VideoPoints

••• •• •••••
BIOL 2320_Microbiology for Non-Science Majors - 10_27_22_Lecture
Help Tour
© Distribution of this video is restricted by its owner
Transcript ×
Auto highlight
Font-size
00:21 Ok folks, let's get started Um 14 we only have a couple
00:33 five plants from that. So then . So 1617 immune system.
00:43 I'm gonna start the immune system a minutes. So that will go on
00:50 next week and then on to So back to weekly quizzes um
01:00 Uh So just be aware of that up due on monday. So uh
01:07 . O. Exam two was opened yesterday so I forgot to mention that
01:11 today's email. So uh do take look at it. You got
01:15 Uh let me know but give yourself chance to go through it, see
01:19 you can go through the questions. may just see if you can figure
01:22 out. If not I'll certainly let uh let me know. Okay.
01:28 Let's see. So our exam is for another three weeks yet but the
01:36 er for that will open next friday that exam. Okay so um
01:44 rapidly approaching the end here. Okay Let's look at so again as I
01:57 several times already, 14 is a of terms. Right? So you've
02:01 a a list here. I just literally just went to the slides and
02:08 just put them and group them all . Okay? So uh so this
02:13 really just writing these things out and remembering them. Okay. Um So
02:23 last time. Okay we talked about last very last thing we talked about
02:29 epidemiology. Right? So that's using data basically looking at data which are
02:41 regarding instance incidences of disease. and looking at it in different ways
02:48 it to, to um, maybe cause of the disease to find out
02:54 you can prevent disease. Um, to use it to, to figure
03:01 what's the source of the illness. there a particular demographic group that's more
03:07 to it? So lots of different to use the data? Um,
03:11 these are some examples here. There's ways. So what they described as
03:16 , analytical and um, uh, other one, the other one is
03:26 experimental. Okay. And grant there some overlap between these because they're all
03:30 at data. Okay. All three course are, but in um descriptive
03:36 I just realized Jon snow, you know who Jon snow is.
03:42 of Thrones. It's so that's not Jon snow obviously, although they're both
03:47 . I guess so. But mm The so he used, his
03:56 was kind of after the fact more less so color outbreak in London,
04:02 is very common thing during these times mid 1800s. I think people use
04:07 main river going through London that's kind their water source for everything both to
04:12 and dump into. Um, and water would be pumped there in various
04:17 with like a old fashioned, you not be aware of, you
04:21 back back in these days and you the water with one of these things
04:24 out of a spout in the middle the neighborhood. And that's where people
04:27 to collect water. And so just going around to these neighborhoods, he
04:32 basically looked at um death records of , People dying from cholera. And
04:38 um kind of went from house to asking okay, who who in your
04:43 had it, where were they at they became sick, these kind of
04:48 . And then kind of pieced together map of the area um in downtown
04:53 and saw a high number of cases the red arrow was at. That
04:57 traced to a particular pump and it a faulty uh contaminated or something when
05:05 changed it out to a brand new . The instances of cases went way
05:11 . But you wouldn't have known that you hadn't done this kind of these
05:15 . And so um that's what we descriptive. And so the analytical is
05:22 looking at a ton of statistical this is what Florence nightingale did.
05:28 looking at typhus, typhus is a that is really um a disease of
05:38 sanitary conditions, bad hygiene, close being together, um could be um
05:48 know, it's carried by fleas, types of fleas and ticks lice
05:54 many are carried by rodents, mice rats and things. And so um
05:59 just kind of like a fever and headache and symptoms become worse after
06:06 But it was a common in this and before this time it was very
06:11 because of course didn't have the sanitary we do nowadays in most places.
06:16 so that contributed heavily to that But she was interested in looking
06:20 you know, what is the nature this compared to our military,
06:24 Looking at military members of the military to just the average, you
06:29 civilians. Okay. And what is difference in terms of these cases of
06:34 ? And so let me flip flip real quick just to show you.
06:38 , he's just looking at this is looking at both typhus and cholera,
06:44 label that contagious diseases. She was looking at both of these, but
06:48 typhus cholera was a waterborne, you , people contaminated water. And so
06:54 course in the military, there were together at this time. You
07:00 they may not have had the best , uh, maybe not bathing
07:05 stuff like that. Um she especially for those that are just soldiers
07:11 were in England right, had a incidence and the general public.
