Quel rôle jouent les jonctions serrées ?

Les jonctions serrées agissent comme des barrières de diffusion empêchant le passage de molécules entre les cellules.

Quels tissus sont particulièrement dépendants des desmosomes ?

Les tissus cardiaque et cutané sont particulièrement dépendants des desmosomes pour résister aux forces de cisaillement.

Quels sont les composants clés des jonctions adhérentes ?

Les composants clés sont les cadhérines, dépendantes du calcium, qui aident à connecter les cellules entre elles.

Comment les jonctions communicantes facilitent-elles la communication cellulaire ?

Elles permettent le passage d'ions et de molécules de signalisation, facilitant la communication directe entre cellules.

Quels sont les effets possibles d'un dysfonctionnement des jonctions cellulaires ?

Cela peut entraîner des maladies comme le pemphigus vulgaire et même favoriser la métastase dans le contexte du cancer.

Quelle est la différence entre les desmosomes et les hémidesmosomes ?

Les desmosomes relient les cellules entre elles, tandis que les hémidesmosomes connectent les cellules à la matrice extracellulaire.

Cell Junctions

00:45:44

https://www.youtube.com/watch?v=gmlA8V2zMv4

Zusammenfassung

TLDRDans cette vidéo éducative sur les jonctions cellulaires, le présentateur explique les divers types de jonctions qui relient les cellules, tels que les jonctions serrées, les jonctions adhérentes, les desmosomes, les hémidesmosomes et les jonctions communicantes. Chacune de ces jonctions est discutée en détail, couvrant leur structure moléculaire et leur rôle fonctionnel. Les jonctions serrées agissent comme des barrières de diffusion, essentielles dans des régions comme la barrière hémato-encéphalique. Les jonctions adhérentes et les desmosomes résistent aux forces de cisaillement et d'étirement, se trouvant dans les tissus soumis à des tensions comme la peau, les poumons et les tissus cardiaques. Les hémidesmosomes attachent les cellules à la matrice extracellulaire. Les jonctions communicantes permettent la communication entre cellules via le passage d'ions et de molécules de signalisation. La vidéo aborde également les implications cliniques des défaillances de ces structures, telles que le développement du cancer lié aux mutations des cadhérines et les maladies auto-immunes comme le pemphigus vulgaire.

Mitbringsel

🔗 Les jonctions serrées agissent comme des barrières de diffusion empêchant le mouvement à travers les cellules.
🦠 Implication clinique des jonctions serrées dans la protection du système nerveux central via la barrière hémato-encéphalique.
🔬 Les jonctions adhérentes aident à résister aux forces de cisaillement et sont essentielles dans les tissus soumis à l'étirement.
🫀 Les desmosomes sont cruciaux pour le tissu cardiaque et aident à prévenir la séparation cellulaire sous pression.
🧬 Hémidesmosomes connectent les cellules à la matrice extracellulaire.
📞 Les jonctions communicantes permettent la communication cellulaire via le passage d'ions et de molécules de signalisation.
🧪 Dysfonctionnement des cadhérines peut entraîner la métastase dans le cancer.
💡 Les connexons, constitués de connexines, forment des canaux entre les cellules pour permettre la communication.
🩺 Pemphigus vulgaire et pemphigoïde bulleuse illustrent les effets auto-immunes sur les jonctions.
🫁 Importance des jonctions dans la structure et la fonction des tissus respiratoires, cardio-vasculaires et cutanés.

Zeitleiste

00:00:00 - 00:05:00
Les ninja nerds introduisent les jonctions cellulaires, incitant à s'abonner pour plus d'informations détaillées disponibles sur leur site.
00:05:00 - 00:10:00
Présentation de Chegg comme ressource d'étude avec explication des outils disponibles sur leur plateforme.
00:10:00 - 00:15:00
Introduction aux jonctions cellule à cellule, expliquant brièvement leur fonction de maintien structurel.
00:15:00 - 00:20:00
Les types de jonctions cellulaires incluent jonctions serrées, d'adhérence et desmosomes, chacun ayant une fonction spécifique dans la structure cellulaire.
00:20:00 - 00:25:00
Explication des jonctions serrées avec leurs rôles dans la barrière de diffusion et exemples dans le corps humain.
00:25:00 - 00:30:00
Les jonctions d'adhérence sont détaillées pour leur résistance aux forces de cisaillement, présents dans divers tissus corporels.
00:30:00 - 00:35:00
Les desmosomes, avec leur résistance aux tensions, sont liés aux disques intercalaires en tissu cardiaque.
00:35:00 - 00:40:00
Présentation des hémidesmosomes, se concentrant sur leur connexion entre cellules et matrice extracellulaire.
00:40:00 - 00:45:44
Les jonctions gap permettent la communication intercellulaire, essentielles pour les tissus excitables comme muscles cardiaques et certains neurones.

Mind Map

Video-Fragen und Antworten

Quels sont les principaux types de jonctions cellulaires abordés ?
Les principaux types discutés sont les jonctions serrées, les jonctions adhérentes, les desmosomes, les hémidesmosomes et les jonctions communicantes.
Quel rôle jouent les jonctions serrées ?
Les jonctions serrées agissent comme des barrières de diffusion empêchant le passage de molécules entre les cellules.
Quels tissus sont particulièrement dépendants des desmosomes ?
Les tissus cardiaque et cutané sont particulièrement dépendants des desmosomes pour résister aux forces de cisaillement.
Quels sont les composants clés des jonctions adhérentes ?
Les composants clés sont les cadhérines, dépendantes du calcium, qui aident à connecter les cellules entre elles.
Comment les jonctions communicantes facilitent-elles la communication cellulaire ?
Elles permettent le passage d'ions et de molécules de signalisation, facilitant la communication directe entre cellules.
Quels sont les effets possibles d'un dysfonctionnement des jonctions cellulaires ?
Cela peut entraîner des maladies comme le pemphigus vulgaire et même favoriser la métastase dans le contexte du cancer.
Quelle est la différence entre les desmosomes et les hémidesmosomes ?
Les desmosomes relient les cellules entre elles, tandis que les hémidesmosomes connectent les cellules à la matrice extracellulaire.

