. | |
| Pretty impressive. | |
| I mean, I'm glad they caught on video. | |
| You can imagine. | |
| So we'll get to that right now. | |
| So bear that in mind. | |
| That's how I think of neurones. | |
| Okay. | |
| So each of these acts on this axon is a | |
| single axon, but it sprouts. | |
| Multiple contacts with the same and about thousand on average, | |
| I think. | |
| Multiple contacts, multiple output points. | |
| So what's happening in each of those Apple points? | |
| That's the question. | |
| So this is a couple of schematics which try to | |
| illustrate to you what it looks like. | |
| Each of these outputs in this case is what we | |
| would call an access somatic finance assignment between the Exxon | |
| and the Soma. | |
| You can also have accident reading between acts on the | |
| dendrite. | |
| This is actually somatic signups. | |
| So if you look on the left, you have this | |
| line at the end of the tunnel, good on the | |
| axon coming to the cell. | |
| We look in there. | |
| This is what it looks like, the green thing here. | |
| That's the sign at the end of the axon. | |
| And over here, that's the post traffic sign personality. | |
| So after the sign ups. | |
| The sign up is actually this whole thing together, the | |
| presynaptic, postsynaptic. | |
| And in between this thing we call the synaptic cleft. | |
| About 20 nanometres in size. | |
| Really? | |
| Really. | |
| Molecules can actually diffuse across that little cleft. | |
| And quite rapidly less than a millisecond. | |
| So if an accent comes down. | |
| That's right. | |
| I can take what comes down this axon. | |
| It enters this sinus presynaptic space. | |
| When it does that, it actually causes the influx of | |
| calcium ions. | |
| Don't worry too much about that. | |
| The presence of calcium. | |
| Causes these little bags, which we're going to call critical. | |
| Wilbanks Within bags or bags? | |
| Within bags, through bags to move towards a membrane presynaptic | |
| membrane. | |
| So this bag contains a little bunch of neurotransmitters, a | |
| particular chemical. | |
| That bag growth was a membrane binds with the membrane. | |
| Cause a little gap in the membrane to open up | |
| the bags of neurotransmitter. | |
| So the neurotransmitter then crosses into the sign of a | |
| cleft. | |
| What is in the Senate declared didn't go anywhere. | |
| But a lot of it goes to the other side | |
| of the cliff and on the other side of the | |
| Senate to propose an epic membrane of things we call | |
| neurotransmitter receptors. | |
| The proteins within the person. | |
| I pick my brain, which are designed to receive these | |
| neurotransmitter signals. | |
| Yeah, I do. | |
| So not supposed to be able to do drugs. | |
| Good question. | |
| I don't know the answer to that. | |
| Look it up. | |
| I mean, this is not a passive process. | |
| There's an active process here. | |
| I'm not exactly sure how to go about coming from | |
| it. | |
| It's a good question. | |
| If we look at the electron microscope picture, this is | |
| a real Darnold schematic. | |
| On the left is a high as a relatively high | |
| power. | |
| This sort of a sign ups in this case is | |
| connected and really connects to the dendrite and the axon. | |
| You can see all these little bags. | |
| These this is what we call a postsynaptic density. | |
| That's a that's the way you can recognise these sign | |
| with an electron microscope. | |
| And there's these bags that kind of near this. | |
| And we looked at this and even more detail we'd | |
| see here these bags, some of which are binding with | |
| the membrane, allowing the neurotransmitters to enter synaptic cleft. | |
| What happens when a neurotransmitter enters unhappy cleft? | |
| On the other side, you have these neurotransmitter receptors. | |
| Each of these are designed to be sensitive to one | |
| or very small number of molecules. | |
| When that molecule wanders across the crest of bonds, this | |
| protein that spans the postsynaptic membrane. | |
| That protein undergoes what we call inflammation, trying to change | |
| the shape. | |
| When it changes shape, it creates a pour in the | |
| membrane, when it creates that pore in the membrane. | |
| IONS In fact, through the membrane. | |
| So, for example, glutamate, which we call an exaggerated neurotransmitter, | |
| a lot of its receptors which bind glutamate, open up, | |
| allow sodium lines to flex across the membrane for 30 | |
| lines, are positively charged. | |
| That polarises the person. | |
| I think so. | |
| Gabba. | |
| Gabba Gabba Gabba is an inhibitory neurotransmitter because its receptors, | |
| generally speaking, open up a loophole that allows corridor lines | |
| to cross the membrane of Florida ions and negatively charged | |
| that are hyper polarised so they inhibit activity. | |
| Deconstruction of these receptors might be sensitive to a particular | |
| type of neurotransmitter and allow particular type of ion to | |
| cross the membrane. | |