07:16 .2 verse 18. But then we at soldiers actually in war war time
07:22 a I forget the Crimean war uh it was much higher. And so
07:28 attributed to that she attributes, she she investigated this and saw,
07:33 what's different here in this group compared these other two groups is the poor
07:39 , Right? So that's that's what immune system plus unsanitary conditions, poor
07:46 , poor um just day to day overall. And so altogether contributing to
07:52 uh these higher instances of typhus. so when she saw this and
07:57 well let's do X, Y and . To minimize these things get better
08:02 , cleanup, bathe regularly, etcetera. And of course instances go
08:09 down to 42 to 2%. Pretty . Okay. And so apparently she
08:14 had like 1000 page report with a of tons of graphs and data and
08:19 and things. That's of course that fits it. Being an analytical um
08:26 um epidemiology. Okay, experimental. kind of like uh basically taking up
08:34 experiment and a control group and in experimental group in similar ways. I
08:39 have briefly talked about this earlier, way back in the first chapter,
08:45 he instituted the use of uh antiseptics acceptance. And so in the hospital
08:53 was working at um he saw that in the hospital, the ward where
09:02 went to to give birth, that was a super high incidence of this
09:07 called childhood fever is kind of the term. Purple fever is the medical
09:13 is due to streptococcus bacterium acquired during . The baby uh can contract it
09:22 well as it can spread into the and then also affect the mother.
09:26 both mother and baby can be Um and so he said well what
09:32 what's contributing because he saw this group in the hospital that had a really
09:37 incidence of this disease and then he um you know women that didn't come
09:43 the hospital gave birth outside the hospital uh used the midwife that they outside
09:50 hospital that they were much lower instance this. And so he looked and
09:54 what's the common denominator here? Well these other groups um wash their
10:01 It was a regular practice of washing as a woman about to give
10:06 And in the hospital, the area maternity ward number women were giving
10:14 The doctors that did that were the doctors. So they would be like
10:20 2nd year medical students that would come of a uh cadaver awards. So
10:28 course as a doctor, you work cadavers to study the body and how
10:31 works and what not, they would directly from there to the maternity
10:36 Of course dirty and bloody and hands not clean and not privately. That's
10:41 what contributed to the high incidence of child bed fever. And so when
10:45 instituted said you aren't going in there you wash your hands. And so
10:50 that, I mean the numbers dramatically , much like the what we saw
10:55 uh with uh typhus, like a that's that like that very significant drop
11:02 again just washing your hands, So, um, but actually back
11:07 the day, it was a much soap to with this lye soap,
11:12 is actually very, almost like washing with bleach almost. Right? So
11:16 definitely gonna kill any bacteria likely kill of your own cells on there,
11:21 will definitely lead to this drop in number of diseases of this particular one
11:28 , referring to child bed fever. , you know, we all heard
11:33 clinical trials when the drug is on market then you test different groups,
11:38 ? Could be one gets a placebo doesn't these kind of things that all
11:43 into the the umbrella of experimental Okay, so, um, the
11:54 reporting. So I mentioned this already well. So case reporting and nationally
11:59 diseases kind of goes hand in Okay. So there are just quickly
12:05 do not memorize this table obviously. these are the nasty notifiable diseases.
12:13 what you might think, communicable obviously things like measles, mumps,
12:18 , um, uh, influenza Um, and then certainly all of
12:25 sexually transmitted diseases following this group, , and then certainly a number of
12:29 . Okay. And it's with this , of course, how you can
12:36 , see if there's an outbreak is what's going on and try to
12:40 that chain of transmission. We call . Okay, to to um,
12:44 contain the disease. So essential information have. So we can uh,
12:50 it's basically all that information is put together in this publication here.
12:58 . Which covers every infectious disease, think even non infectious diseases too.
13:05 on a weekly basis, you they track all this data if they
13:08 something that's, you know, spiking or what have you and report on
13:12 course and follow it to see it something significant. Um, you
13:18 if you're interested, you know, just google that and you can see
13:21 actual weekly reports here. But once the end of the year are kind
13:25 interesting. It's kind of a review the previous year and the it has
13:31 infectious disease and the number of cases during the year. Um, but
13:37 so with that the terms you see and mortality. Okay, So,
13:45 , I'm sure you've all heard of , obviously mortality rate. The number
13:48 deaths. Right. It's about deaths these diseases, morbidity is the symptoms
13:55 rather the instance of a specific Okay, you don't necessarily die of
14:00 . But you reported two people reported have it. It's been confirmed from
14:06 that they have the disease. whether they fall into the mortality
14:11 of course, depends if they die number than mortality, Mortality and morbidity
14:33 . That's like 100% mortality rate. get the symptoms of disease and you
14:37 . All right. So you're not to be the same. Okay.
14:42 mean, I guess it be close it was something like Ebola, but
14:46 with that it's not equal. So morbidity is gonna be higher.