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Untertitel

Automatisches Blättern:

00:00:07
what's up ninja nerds in this video
00:00:08
today we're going to be talking about
00:00:09
cell junctions but before we get started
00:00:11
if you guys like this video you benefit
00:00:13
from it it makes sense it helps you
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please support us by hitting that like
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button commenting down the comment
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section and please subscribe also down
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in the description box below click on
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00:00:23
guys can actually come here purchase all
00:00:26
of these awesome notes illustrations
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everything that's going to help you guys
00:00:29
to truly understand this topic
00:00:31
all right engineering so let's go ahead
00:00:32
and take a look here at the chegg
00:00:34
website so if you guys go down in the
00:00:35
description box below we'll have a link
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there it'll take you guys to this part
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of their website and the nice thing
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about clicking on that link it'll give
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you this nice coupon code five dollars
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off for your first month of chegg study
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pack click on that when you click on
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their website their home page
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on their home page there's a sidebar
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here called study tools okay there's a
00:00:58
lot of different options there but what
00:00:59
i want us to do is take a look here at
00:01:02
one of my courses that i'm just picking
00:01:04
at random let's say organic chemistry
00:01:05
let's say you're taking a class organic
00:01:07
chemistry you need some extra help and
00:01:09
one of the things that you really need
00:01:10
some help with is let's say that you're
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you're getting ready to take a a an exam
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on mass spectroscopy and infrared
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spectroscopy so you go ahead and click
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on that right there
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and what it takes you to is a nice
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little kind of course particularly kind
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of like a question process that will
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help you guys to test your knowledge on
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whatever you guys are learning in
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organic chemistry particularly on this
00:01:32
topic and let's say that you guys go
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ahead you pick one of these questions
00:01:35
you get it wrong you picked c and it was
00:01:38
oh it was actually it was it was a all
00:01:40
right well here's the reason why it was
00:01:43
a and it'll give you guys kind of a nice
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little solution it'll tell you okay
00:01:47
here's the particular reasoning as to
00:01:49
why and it gives you all the concepts
00:01:52
the reasoning the fundamentals takes you
00:01:54
through it all step by step and gives
00:01:56
you an explanation of why that was the
00:01:58
correct answer some common mistakes that
00:02:00
you guys need to be thinking about and
00:02:02
even hints for the next step alright so
00:02:05
i think this is a really cool
00:02:07
resource for those of you guys who are
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out there need a little bit of extra
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help i think chegg will be the people
00:02:12
that will help you guys in doing this so
00:02:14
please go down the description box below
00:02:16
check out that link and check out this
00:02:17
check website all right ninja nerds
00:02:19
let's get into this video all right
00:02:20
ninjas let's talk about cell to cell
00:02:22
junctions really it's not that hard
00:02:24
right it's basically just little
00:02:26
adhesions that are forming between cells
00:02:28
and there's many different functions of
00:02:30
these cell to cell junctions obviously
00:02:32
if you had one cell here in one cell
00:02:35
here and we had just certain proteins
00:02:37
that were anchored between these maybe
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it's to hold them together so that way
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if there's any kind of shearing forces
00:02:42
or stretching or abrasive forces it can
00:02:45
resist the separation of those cells or
00:02:48
if you have ions that are trying to move
00:02:50
between the cells and you don't want
00:02:52
those certain things to move through it
00:02:53
can block that it can act as like a
00:02:55
diffusion barrier or
00:02:57
maybe you have little channels that
00:02:59
exist between these two cells and you
00:03:01
want the cells to communicate with one
00:03:03
another or last but not least you know
00:03:05
there's a structure here we have a cell
00:03:07
here we have a cell there's a structure
00:03:09
underneath these cells called a basal
00:03:11
lamina
00:03:13
and a basal lamina is actually a little
00:03:15
bit of connective tissue and we also
00:03:17
have a heat adhesion molecules that not
00:03:19
just connect cell to cell
00:03:21
but connect the cell to the
00:03:23
extracellular matrix or the basal lamina
00:03:26
and this is what makes up what's called
00:03:27
your basement membrane
00:03:29
in order for us to truly understand
00:03:31
cell-to-cell's junctions though we have
00:03:33
to really zoom in look at their
00:03:35
structure know the names of those
00:03:36
structures the significance of it what
00:03:38
these things are actually functionally
00:03:40
for
00:03:41
and know what happens if these things
00:03:43
are damaged or what clinical things are
00:03:45
important
00:03:46
so what i want us to do is actually want
00:03:48
to really zoom in
00:03:50
on this connection between the cells
00:03:53
blow that up and look at these cells in
00:03:56
a more zoomed in fashion and this is
00:03:58
what we're going to be pretty much
00:04:00
focusing on for the rest of this video
00:04:02
there is a couple different types of
00:04:03
cell to cell junctions and then cell
00:04:05
extracellular matrix or basal lamina
00:04:07
junction
00:04:08
the first one that we'll discuss is
00:04:10
called tight junctions and there's
00:04:12
proteins called occludings and claddins
00:04:14
and zone occludens all of these things