| These are called iron or tropic receptors because they directly | |
| flex the lines of the membrane in the neurotransmitter. | |
| There are another class of neurotransmitter receptors which we will | |
| encounter in the next lecture called metabolic Tropic. | |
| They rely on post processes inside the postsynaptic cell that | |
| in turn called the flux lines. | |
| I don't really open pore in the membrane. | |
| I just want to spend 2 minutes playing them. | |
| Why? | |
| These are important. | |
| If you imagine glutamate and GABA, imagine a neurone here | |
| which has three sign ups, two green, one red green | |
| sign ups as we're going to call glutamatergic sinuses. | |
| That is glutamate is released to the presynaptic space causes | |
| the membrane synaptic membrane. | |
| The other sign ups is a inhibitory neurone. | |
| It's a sign. | |
| It uses GABA release from release from prison up in | |
| space. | |
| Causes a cleft or the postsynaptic membrane. | |
| So this neurone has two glutamatergic finances and one refinance. | |
| As I said before, government allows positive ions into the | |
| next year. | |
| So they polarises. | |
| The person I think you're on is that it allows | |
| negative ions. | |
| I almost imagine the sequence of events over several milliseconds | |
| here. | |
| Whereby one of those finances is active, government finances is | |
| active and therefore allows a small excited person, active potential | |
| dps p small depolarisation away from the rest and the | |
| potential towards the threshold for activation of certain channels. | |
| Now that may not be sufficient to reach that threshold, | |
| but if you have the two sign ups as active, | |
| then you might increase that threshold allowing that neurone to | |
| generate an action potential. | |
| On the other hand, for example, inhibitory signups, since everyone | |
| here would continue on to operate away from the resting | |
| potential, or if you activate that inhibitory sign at the | |
| same time as to group protected classes, effectively cancel out | |
| one of those two glutamatergic sign ups, therefore stopping the | |
| neurone from firing. | |
| So these little neurotransmitter receptors in these different sinuses allow | |
| this neurone to compute. | |
| If it crosses the threshold, the signal crossed threshold for | |
| an action potentially only crosses the threshold if the neurones | |
| input in have enough inputs. | |
| And that exactly input outweighs the inhibitory input. | |
| There is a simple algebraic computations. | |
| He says what in your and does? | |
| It sums to hundreds and thousands of inputs that it | |
| gets to ten drives to produce a single number of | |
| the axon hillock which says Am I above or below | |
| the threshold for generating maximum potential? | |
| And then sends that signal number one or zero down | |
| to the axon terminals. | |
| That is the fundamental computation of frame systems is what | |
| allows us to see allows us to think of what | |
| allows us to hear, for example. | |
| And that is the fundamental point I want you to | |
| take away from this lecture. | |
| All little chemical transmitters, etc. allow these neurones to perform | |
| simple functions to some eight inputs. | |
| But those when you cross those functions, make them hierarchical, | |
| as we'll discover in the later lectures. | |
| You can now build into that. | |
| Interesting. | |
| But it all relies on this very simple process. | |
| One last question. | |
| What decides what your interests? | |
| That's a great question and we'll get back to that | |
| in the next lecture, actually. | |
| So the question is, which neurotransmitter has been expressed by | |
| the presynaptic, Kiran, that makes it exciting or inhibitory? | |
| And the answer to that is very complicated and has | |
| to do with evolution and genetics and everything else. | |
| But it will get back to the major point that | |
| one expects. | |
| All right. | |
| Thanks, everyone. | |
| If you can leave by this time. | |
| You. | |
| I now feel less nervous. | |
| It's a great warming up at the believe through here. | |
| I'll wait out there if you have any questions as | |
| well. | |
| Thanks. | |
| Yeah. | |
| I just want to be very aware of the network. | |
| Right outside of the other. | |
| Networks. | |
| Thanks. | |
| So. | |
| Yeah. | |
| I'll be out there and checking out. | |
| What is. | |
| If we had questions, if we just wait outside for | |
| the people to come in and we'll be out there | |
| and giving. | |
| All right. | |
| Those questions. | |
| Do we just wait out? | |
| Oh. | |
| Humphrey with the math right now, I. | |
| We see it in the summer. | |
| But yes, I've. | |
| Yes. | |
| It'd be great to chat with you guys. | |
| I think they're going to try to. | |
| I forgot how long it takes. | |
| I have this whole exercise. | |
| If you can actually help me out. | |
| I didn't like. | |
| Yeah. | |
| You can just follow me outside, then. | |
| That's fine. | |
| No, I'm sorry. | |
| Let me just check to make sure. | |
| Think. | |
| Okay. |