14:51 You have a lot of people that down with influenza, right, contributing
14:55 the morbidity numbers. But how many gonna actually die? Much less?
15:00 gonna die than actually? Yeah. that make sense? That morbid is
15:04 to be immortality how they relate? . Um Okay, so I see
15:13 that ends 14. Okay. Any about it? Okay, so let's
15:21 so we're going to in a So two parts here innate and adaptive
15:26 immunity 17. And that 17 is of those uh you're gonna kind of
15:32 on it yourself? Right. So I think the material should be
15:38 the lecture video and stuff. So ahead and take a look at that
15:41 already. For 17. For Okay. And we'll go through that
15:45 Thursday. Okay, I'll have a of questions and kind of frame it
15:51 that. So you've seen this already times, but again, just to
15:56 we're not gonna focus on this is this really host offenses. Okay,
16:05 which of course relates to, you , do you come down with
16:08 What's your level of resistance or you're so resistant? You're more susceptible.
16:14 . Of course, that relates to your immune system obviously. Okay,
16:19 with the innate immune system, that's you come out of the, you
16:24 , come out right, you're born boom, you've got that innate immune
16:28 already working not, you know, a baby, obviously not at the
16:32 level as it will a few months years from that point, but you
16:37 have obviously skin, that's a physical , certainly part of the immune
16:41 You have mucous membranes lining your body and whatnot, That's that's part of
16:46 . Um We call the innate immune non specific. Okay, and there's
16:53 reason for that. But let's look at this question here, just to
16:57 if we can come up with something . So remember, so as we
17:01 through this, your your innate and immune system, you can look at
17:06 as 12 and three in terms of . And one way to visualize that
17:12 really if you're a if you're a out here, right, and it
17:17 to the body. Okay, what the layers it's going through?
17:22 As it penetrates deeper into your if it does. Okay, and
17:26 that's one way to look at it terms of first line, second
17:28 third line. Okay, um let's here. Um so as you're answering
17:39 , so specific versus non specific. specific the immune system is the adaptive
17:46 system. Okay, because it relies on binding of components to each other
17:57 antibody very often. So there's there's definite specificity to it because it involves
18:02 binding to an antigen. Okay and what sets in motion. All the
18:08 that follow. Okay your innate immune is not oh there is molecules binding
18:15 certain in part of the process. not all centered on that, it's
18:21 microbes coming in and you have different that they can encounter and may or
18:27 not get through but it's not as as adaptive system. Okay So let's
18:33 down here from 10. Alright. Yeah that's uh yeah it's corrected fever
18:51 is is I think more of a line of defense. Okay and so
18:57 look at um both sides of this here. Here we go. So
19:04 not specific and specific. Okay so new system falls into that category.
19:09 specific. Um So first line so I said picture microbe here is coming
19:15 what's gonna encounter first skin skin barrier if it gets into your nose or
19:21 maybe mucous membranes line your nasal Um You ingest it right? Your
19:28 membranes coat your throat and then your . And so basically a colleague of
19:35 that teaches A. And P. human fit said this gives the analogy
19:40 the body is a donut. Okay right through right? So your mouth
19:46 alright the whole right exposed to the right? But they have your fist
19:52 your guts and everything else around So of course uh what goes through
19:56 hole is what you breathe in And of course that will contain uh
20:03 with everything encounter right in the mucous as they pass through. So um
20:10 skin membranes and don't ever forget your own microbiome right there. They're part
20:17 that certainly as well. Okay now going to be somewhat redundant because um
20:25 your first line defense you can look these especially um skin and mucous membranes
20:35 as a physical barrier. Okay. they also produce a chemical barrier which
20:42 skin and mucous membranes produce chemicals and chemicals also can interact and uh counteract
20:52 that committee. So so your first of defense is both a chemical physical
20:57 chemical barriers as as you'll see um line defense. So getting past your
21:05 line then. Second line I kind characterize as cells specific cells that are
21:12 to interact with pathogens to get rid them and also processes. So I
21:17 like inflammation fever. These I call these of course are particular cell types
21:27 now. Even the processes of course cells. Okay but you when your
21:32 ways to fight infection of course is figural psychosis, literally just engulfing pathogens
21:39 breaking them up license. Okay so a number of number of cells and
21:46 processes that are part of the second of defense. And so the third
21:49 which will will get to until next from the day is your data review
21:55 . So this requires um it only activated. Okay so they respond two
22:09 what activates that system. Right? And so uh that's why we have
22:17 that's what we call it specific. you have cells in your immune system
22:22 the immune system we'll recognize antigens. um antibodies is one way production of
22:31 . You can of the thousands if millions of potential engines out there.