00:04:16
that we'll get into that that's the
00:04:17
first one
00:04:19
the second one that we'll talk about is
00:04:20
called the adherence junctions
00:04:23
and the third one that we'll talk about
00:04:25
is called your desmosomes
00:04:28
now what you guys will understand is
00:04:29
that tie junctions big thing to take
00:04:31
away from it is they're more of like a
00:04:32
diffusion barrier they block things from
00:04:34
moving between cells and help to hold
00:04:35
cells tightly together
00:04:37
adherence junctions are much stronger
00:04:39
than type junctions and they're really
00:04:41
good for shearing forces and abrasive
00:04:43
forces but you know desmosomes are the
00:04:45
most tough and really really high
00:04:48
tensile against high shearing forces a
00:04:50
lot of abrasive stretch
00:04:53
next thing is gap junctions and these
00:04:54
are good for cell to cell communication
00:04:57
and last but not least is what's called
00:04:59
your hemidesmosomes and these are what
00:05:02
connect cells
00:05:04
to the basal lamina or the extracellular
00:05:06
matrix so we have tight junctions at
00:05:09
hearings junctions desmosomes gap
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junctions and hemidesmosomes let's talk
00:05:13
about each one of these individually
00:05:14
understand their structure understand
00:05:16
their function and understand the
00:05:17
clinical significance all right so the
00:05:19
first solid cell junction that we have
00:05:20
to talk about is called tight junctions
00:05:21
now tight junctions what i need you guys
00:05:23
to know i need to know the structure the
00:05:24
function and the clinical significance
00:05:26
okay so first thing about the structure
00:05:29
when we talk about these here's cell
00:05:30
number one let's actually let's call
00:05:32
this cell number one and this is cell
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number two
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and again we're just looking at the cell
00:05:36
membranes of cell number one and cell
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number two and how these cell membranes
00:05:41
are actually joined together okay
00:05:43
because that's the point of the junction
00:05:45
that we have here this tight junction
00:05:47
there's two particular proteins that
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come out from the cell membrane and
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interact with one another in between the
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space between these cells
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and this per this pink protein up here
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there's two types one is called clawdens
00:06:02
so you have what's called clawdens
00:06:05
and then the other one down here in this
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purple color here is called occludens
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so you have two particular proteins that
00:06:14
are basically spanning through the
00:06:17
extracellular
00:06:18
space and actually anchored into the
00:06:20
cell membrane of cell one and cell two
00:06:22
and again these proteins are called
00:06:24
claudines and occludens
00:06:27
now
00:06:28
on the inner cytosolic so this would be
00:06:30
on the cytosol side right so this is the
00:06:31
cell membrane this would be on the
00:06:33
cytosol this would be the extracellular
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space
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on the cytosolic side there's these
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black proteins these black circular
00:06:39
proteins
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these black circular proteins are called
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zona
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occludins
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they're called zona occludings and
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there's different types there's zo1
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zo203
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okay
00:06:54
so again you have spanning through the
00:06:56
cell membrane out into the extracellular
00:06:58
spaces the claudines and occludens they
00:07:00
connect with one another from cell one
00:07:01
to cell two on the cytosolic side you
00:07:04
have the zona occludens and they're
00:07:06
bound to that actual cludens and
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claudin's proteins okay
00:07:11
then the last protein here on the inner
00:07:14
cytosolic side that are bound to the
00:07:16
zone occludens these kind of navy blue
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ones here
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these are called actin
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filaments
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they're called actin filaments
00:07:26
so there is again
00:07:28
knowing these proteins this is a very
00:07:29
important thing
00:07:30
because if they ask you on the test high
00:07:32
junctions
00:07:33
the actual part of the protein that
00:07:35
spans through the cell membrane out to
00:07:36
the extracellular component and attaches
00:07:39
cell to cell those are called
00:07:41
clawdens and occludens
00:07:44
the proteins on the cytosolic side that
00:07:47
is bound to those actual transmembrane
00:07:50
proteins the occludings and claudians is
00:07:51
called
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zona occludens
00:07:54
and then the proteins that are bound on
00:07:55
the most inner cytosolic side to the
00:07:57
zona occludens are called the actin
00:08:00
filaments
00:08:01
now
00:08:02
why is this important
00:08:04
the significance of the tight junctions
00:08:07
is really within the name they tightly
00:08:09
hold the cells together
00:08:12
and the main focus of that is imagine
00:08:14
you have some type of like
00:08:16
sodium molecule or potassium molecule or
00:08:19
maybe you have some type of like protein
00:08:22
molecule that you don't want to be able
00:08:24
to
00:08:25
move
00:08:26
between these cells you want to block
00:08:29
that process
00:08:30
that is the function of these actual
00:08:32
tight junctions so their design is to
00:08:35
act as a diffusion barrier
00:08:38
and pretty much block
00:08:40
the transport of ions and different
00:08:44
types of large molecules between the
00:08:46
cells okay that's really it
00:08:49
what i really want to add on though
00:08:51
is imagine that we have two parts of the
00:08:53
cell right
00:08:54
so you have this part of the cell all
00:08:56
right let's imagine here i have this
00:08:57
blue
00:08:58
tissue here this remember this was
00:08:59
called the basal lamina
00:09:01
it was just underneath it's called the
00:09:03
it basically makes up whenever you have
00:09:04
the cell and then this basal lamina
00:09:06
makes up what's called the basement
00:09:07
membrane