22:36 can likely produce antibodies to each and one of them allergies are about kind
22:47 a hyper response to certain antigens and any case the uh and so T
23:09 and B. Cells and also a other types. And we're also going
23:18 see is that there will be cell that will bridge that both sides you
23:29 cell types that both are part of adaptive and DNA. And so they
23:34 kind of connected to. So um knowing I just told you now let's
23:43 see this is a this is a response faster right. Or the
23:56 So I'm gonna have to run the on this one. Hey winding
24:29 Alright count down from four. So it's definitely gonna be an eight and
24:40 really has to do with that that to Well the energon the energy in
24:49 or response to energy which is what adaptive immune system relies on.
24:57 Um There are 2 2 things. is um identify. Okay,
25:09 Find it so to speak. And then bind it. Uh It's
25:22 be very not scientific but I'll just new stuff. Okay, I'll elaborate
25:32 that. Of course it's a lot that. But do stuff means um
25:38 identifying to recognizing, finding it There's a time element that doesn't happen
25:43 , right? Uh then bind engine then that then induces a lot of
25:51 going on inside the cell. making different types of molecules etcetera
25:56 And then um that that then leads so they do stuff is then does
26:02 believe or sell itself buys an engine then stuff happens. Right, More
26:07 happens. So it's uh for now is this is why we'll get the
26:13 and bolts next week. But um yeah, this all takes time.
26:19 of course the native resources right Right. It's a better it stops
26:25 so again, put the kind of terms in this chapter together here.
26:34 we get I broke it down and of chemical defenses, physical barriers,
26:38 mucous membranes, right? Um Different types we see here. Okay.
26:47 Another cell type here that the immune relies on Auntie Gin. This is
26:53 one side to kind of something you'll over and over. Okay. So
26:58 it's basically a generic term chemicals that basically tell other cells of the immune
27:07 what to do. And they have variety of different functions as you'll
27:12 Um And names. Right? The kind of a generic name but their
27:17 names for all these things um and there are some processes here in this
27:24 . Okay. Um pam oops. . Not sure what that is
27:29 We'll talk about it. Figure The other thing is the type of
27:37 your body has to deal with. . Will require two different strategies.
27:46 you're gonna have pathogens who do their . So now this is in your
27:52 . Okay. Do their thing by outside yourselves. Right so we call
27:57 cellular pathogen. Okay. But then types that go inside yourselves and that's
28:03 motive infection viruses. So you have interest cellular and intracellular pathogens but you
28:11 to have two very different ways of with that. Okay because when a
28:16 is inside itself it's kind of hidden the body. Okay. And so
28:22 has to be a way to identify kind of infected cells and there
28:26 Alright so so they're gonna be way deal with both. Okay so you
28:32 the rule of thumb typically is fabulous . Won't work if it's inside of
28:38 cell. Right? Certainly if it's susceptible to fake a psychosis engulf it
28:44 chew it up. So we'll see are several strategies for what type of
28:50 is how we can be used to it maps. Okay champs champs
29:14 A. M. P. Yes it's so two operative right for
30:41 . Um And so and also your doesn't go into it and I'm not
30:46 touch you on it. Cells have . We have a bunch of cells
31:24 your body that have peace. Um And when they encounter passages like this
31:32 that that signal sort of a defect sets into motion the production of
31:41 Okay as I mentioned you have a of different functions. Okay. From
31:47 a few. Okay I will mention as we go through but uh come
32:31 With Octopus with a bunch of eight right? That would be an active
32:40 no arms. Right? That's an the part of me. They infection
33:04 is to get yourselves to that And so chemo taxes right? This
33:11 toward a chemical and so that's what does. Okay so if you have
33:16 skin cut or wound or something here whatever these chemo tactic signals will draw
33:24 immunity themselves there. Uh inflammatory response um That will go through that.
33:31 today. But next time. So these are typical responses. We've all
33:35 fever. We've all had inflammation. ? These are specific responses really.