00:09:08
this is the basal surface of the cell
00:09:11
this is the apical surface of the cell
00:09:14
tight junctions are mainly connecting
00:09:17
cell to cell
00:09:18
at the apical surface that's a very
00:09:21
important thing so another thing i need
00:09:22
you guys to remember is that they're
00:09:24
connected at what surface
00:09:26
the apical
00:09:27
surface
00:09:29
so they connect cell to cell at the
00:09:31
apical surface and they're primarily a
00:09:33
diffusion barrier for things like ions
00:09:35
and large molecules that's really it
00:09:39
now
00:09:40
what kind of locations would you want
00:09:42
these diffusion barriers where you want
00:09:45
to really kind of hold cells tightly
00:09:46
together and maybe block certain things
00:09:48
that you want to be able to move
00:09:50
not to be able to actually move between
00:09:52
the cells and get into a particular area
00:09:54
well i would think that one really
00:09:56
important one that you'd really really
00:09:58
want to be careful of
00:10:00
is your brain right you don't want just
00:10:02
proteins just moving wherever they want
00:10:04
in and out of the blood and into your
00:10:06
actual neural tissues so the blood-brain
00:10:09
barrier is definitely riddled with lots
00:10:11
of tight junctions so the blood
00:10:14
brain barrier would definitely be one
00:10:16
big one
00:10:17
so you know within the blood-brain
00:10:18
barrier you have these cells here this
00:10:20
is a capillary here this is a blood
00:10:22
vessel
00:10:23
and then this blue stuff is called the
00:10:24
basal lamina and then this third thing
00:10:27
is called your astrocytes right
00:10:30
so these three things are what make up
00:10:31
your blood-brain barrier
00:10:33
well these
00:10:35
uh kind of red cells are called
00:10:37
endothelial cells
00:10:39
and in between the endothelial cells you
00:10:41
see these these actual pink and purple
00:10:43
proteins those are called your tight
00:10:45
junctions so whenever you have molecules
00:10:48
that are running through here maybe you
00:10:50
have some type of like
00:10:51
amino acid or some type of protein
00:10:54
molecule that you don't want to be able
00:10:56
to get out into this area where the
00:10:58
neurons are at these actual proteins
00:11:01
will block that so that's their function
00:11:03
of it as a diffusion barrier so think
00:11:05
about blood-brain barrier
00:11:06
another one
00:11:08
is you know actually within our gi tract
00:11:10
our git is a really important one that i
00:11:12
want you guys to remember so two big
00:11:14
ones if you don't remember the other
00:11:15
ones please don't forget this one blood
00:11:18
brain barrier and git
00:11:20
the git we also have lots of these
00:11:22
little tight junctions near the apical
00:11:24
surface
00:11:24
because we also want to be able to again
00:11:26
prevent certain types of
00:11:28
pathogens certain types of molecules
00:11:30
that are in our gi tract from getting in
00:11:33
to the actual blood where things are
00:11:35
supposed to be absorbed
00:11:37
so we want to have tight junctions here
00:11:39
that control the movement of certain
00:11:41
types of molecules
00:11:43
from the actual lumen and into the
00:11:45
bloodstream
00:11:47
you know what else
00:11:48
is that especially in the stomach you
00:11:51
know the cells are tightly bound to one
00:11:52
another
00:11:53
if you have these cells that are tightly
00:11:55
bound to one another in the stomach
00:11:57
what's the stomach make a lot of
00:11:59
hydrochloric acid we want those cells to
00:12:01
be really tightly close to one because
00:12:03
if we have some separation between them
00:12:05
what can happen that hydrochloric acid
00:12:06
can seep in between those cells and
00:12:09
cause necrosive damage so it's also
00:12:12
really important to think about this
00:12:14
whenever you have these two cells within
00:12:16
the stomach you definitely want a really
00:12:17
tight connection because imagine if that
00:12:20
nasty hydrochloric acid was able to seep
00:12:23
between these it would cause destructive
00:12:25
lesions
00:12:27
so that's another thing so again it's
00:12:28
trying to prevent nasty molecules and
00:12:30
nasty proteins or pathogens from being
00:12:32
able to move from the lumen and into the
00:12:35
tissues or the blood around that actual
00:12:37
gi tract
00:12:39
other areas to think about
00:12:41
is your respiratory system obviously
00:12:43
within the respiratory tract
00:12:45
there's definitely going to be these
00:12:48
beautiful tight junctions
00:12:50
and there's actually a specialized tight
00:12:52
junctions we actually have to mention
00:12:54
this this might come up in your usmle is
00:12:57
that in the kidneys there's what's
00:12:59
called leaky i know it's weird but we
00:13:02
call them leaky junctions they're a sub
00:13:05
of tight junctions
00:13:07
and in the actual proximal convoluted
00:13:09
tubule is the specific place that i want
00:13:12
you guys to remember there's what's
00:13:13
called leaky junctions so if you imagine
00:13:15
you take kind of an uh a cell here and a
00:13:18
cell here and let's imagine this is a
00:13:20
part of the kidney tubules
00:13:22
these cells have these little leaky
00:13:24
junctions between them they're like
00:13:26
tight junctions but they allow for
00:13:29
certain types of ions to be able to pass
00:13:31
through things like potassium things
00:13:32
like chloride things like sodium and
00:13:34
water okay so that's a specialized tight
00:13:37
junction they're called leaky junctions
00:13:39
and they're found in the proximal
00:13:41
convoluted tubule of the kidneys so to
00:13:43
recap occludants claudines zona
00:13:45
occludens actin again apical surfaces
00:13:49
where these tight junctions are
00:13:50
connecting they're a diffusion barrier
00:13:52
big ones to remember is blood-brain
00:13:53
barrier
00:13:54
git
00:13:55
respiratory tract and again there's this
00:13:58
modified type called leaky junctions in
00:14:00
the kidney tubules why is all this
00:14:02
important why do we need to know this
00:14:04
here's why here's the clinical relevance
00:14:06
to it you know there's a nasty pathogen
00:14:10
okay two of them
00:14:11
one is called helicobacter
00:14:14
pylori you guys know this pathogen
00:14:17
and there's another one called
00:14:19
clostridium
00:14:21
difficile
00:14:23
these pathogens they release nasty types
00:14:25
of toxins you know what these toxins do
00:14:29
they cause destruction
00:14:32
of these tight junctions
00:14:34
if you destroy the tight junctions and
00:14:35
you form kind of a little space between
00:14:37
these
00:14:39
okay so now i can form like actual space
00:14:41
between these cells
00:14:43
i can now easily allow for certain types
00:14:46
of
00:14:47
things molecules whatever it may be
00:14:49
to be able to go in between these cells
00:14:52
a lot easier
00:14:54
in the stomach where h pylori likes to
00:14:56
stay
00:14:57
what would that do
00:14:59
if you actually got rid of the tight
00:15:00
junctions in this area
00:15:03
you would allow hydrochloric acid to
00:15:04
start eroding its way through and then
00:15:06
imagine what can happen if you start
00:15:08
having like that kind of process
00:15:09
happening
00:15:10
where you start forming these nasty
00:15:12
little things called
00:15:14
ulcers
00:15:15
so then the actual helicobacter pylori
00:15:17
again it can actually invade into these
00:15:19
areas
00:15:20
and what can this cause what is this
00:15:21
disease called this is called peptic
00:15:23
ulcer disease
00:15:24
so peptic
00:15:26
ulcer disease is the result of the h
00:15:30
pylori separating the tight junctions
00:15:32
within the stomach and allowing for the
00:15:34
acid to infiltrate in between causing
00:15:36
ulcers
00:15:38
c diff you guys know this one it's going
00:15:40
to infiltrate in between these actual
00:15:42
cells start separating them
00:15:44
and when you separate them what's going
00:15:46
to be able to leak out different things
00:15:47
like water and different ions and that's
00:15:50
going to cause lots of
00:15:52
diarrhea
00:15:53
and as a result if you get all of this
00:15:55
intense diarrhea
00:15:57
this is a infectious process called
00:16:00
clostridium difficile associated
00:16:01
diarrhea and that is due to the c diff
00:16:04
because again you're forming separation
00:16:07
between those cells and allowing for
00:16:08
things to now easily be able to get
00:16:10
pulled into the lumen of the gi tract
00:16:13
and plus more inflammatory molecules
00:16:15
like more pathogens can actually leak
00:16:16
into the bloodstream that way as well
00:16:18
so
00:16:19
you get the significance of type
00:16:21
junctions now
00:16:22
let's now move on to the next one which
00:16:24
is called the adherence junctions all
00:16:25
right so let's talk about the second
00:16:27
junction the adherence junctions the
00:16:29
adherence junctions are really cool so
00:16:31
when we talk about in comparison tight
00:16:33
junctions versus adherence junctions
00:16:36
these are more specifically what we're
00:16:37
going to talk about for more shearing
00:16:39
forces stretch being able to resist a
00:16:41
lot of high tensile types of abrasive
00:16:44
forces really
00:16:46
but in order to do that we have to know
00:16:47
the particular proteins that are
00:16:49
involved to help in that process so the
00:16:51
first component here is these blue
00:16:53
proteins and this is actually a really
00:16:54
important component here so these
00:16:56
proteins here are called
00:16:59
cadherins but we give them a special you
00:17:01
know number a little letter before we
00:17:03
call it e
00:17:05
cad adherence
00:17:08
so it's the extracellular component of
00:17:10
the catherine okay because the catherine
00:17:12
actually anchors into the cell membrane
00:17:14
and then you have the component of it
00:17:15
that actually is going to bulge out from
00:17:18
the cell membrane into the extracellular
00:17:20
space so this is an e-cad here and this
00:17:22
is an e-cad here and it actually it's
00:17:24
interesting is that they're both kind of
00:17:25
like homologous to one another they both
00:17:27
are pretty much the same type of
00:17:29
structure
00:17:30
now when we have this e-cad hearing and
00:17:32
this e-cad here and actually binding
00:17:33
with one another we have to have some
00:17:35
special molecule between them that
00:17:38
actually helps to really anchor them
00:17:39
together you know what that beautiful
00:17:40
molecule is that actually sits right in
00:17:42
this space here
00:17:44
good old calcium so once you have once
00:17:46
you remember here is cad hearings
00:17:49
anytime you see that word cad hearings
00:17:52
these are calcium dependent proteins
00:17:55
that's a big thing for your test cad
00:17:57
herons are calcium dependent proteins so
00:18:00
usually calcium acts as the bridge
00:18:02
between anchoring these two cadherins
00:18:04
together okay so that e-cadherins coming
00:18:06
from the cell membrane outwards into the
00:18:08
extracellular space binding with one
00:18:10
another via the process of calcium
00:18:13
the next protein which is actually going
00:18:15
to be on that inner cytosolic side of
00:18:17
the cell membrane is this purple protein
00:18:20
this purple protein here is called
00:18:22
vinculin
00:18:25
and then there's another one which is
00:18:27
this maroon color protein which is again
00:18:30
on the inner cytosolic side
00:18:32
and usually it's kind of like coupled
00:18:34
right next to the vein killing just for
00:18:35
simplicity's sake we put it right after
00:18:37
it but usually they're kind of like
00:18:38
around the same proximity with one
00:18:40
another and these are called the katinin
00:18:42
proteins and there's different types of
00:18:44
ketene and proteins okay so you have the
00:18:47
e-cadherins then you have the vinculin
00:18:49
and catenan proteins and then the last
00:18:51
part which is on the most inner
00:18:53
cytosolic side
00:18:54
is what's called your actin filaments
00:18:57
these are called your actin
00:19:00
filaments
00:19:01
so when someone says hey which types of
00:19:03
junctions contain actin filaments on
00:19:05
their most inner cytosolic side you can
00:19:07
say
00:19:08
tight junctions and adherence junctions
00:19:10
and you'll see later that even other
00:19:12
proteins as well but
00:19:14
that is the basic structure so from
00:19:16
extracellular side e-cadherins with
00:19:18
calcium then vinculin and katanan and
00:19:20
then actin filaments on the almost inner
00:19:22
part now because these have all of these
00:19:26
really important anchoring proteins
00:19:28
they're more for resisting a lot of
00:19:29
stretch
00:19:30
okay so when we talk about their
00:19:32
function if we have cell one here
00:19:34
and cell two
00:19:36
these are if you actually look compared
00:19:37
this is the apical surface so if i had
00:19:39
kind of that basal lamina again
00:19:41
this is the basal lamina here
00:19:44
this is the apical surface this is the
00:19:46
basal surface
00:19:47
these are usually a little bit more
00:19:49
basil so if we had to compare let's say
00:19:51
here's your tight junctions
00:19:53
it's going to be more basal in
00:19:55
comparison to the tight junctions so if
00:19:57
we were to put here for their actual
00:19:59
position of where they are they're more
00:20:01
basal
00:20:04
in comparison
00:20:08
two
00:20:10
tight junctions
00:20:12
okay beautiful that's one thing the
00:20:15
second thing that i really want you to
00:20:16
remember is tight junctions are more as
00:20:17
a diffusion barrier right they block
00:20:19
ions molecules large proteins things
00:20:21
from being able to move past them
00:20:23
between the cells
00:20:24
adherence junctions are more for
00:20:27
shearing
00:20:30
or abrasive forces
00:20:33
so any type of like thing where there's
00:20:35
a lot of stretching there's a lot of
00:20:37
rubbing
00:20:38
anything that's trying to separate cells
00:20:40
apart from one another this is their
00:20:42
design they're more designed to be able
00:20:44
to resist those shearing and abrasive
00:20:47
forces that is their design they're not
00:20:49
really a diffusion barrier they're more