33:41 is really about um containing that's just where it entered the body so to
33:51 . So we have like a splinter it's contaminated and you have an infection
33:56 the inflammatory response was meant to kind continue right there and not let it
34:02 . Um fever has its own use activate T. And B. Cells
34:09 that's activating the adaptive. So again are just four things five things but
34:15 of kind of doing a bunch of stuff as well. Okay all all
34:20 of activating some part of the immune . Okay so back to what so
34:26 of this system on this slide here total like receptor system right This is
34:33 like it's it's it's like pulling the smell smoke in the building and you
34:41 the fire alarm to alert everybody. kind of what this is kind of
34:47 alert the body let's get let's get kind of thing. Okay and I
34:54 do that and outside of kinds because will get certain cells to respond as
35:01 . Okay so to like receptors kind the alarm system so toll like receptors
35:07 these things. Right these things do kill anything. Okay they don't have
35:13 role in killing a pathogen. Their is in warning the body of a
35:19 pathogen is present. And let's get do something. Okay that's what it
35:24 . Right? Um so again it's obvious to you but the total receptor
35:32 not a cell is a protein on cell surface that interacts with a
35:38 A. M. P. And activates it. Um Okay so first
35:43 defenses so it's gonna be a little redundant as I said. So we
35:46 at it first as a physical So skin of course is a very
35:52 thick layer of multiple layers of Okay epithelial cells. And so that
35:59 itself provides a strong barrier. But you put in this kind of protein
36:06 that kind of holds it together and it keratin, keratin. Okay keratin
36:11 very and it's on the surface of body it's very thick on your fingernails
36:19 your fingernails are basically tearing your Okay. But but your body is
36:24 with this skin is covered with this well so it makes it very almost
36:29 Impenetrable but very stout barrier. But do have of course natural openings in
36:35 skin. Right? You have Right? Sweat glands, hair
36:41 So these are kind of can be openings where bacteria may be able to
36:45 . Okay and of course you have cut or otherwise away from bacteria to
36:52 your skin through a wound. That's what we call subcutaneous infection. So
36:57 membranes of course line which means that G. I tract obviously G.
37:03 track respiratory track etcetera. Okay and simply have a structure like this a
37:11 we often call a basement membrane. need to worry about that term.
37:16 as the blue kind of like the on top of that you have various
37:21 . This would be cells from your goblet cells are part of that.
37:26 And so but again very thick, and often producing uh always hold your
37:35 . Remember to produce some sort of secretion. What's the mucus is a
37:40 right to keep the cells moist uh the intestine and serves also the function
37:45 helping food pass through. But mucus nature of it can also help track
37:54 uh plus your your cilia in your form this thing called Salieri. You're
38:15 felt to see 54 3 uh and hair and track stuff right? Just
39:10 the cilia in your throat. Um and saliva. Uh So you always
39:18 your eyes. Well some are your but that you know, tears are
39:25 that to kind of keep washing wash microbes up, live what wash
39:31 your teeth and whatnot. Um So then as well earwax, earwax does
39:38 a function. I think that maybe trap bugs in your ears.
39:45 it's gonna be bugs as well, insects anyway. Um but certainly digestion
39:52 ? You eliminate lots of facts, past your system. Uh epiglottis,
39:58 the cover your wind pipe wall. you don't get things in your
40:02 So yeah all these are part of helping kind of prevent at least as
40:08 they can microbes from getting into your and where they're at more or
40:13 Okay so again all of these, of these will also act as chemical
40:20 . Okay so because they all have tends to be kind of a salty
40:29 acidic because the kind of molecules that produced there. And so that in
40:33 is a way to kind of um effect we can actually live there.
40:39 , staphylococcus like those conditions with july is one of the main bacteria you
40:45 on your skin. Another one uh . So survive a gastric juice.
40:52 very low ph um vaginal secretions. acidic urine is also actually slightly acidic
40:59 the one common thing in all many these is circled them here is
41:04 Okay in multiple places, write down right hand, is that material That
41:17 what they're so only. Okay so so definitely a defense against the bacterial
41:24 um that happened so long. And again as mentioned before we talked about
41:30 that this is part of your innate system as well, your microbiota.
41:35 their mere presence alone keeps other things taking hold um and they produce their
41:44 kind of micro environments that can oftentimes things from so very essential. Um
41:53 so first line uh physical and chemical then after them are second line.
42:01 so we start with kind of different types uh specific cell types involved.
42:06 you break down blood plasma fraction, centrifuge it um you have a protein
42:14 , the platform that contains anti biasing and other types of proteins. The
42:22 other part of this contains what are form elements. So red blood
42:25 Red blood cells um Our basically our sacks of hemoglobin and hemoglobin binds
42:37 Okay uh red blood cells don't have nucleus. Okay. Um But uh
42:45 also are not really cells are fragments involved in clotting but the cell types
42:51 course are your leukocyte, your white cells um of various types. And
42:56 these terminology of the granule sites and granule sites a little bit deceiving because
43:05 they all they all can have Okay, it's just that way,
43:12 at them under a light microscope, much more obvious in these types
43:18 Basic skills you look at and go that's a that's a grainy appearance.