00:20:51
resistant allowing for stretch okay
00:20:53
keeping those cells together
00:20:55
so
00:20:56
with that being said what type of
00:20:58
tissues would you really want to have
00:21:00
these kinds of junctions really anywhere
00:21:02
where there's tight junctions we have
00:21:04
adherence junctions they give a little
00:21:05
bit more of that ability to prevent the
00:21:08
cells from separating from one another
00:21:10
from intense types of stretch or
00:21:12
abrasion
00:21:13
what kind of things would that be well
00:21:15
your stomach and your gastrointestinal
00:21:16
tract have to accommodate
00:21:18
to food and fluids so they're going to
00:21:20
have to stretch they have to accommodate
00:21:21
to that so they'd be found within your
00:21:24
gastrointestinal tract so that'd be one
00:21:26
your git
00:21:28
the other thing is your epithelial
00:21:30
tissue
00:21:31
your epithelial tissue within your
00:21:32
respiratory tract your respiratory tract
00:21:34
may have to also undergo particular
00:21:36
dilation and constriction within your
00:21:37
bronchioles and so because that they
00:21:40
also have to not only have that process
00:21:42
but you know whenever your alveoli are
00:21:44
inflating they have to be able to
00:21:45
accommodate maybe a certain amount of
00:21:46
stretch or distensibility our lungs are
00:21:48
naturally compliant so we want the lungs
00:21:50
to be able to have some compliance and
00:21:52
ability to stretch whenever they're
00:21:53
being inflated versus whenever they're
00:21:55
actually exhaling and they're collapsing
00:21:57
so lungs would be another tissue that
00:21:59
you want to allow for them to stretch
00:22:01
but not separate from one another
00:22:02
whenever they're actually expanding
00:22:04
so the lungs
00:22:06
or any part of your respiratory tract
00:22:07
really
00:22:09
also
00:22:11
your urogenital system which part of
00:22:13
these would actually be the bigger one
00:22:14
though
00:22:15
your bladder right your bladder has to
00:22:17
be able to stretch and accommodate urine
00:22:19
so your urinary tract would be a very
00:22:21
important one so whenever your your
00:22:22
bladder is getting filled up with all
00:22:24
that urine and you're like oh baby i
00:22:26
gotta go
00:22:27
these cells help to be able to prevent
00:22:28
those these uh adherence junctions
00:22:30
prevent these cells from wanting to
00:22:32
separate from one another they allow for
00:22:33
more of that stretch
00:22:34
and again shearing type of abrasive
00:22:36
forces all right so not just these areas
00:22:38
but also think about blood vessels blood
00:22:40
vessels have to be able to stretch right
00:22:43
particularly it have to undergo what's
00:22:44
called vasodilation
00:22:46
so they have to be able to expand but
00:22:48
they also have to be able to constrict
00:22:50
so because of that they're going to
00:22:52
undergo particular you know stretching
00:22:54
shearing abrasive forces also blood flow
00:22:57
is hitting against these so there's also
00:22:59
that type of force there so we want to
00:23:00
be able to have nice junctions there to
00:23:02
allow for again the vasodilation aspect
00:23:05
which prevents the cells from separating
00:23:07
during that process but also if blood is
00:23:09
flowing through here and hitting against
00:23:11
these vessels with high pressure they
00:23:13
have to be able to accommodate that high
00:23:14
shearing forces all right what's another
00:23:16
type of tissue that undergoes a lot of
00:23:17
you know abrasive and kind of like
00:23:19
shearing forces the skin right
00:23:21
yeah so the skins are definitely a big
00:23:23
one that one's going to take on a lot of
00:23:25
stretching abrasive types of forces a
00:23:27
lot of like anything that's really going
00:23:28
to be involving a lot of excessive
00:23:30
rubbing against the skin so that would
00:23:32
be a big thing to think about as well so
00:23:34
we got git respiratory tract urinary
00:23:36
tract blood vessels and skin this is a
00:23:39
big big one though don't forget that one
00:23:41
and that's one of the things that really
00:23:42
differentiates tight junctions from the
00:23:43
adherence junctions as well
00:23:45
now here's what's really cool clinical
00:23:47
significance wise you know uh these
00:23:49
adherence junctions especially those eek
00:23:51
adherents
00:23:53
you know whenever people develop cancer
00:23:55
unfortunately
00:23:57
cancer
00:23:58
certain types of genes
00:24:00
may be
00:24:02
mutated i guess is the best way of
00:24:04
saying it and whenever these genes are
00:24:06
mutated it can alter the structure of
00:24:08
some of these proteins and what it can
00:24:11
do is it can alter the structure of
00:24:13
those cadherin proteins
00:24:15
and what can happen is if those cadherin
00:24:17
proteins aren't actually present are the
00:24:19
cells going to be able to stick with one
00:24:21
another very well
00:24:22
no
00:24:23
and so what happens is these cadherin
00:24:25
proteins maybe become mutated in a
00:24:27
particular way where they aren't
00:24:28
allowing for these cells to stick with
00:24:29
one another think about why that could
00:24:31
be a problem let's say that you have
00:24:32
somebody who develops a cancer right and
00:24:35
these cells are basically kind of glob
00:24:37
together you have this mass now
00:24:40
and
00:24:41
it undergoes a particular mutation
00:24:43
and that mutation allows for maybe a
00:24:46
clump of these cells to separate off
00:24:48
from one another so let's say that these
00:24:50
cells just kind of clumped off and
00:24:52
separate because these actual proteins
00:24:54
got mutated
00:24:56
now i can have a clump
00:24:59
of these cells that can spread from this
00:25:01
primary location to a secondary location
00:25:04
of some other portion of the body
00:25:06
what does that call whenever you have a
00:25:08
solitary cancer where some of the cancer
00:25:10
cells can break off and spread to other
00:25:13
areas of the body this is called
00:25:14
metastasis
00:25:16
and so having that process there
00:25:20
can be due to
00:25:22
mutations that involve these catherine
00:25:24
proteins so you see why that's actually
00:25:26
somewhat significant to think about okay
00:25:29
now let's talk about desmosomes all
00:25:30
right so let's talk about desmosomes the
00:25:32
desmosomes are actually a really cool i
00:25:34
want you to compare these similar to the
00:25:36
adherence junctions so they're really
00:25:38
good for shearing forces again a lot of
00:25:40
you know pretty much keeping cells
00:25:41
tightly together
00:25:43
a lot of abrasive forces they provide
00:25:44
resistance to that you know again
00:25:46
shearing and abrasive forces but they're
00:25:49
stronger than the adherence junctions so
00:25:51
when you're comparing you have tight
00:25:52
junctions adherence junctions and
00:25:55
desmosomes the strength actually of the
00:25:58
adhesion between the cells is stronger
00:26:00
as you're going in tight junctions to
00:26:02
adherence junctions to desmosomes okay
00:26:05
now what are the proteins that make up
00:26:07
the desmosome structure when you're
00:26:09
looking at it again you have these
00:26:10
proteins they're called cadherins
00:26:13
so cadherins again these are the
00:26:15
components of these proteins the red
00:26:17
ones that are from the cell membrane
00:26:20
they span outwards into the
00:26:22
extracellular space so these cadherins
00:26:25
here
00:26:26
they're really cool and there's these
00:26:27
proteins that kind of like connect
00:26:29
together almost like a zipper really and
00:26:31
they're really interesting there's two
00:26:32
types here
00:26:33
one is called desmoglian
00:26:38
and the other one is called desmocolon
00:26:43
so you have desmoglian and desmocolon
00:26:46
these are two types of cadherins that
00:26:49
are interlocking with one another in the
00:26:51
extracellular space now remember what i
00:26:53
told you
00:26:55
cad hearings
00:26:56
what does that mean they're calcium
00:26:58
dependent proteins so what are you gonna
00:27:00
have interlocking
00:27:02
these proteins together you're gonna
00:27:04
have calcium out here interlocking these
00:27:06
proteins together it's a very important
00:27:08
thing so from the extracellular side
00:27:11
spanning through the cell membrane into
00:27:13
the extracellular space you have
00:27:14
cadherins called desmoglian and
00:27:16
desmocolin and their calcium dependent
00:27:18
connection
00:27:20
then you have this big fat plaque
00:27:23
that actually is going to be anchoring
00:27:24
these down to the cytosolic part of the
00:27:26
cell membrane and this is called desmo
00:27:31
plaquen
00:27:33
so this is pretty much what's called the
00:27:34
plaque protein and the main component of
00:27:36
that is called the desmoplaquen
00:27:39
okay so this is kind of anchoring the
00:27:41
actual desmoglean and desmocolon to that
00:27:44
structure which is going to be again
00:27:45
more towards the actual in part like the
00:27:47
cytosolic membrane of that component
00:27:50
right so you have the cytosolic
00:27:51
component of the cell membrane that's
00:27:52
where the desmoplacken is primarily
00:27:54
anchored and then coming from that out
00:27:57
into the extracellular space is the
00:27:58
desmoclean and desmocolon proteins which
00:28:01
are calcium dependent connection
00:28:03
okay the next part which is actually
00:28:06
going to be on the inner side here which
00:28:07
really helps to hold these cells tightly
00:28:09
together this purple component here is
00:28:12
called your intermediate
00:28:14
intermediate filaments
00:28:17
and the main component here that's
00:28:20
really really important is called
00:28:22
keratin
00:28:24
so it's keratin that's the main
00:28:25
intermediate filament
00:28:26
so
00:28:28
if i were to ask you again
00:28:30
the components of the desmosomes from
00:28:32
the extracellular space you have the
00:28:34
cadherins desmoglia and desmocol which
00:28:36
are calcium dependent then on the inner
00:28:39
cytosolic component of the cell membrane
00:28:40
of cell one cell two is the plaque
00:28:43
protein which is mainly desmoplacan and
00:28:45
then all the way in the cytosol spanning
00:28:47
into it is the intermediate filaments
00:28:49
which is primarily keratin
00:28:52
now we already said a little bit here is
00:28:54
that these particular desmosomes are
00:28:57
really good for
00:28:58
high
00:29:00
tensile
00:29:02
stress and stretch right so anything
00:29:04
that's going to be involving a lot of
00:29:05
stretch
00:29:06
anything for a lot of your abrasive
00:29:10
anything with high abrasive and kind of
00:29:13
shearing forces is what these things are
00:29:15
really good at so any abrasive
00:29:18
shearing forces
00:29:20
these are extremely extremely good at
00:29:23
okay
00:29:24
now
00:29:25
there's
00:29:26
two particular types of tissues that i
00:29:27
want you to remember okay there's a lot
00:29:30
of them but there's two particular types
00:29:32
that i really don't want you guys to
00:29:33
forget
00:29:34
desmosomes are highly populated within
00:29:37
your cardiac tissue
00:29:39
so they're highly populated within the
00:29:41
cardiac tissue
00:29:42
and there is a special name for these
00:29:45
desmosomes that are located in the
00:29:47
cardiac tissue
00:29:48
and we'll talk about them
00:29:50
when you have these cardiac myocytes and
00:29:52
they're connecting from one another
00:29:54
we you know heart tissue has to be able
00:29:56
to stretch accommodate blood coming into
00:29:58
it
00:29:59
so what you want is you don't want those
00:30:01
cardiac myocytes to separate from one
00:30:02
another so they have to be able to
00:30:04
accommodate a decent amount of stretch
00:30:06
so what happens is there is a very
00:30:07
specific name
00:30:10
for this thing
00:30:11
and when we have these they're called
00:30:14
inter
00:30:16
collated
00:30:19
disks
00:30:20
and basically what these things are is
00:30:22
there are two components there's the
00:30:24
desmosomes which is what we're talking
00:30:26
about now and there's one more thing and
00:30:29
that is called
00:30:31
gap junctions and we're going to talk
00:30:32
about that in a little bit
00:30:34
but these are the two components that
00:30:36
make them up in the cardiac tissue and
00:30:39
again very very high yield don't forget
00:30:40
this intercalated discs
00:30:43
so we have cardiac tissue the other one
00:30:45
is the skin very very important
00:30:47
especially for the clinical significance
00:30:49
so i don't want you guys that it's also
00:30:50
know that it's important for your skin
00:30:52
tissue especially the epidermis so it
00:30:54
helps to connect the epidermal cells to
00:30:56
one another
00:30:57
why is this important well you know
00:30:59
there's a disease
00:31:01
it's a very interesting one it's called
00:31:02
pemphigus vulgaris you're like what
00:31:05
pemphigus
00:31:07
vulgaris
00:31:08
this is an autoimmune disease
00:31:11
and
00:31:12
what happens is your actual immune
00:31:13
system cells your plasma cells they make
00:31:15
auto antibodies
00:31:17
against their own tissues but guess what
00:31:19
those proteins are that it's attacking
00:31:21
these antibodies love to attack the
00:31:23
desmosomes specifically the desmoglian
00:31:28
and when you actually separate the
00:31:30
desmoglin when you destroy that then
00:31:32
these two cells aren't able to connect
00:31:34
well with one another
00:31:35
and they start separating and when the
00:31:38
epidermal cells start separating from
00:31:40
one another guess what you get
00:31:42
you get a nasty blistering ulcerative
00:31:44
type of disease and that's what this
00:31:47
disease is it's an autoimmune kind of
00:31:49
skin condition it's a blistering disease
00:31:51
that's due to the destruction of the
00:31:54
desmoglin proteins which is basically
00:31:57
the desmosomes and these can cause nasty
00:32:00
blisters
00:32:02
and ulcers
00:32:04
and one of the biggest things that
00:32:05
differentiate from the other one we're
00:32:06
going to talk about is this usually
00:32:08
involves the oral mucosa whereas the
00:32:10
other one does not involve the oral
00:32:11