43:22 . Not because they have lots of . Okay. Um It's just not
43:26 visible under a microscope. But these although although they do have but anyways
43:33 sometimes with terms it's a historical thing it never changes but that's that's how
43:38 still in front of the granule sites a granule sites. Um And so
43:44 go through each of these here alright neutrophils are gonna be your Early on
43:52 is neutrophils that are your primary fake cell types that do the bulk of
43:59 work initially. Right? Um so are in blood. So you see
44:05 70%, don't worry so much about percentages but just to show that they
44:12 in the highest quality of your And so if they're in your blood
44:18 you have an infectious agent that's in tissues outside the blood, right,
44:23 you have to get them out of blood into the surrounding tissues.
44:28 And that's what interferes do. so the exit blood is all part
44:33 that inflammatory response which was going next . But it's uh but you
44:42 aren't you floating around everywhere in your , there in your bloodstream? And
44:45 have to get them out of the . And there's a mechanism that they
44:49 let that happen. But they are primary infection fighters early on, they
44:52 taken over later. They um One thing. So you might look at
44:59 these cell types. They have like weird um morphology. Well they look
45:05 inside. You have these purple this is actually the D.
45:10 A. Chromosomes and they just form like sacks inside. They're all
45:17 But that's just how they look. what they call them, polity morpho
45:24 , probably more like it means many kind of nucleus just kind of a
45:29 future of those types. Basic So basic fields, unlike neutral fields
45:35 not specific cell types. They're thing to um release toxins typically and other
45:42 of cyber crimes. And so um so um lots of chemical services,
45:57 basically the amount in their blood is that high. So uh if you
46:02 hay fever, things like that, can probably blame your basic feels
46:06 Um so these are big acidic uh this big contributors and inter fields but
46:16 they do can act is in very pathogens by large. I mean we
46:21 about these worms before, right? those those can be attacked by
46:26 Their their thing is often to produce of tires and they actually interact with
46:33 pathogens. Um so again large practically like a big helmet or something like
46:41 right center field will be attracted to site and they actually interact with um
46:51 react with antibodies. So we'll see antibodies will interact with different of your
46:57 system selves in different ways. So antibodies our antibodies to the worm that
47:06 fills can also bind the antibody. then you get these all together.
47:10 a way to kind of collect a of sender films together so that when
47:15 release toxin right? You have a of toxin. So it's a way
47:20 concentrate center fields around the big right? Because you're gonna have to
47:26 have a lot of toxin and take of these things down. So you
47:30 get a bunch of center fields there have them hook onto the thing then
47:33 will release a toxin altogether and take down. So it's kind of how
47:38 work. Um so but again these these fully grown things are investing in
47:47 . B. Is short for Okay so like I said, you'll
47:55 see interactions between withdraw antibodies kind of this right? Like a why why
48:03 And these are all points that can . And so these this part
48:08 the two that are close together those and the bottom part is one that
48:13 buy into a cell type right? of some sort and even if it
48:19 one type that can do that, others that you'll you'll see as
48:22 Okay. Kind of jumping the gun but because I'll repeat this again but
48:26 we're here it seems like a good . Um So let's uh don't worry
48:34 you can get this thing wrong because gonna go through it again anyway when
48:38 get the antibodies and antigens. Um let's see what else is here we
48:45 . Okay so a grandiosity. These your macrophages. Dendritic cells. So
48:52 macrophages and dendritic cells start out as model site. So motorcycles circulating the
48:58 . But then they go to your system. Your lymphatic system plays a
49:05 part especially in your adaptive immune Okay so your B cells, your
49:11 cells macrophages. Dendritic cells they kind hang out in your lymphatic system,
49:16 what they do. Okay so if have had an infection and your doctor
49:22 this on your throat, right swelling maybe your armpit swell. Okay and
49:30 get painful. Um They're highly concentrated lymphatic vessels, right? And so
49:36 swell because the the cell types in are growing and proliferating right to fight
49:41 infection and that's what caused the Um The uh but they are so
49:48 macrophages and dendritic cells are specific but have this function. Okay, they
49:56 antigen presenting cells. So again these cell types that link up with the
50:01 immune system and uh and they can activated by your activity system. Have
50:11 functions there. Okay so engine presentation a big function that really has to
50:18 with um to alerting the body to their pathogens. I'll hold out for
50:28 . We'll wait. But energy building or a pc. They're also called
50:35 short text. So I'm adventurous Okay Now, very recently they are
51:26 of trying to exploit this activity and by genetically fixing natural killer cells to
51:35 able to be better at this function recognize different types of tumor cells.
51:41 using it to be a cancer fighting . Okay. There's a lot of
51:45 being done on that at the medical on that. Um But our context
51:50 we're looking at cells are infected. , so what happens is let me
51:58 I'm going to I just need to real quick to see. Okay.
52:02 it. Uh So the MHC that's the thing we need to talk about
52:08 affects a lot of different things Okay. So uh so natural killer
52:14 to look for infected or cancer So the thing is elaborate here in
52:19 second. So if your cells have certainly have different types of molecules on
52:28 surface. Okay. I'm just and of those and as opposed to your
52:36 healthy cells have all different types of on the surface, but they also
52:42 have and see energies. Okay, just drawing it like this just for
52:48 obvious. Um So the think of as a barcode there, you're a
52:59 on all of yourselves that identifies the to yourselves. So it's your own
53:03 barcode on all of yourselves comprising all tissues. Okay. So and they're
53:10 to be there. Okay, when not there, that's the signals,
53:15 . Weird. Something's not Right. . So if they're lacking or if
53:20 are only very few this or this they lack or have one or
53:28 that's something weird. The body that's not right. All right.
53:32 so that's what natural killer cells look for. Okay. And so they
53:36 of I guess they kind of hover the cells and they can recognize that
53:40 got the usual are supposed to have things and it's lacking. That's the
53:47 . Right? That cells not what supposed to be something wrong with
53:51 Okay I'll be infected. Okay. so infected cells like with a virus
53:58 other types, They can alter not of them, but many can alter
54:03 happens on the surface of the The types of things that end up
54:07 . And that's what natural killer for example, can detect that.
54:11 then the signals get rid of the , get it out of the
54:14 It's ineffective. Something's not right. also cancer cells can also produce that
54:21 appearance. Not all cancer types, some can and that also is a
54:26 of the cells not normal. Get of it. So that's what natural
54:29 cells do. Okay. Kind of for that. I'll elaborate. And
54:32 may see engine second, but that's of what any questions about that.
54:38 that's that's kind of what they Okay, so um so when they
54:43 bind, what do they do? , they I can hear it make
54:48 easier. Let's do this race. , so when they bind to
54:59 so they will um secrete these So preference. So think of
55:08 If you perforate something, you put punch a hole in it.
55:12 so preference is kind of like Almost protein tunnels. They stick into
55:16 cell and stuff we cut and the . Okay, enzymes are enzymes.
55:25 apoptosis is a feature um it's a feature of all yourselves. It's what's
55:33 a programmed cell death. So when cells are age and they don't work
55:39 anymore. Or something else damages The body says kill yourself, go
55:45 apoptosis basically. Right? You had sunburn, right? And you got
55:51 skin was peeling, That's the way see. It was red, it
55:55 hurt. And eventually the skin That is basically apoptosis going on.
57:44 the uh ability to come, what refers to is his. So oh
58:24 underneath. So you have two right? one and 2. The
59:06 way when I said uh huh. different. That's how uh with these
60:17 in different ways um and create different . Okay. And those effects can
60:24 the parts effect itself. Okay. it lacks MHC antigens, it'll be
60:29 rid of. Okay. Um the other types interact with other T cell
60:40 , interact with macrophages etc. We'll about that as we get into Chapter
60:45 next week. Okay. But the is, it makes the engines it's
60:49 critical to have a system like right? Otherwise, if you had
60:53 infectious agent in you, how would body know is even foreign or
60:59 Right. So you already have a in place with all your cells making
61:03 all your tissues that have those barcodes on them that are telling your body
61:09 is yours. Okay. So if else comes in that doesn't have that
61:14 then your body can say, oh something, not right, Foreign.
61:18 an agent, right, Do something it. So that's having that system
61:22 place allows you to detect something that's part of that system. Okay.
61:28 of course there's even times when your will attack its own, right?
61:35 your auto immune diseases. Right? certainly tissues become, you know,
61:40 body does fight them. That's you , for other different reasons. But
61:44 having a system in place like this you to detect something that's not not
61:49 same as what what that is. pathogens some sort. Okay. The
61:55 system as mentioned is an important So it's not um in terms of
62:02 immune immunity, the be checked against types of things you breathe in things
62:11 eat. Okay. Your your lymphatic will um can be particularly dense in
62:18 parts of your body. Like your particularly dense in lymphatic tissue, your
62:23 your throat, uh very dense. growing areas very dense tissue, swear
62:31 T cells, B cells, Dendritic cells hang out okay? Um
62:40 uh the uh and your spleen has synthetic tissue. You can filter out
62:47 in your blood for example. You have uh lymphatic tissue would concentrate
62:55 different parts of your skin, under skin, your intestinal wall.
63:00 And so how the lymphatic system uh it's a system of vessels of
63:06 But unlike vascular system, there's not heart pumping in fact typically move through
63:16 and through muscle contractions and through the of your arteries and arteries and
63:25 And so your arteries because lymphatic vessels very close to these things. Okay
63:29 so that kind of assists in pumping basically with lymphatic fluid lymphatic system is
63:37 for is to pick up fluid that's from your capillaries. Right? So
63:43 veins and arteries um intersect very very one cell thick vessels called capillaries.
63:52 called capillary bed. And um that's these are concentrating your vital organs.
63:58 so it feeds them, right? you exchange materials in the capillaries,
64:02 waste back and forth. And of when that happens you lose fluid from
64:10 blood volume, You lose fluid from vascular system. So you have to
64:13 able to recover that and dump it in. Right? That's what the
64:17 system does. It collects that what's interstitial fluid. Okay. It collects
64:23 and basically it dumps it back in here around your clavicle. And there's
64:28 where it dumps back into your cardiovascular and so it kind of helps to
64:33 blood volume and and because you do fluid from your cardiovascular system and that
64:40 pick it up. Okay. But it's a place where your these cell
64:46 reside. Okay. And so it's important for that. Um Now here's
64:54 example of your intestinal uh kind of lymphatic tissue very dense in your intestinal
65:02 intestines is in these pirate patches. , so very dense. And what
65:07 looks like in there is you have kinds of what are called m cells
65:12 between your normal kind of cells in intestine that are about absorbing food and
65:18 . Right? And so here are microbes coming through. You have um
65:24 system cells and macrophages and things that any kind of microbes that are that
65:30 in there to get rid of And so you'll have these is a
65:34 section and you see the dense tissue here pires throughout your intestines. Okay
65:44 so here so figure acidosis. Okay again this is one of your main
65:52 fight infection. Okay so your primary are macrophages, dendritic cells and um
66:01 . Okay and so in terms of they can be what are called wandering
66:08 fixed. Okay so wandering like the implies you can travel throughout your lymphatic
66:14 uh wandered around engulfing you know pathogens have you fixed or stay in one
66:22 . So very common to have for al Viola macrophages living a lifetime in
66:28 lungs and they pick up any kind microbes that might be there. Um
66:34 so the grandiose sites like neutrophils, , infections early in the infection
66:47 how this happens. So first get or dendritic cells to the site of
66:58 number one that's chemo taxes then stick the pathogens that part of that is
67:05 engulf mint process. Take it in then break it apart license. Okay
67:11 the four step process. And so so here you see here's a
67:18 Okay. And part of the binding is these pants, right? So
67:25 not just ingesting and figure sensitizing the but also releasing set of alert other
67:33 in the body. So they have as well. That and so um
67:40 is something we'll talk about later. the uh sometimes you have microbial types
67:49 are easier to buy it easier as be taken in than others. Other
67:55 are maybe have a very thick Okay. That makes them less able
67:59 be bound and taken in. That's it's a virulence factor. And so
68:03 do you deal with that? Will produce other chemicals that can code
68:07 And then that can be taken That's what do right. Something like
68:12 complement these coat the pathogen and then what's taken in. It makes it
68:19 to figure ties. Okay, the part. So you have a vehicle
68:27 it's engulfed right into a vehicle called figure zone. And then our feeding
68:34 . And then that fuses with the all Okay. And that's kind of
68:38 digestive organ. L that will then down the microbes either through production of
68:45 radicals. We talked about that Um these are toxic to the cell
68:51 have license line to break down cell and ultimately getting rid of it.
68:57 , now the thing about a about is these can also the particles that
69:07 you see some of these being These can also be the NHC module
69:15 these can present. And so microfiche also be an engine presenting cell,
69:20 ? A Pc. And they can that by taking some of this material
69:26 with MHC molecules in the cell then to the surface and now the engine
69:34 visible to the immune system. That respond in a different way.
69:41 that's what the engine presenting cell does you, allows the body to see
69:45 engine and respond to it. if I hadn't seen it before.
69:50 um the so I just mentioned about optimization, that not everything is easily
70:00 with thai so that's things like a capsule typically aren't. So they enhance
70:05 you can produce antibodies to it. then those antibodies are bound to the
70:12 . Right? And then the cell has a receptor that combined to that
70:18 the antibody Right? And then the thing gets taken in. Right?
70:24 it's a way to make something that not easily monetized. Okay, similarly
70:29 same process can occur. You can it with antibody compliment compliment kind of
70:37 soluble protein factors. So that can to sell and communication as well.
70:45 it's a way to figure these things aren't easily fixed. Okay,
70:50 observations of the molecule that code so can be an antibiotic compliment optimization is
70:56 process of taking it this way. . Um, that's a good way
71:03 pace. To stop. Right, . Thanks for hanging in there.
71:07 , we'll see you next weekend and
-
+