mucosa
00:32:13
okay that's the desmosomes now let's
00:32:15
talk about hemidesmosomes all right
00:32:17
let's talk about the next type of cell
00:32:18
junction now this one's actually kind of
00:32:19
a tricky one because it's not
00:32:20
technically a cell to cell junction it's
00:32:22
actually a cell to extracellular matrix
00:32:25
junction or cell to basal lamina
00:32:27
junction but that's actually nice
00:32:29
because it's an easy one to remember
00:32:30
because it's not a cell true cell to
00:32:32
cell junction
00:32:33
so what are the components of the
00:32:35
hemidesmosomes all right there's a
00:32:37
couple different proteins so remember
00:32:40
this is not a cell to sell so let's call
00:32:42
let's let's actually label this this is
00:32:44
cell right we can sell one doesn't
00:32:46
really matter but it's a cell and then
00:32:48
this blue component here is what's
00:32:49
called the basal
00:32:51
lamina and there's a bunch of different
00:32:53
proteins of the basal lamina right if
00:32:55
you were to list some of them you'll
00:32:56
have things like fibronectin
00:32:59
i'll list a couple of them fibronectin
00:33:01
is a good one
00:33:02
can't go wrong with laminin
00:33:05
and another one that's always a big one
00:33:08
is collagen so these are some of the
00:33:10
proteins that are involved in the
00:33:12
extracellular matrix of the basal lamina
00:33:14
right
00:33:16
this is the connection the
00:33:17
hemidesmondosome is the connection to
00:33:20
the basal lamina made up of these
00:33:21
different types of proteins
00:33:23
to the actual cell membrane okay
00:33:26
now what are the components of it all
00:33:29
right so
00:33:30
the basal lamina i'm just having these
00:33:32
blue things the proteins like the
00:33:33
fibronectin the lamina and the collagen
00:33:35
it's coming up and connecting to this
00:33:36
purple component that is connected to
00:33:38
this cell what is this purple component
00:33:41
here that's really the big thing and
00:33:43
this purple component here is called
00:33:45
integrins
00:33:46
they're called integrins
00:33:48
okay that's really the biggest thing
00:33:50
that you guys need to remember out of
00:33:51
the hemi now is desmond is that the
00:33:53
integrins are the protein that spans
00:33:57
through the entire cell membrane of this
00:33:59
cell and
00:34:00
connects the cell here to the
00:34:03
extracellular matrix
00:34:05
which is the basal lamina consisting of
00:34:07
fibronectin laminin collagen all of
00:34:10
these different types of extracellular
00:34:12
proteins
00:34:13
what's the proteins
00:34:15
on the inner cytosolic side of the cell
00:34:18
membrane that is helping to anchor that
00:34:20
actual transmembrane protein or the
00:34:22
integrins down
00:34:24
this orange proteins are basically the
00:34:26
same thing as the desmosomes they're
00:34:29
intermediate
00:34:32
filaments and this could include
00:34:36
keratin
00:34:38
okay so this would include keratin
00:34:41
that is the basic thing of this
00:34:43
structure so when we're talking about
00:34:45
the components of the hemidesmosomes the
00:34:48
basal lamina which has fibronectin
00:34:50
lamina and collagen it's connected to
00:34:52
the integrins which are the protein that
00:34:54
is actually spanning through the cell
00:34:56
membrane coming out and connecting to
00:34:58
the basal lamina and on the inner
00:35:00
cytosolic side of that cell membrane
00:35:03
there's the intermediate filaments are
00:35:04
keratin proteins okay
00:35:07
what is the different
00:35:10
basic functions really it's super simple
00:35:13
because when we talk about these
00:35:14
hemidesmosomes they're basically helping
00:35:17
to form
00:35:19
what's called your basement membrane
00:35:23
okay it's basically helping to form the
00:35:25
basement membrane which is just this
00:35:27
connection of the basal lamina to the
00:35:30
epithelial cells of different tissues
00:35:32
that's all it is it maintains that
00:35:35
connection between the basal lamina and
00:35:37
the epithelial tissue above it that
00:35:39
forms the basement membrane that's it
00:35:41
nothing crazy so
00:35:43
could you imagine there's a nasty
00:35:45
disease because really the big places
00:35:48
that i really want you guys to think
00:35:49
about this is the skin it's the easiest
00:35:51
one that makes the most clinical
00:35:52
relevance so the skin is a big one right
00:35:56
but any other type of epithelial tissue
00:35:58
your epithelial tissue the respiratory
00:36:00
tract epithelial tissue of the gi tract
00:36:01
epithelial tissue the urogenital tract
00:36:03
any of those epithelial tissues are
00:36:04
going to have this i think the skin is
00:36:06
the easiest one to remember though
00:36:08
but again remember it's any of the
00:36:09
epithelial tissues that are lining your
00:36:11
gi tract respiratory tract and
00:36:12
neurogenital tract
00:36:14
with the skin there's a very interesting
00:36:17
part process here so you know here this
00:36:19
is the epithelial tissue we call that
00:36:20
like the stratum basale
00:36:23
and then that anchors it down to the
00:36:24
dermis below it right well the anchoring
00:36:27
connection here if i were to really draw
00:36:28
it in this kind of like bluish color
00:36:30
right here this is really where
00:36:33
your basal lamina is
00:36:35
so
00:36:36
what if i had a disease
00:36:38
where my body has these plasma cells and
00:36:41
they make these auto antibodies that are
00:36:44
directed against the proteins the
00:36:46
entegrins
00:36:48
that connect the basal lamina to the
00:36:50
epithelial cells and my antibodies go
00:36:53
and destroy that connection so what
00:36:55
would the antibodies do they would
00:36:57
destroy this connection right here i
00:36:59
would no longer have integrins anchoring
00:37:01
the cells to the base membrane and these
00:37:03
cells would separate so imagine me
00:37:05
forming a separation between those two
00:37:07
that's going to form blisters and nasty
00:37:10
ulcers okay what is that disease called
00:37:13
it's called bolus
00:37:16
pemphigoid
00:37:20
bolus pemphigus so these are basically
00:37:22
what's called sub
00:37:24
epidermal
00:37:26
blisters
00:37:27
that can actually ulcerate whenever you
00:37:29
kind of rub them they call it the
00:37:30
positive nikolsky sign we'll talk about
00:37:33
it more with derm but these usually
00:37:35
spare the oral mucosa and they involve
00:37:38
like the axilla they involve like the
00:37:39
anal genital area and the different
00:37:42
inguinal areas and sometimes even the
00:37:44
trunk as well
00:37:45
but
00:37:46
this is the clinical significance is
00:37:47
that these anchor the actual epithelial
00:37:50
cells to the basement or to the basal
00:37:51
lamina forming the basement membrane if
00:37:53
you have an auto antibodies that are
00:37:55
destroying that it can separate them
00:37:56
from these sub-epidermal blisters and
00:37:58
the condition is called bolus pemphigoid
00:38:01
we finished talking about the
00:38:02
hemidesmosomes let's hit it home with
00:38:04
the gap junctions all right instead of
00:38:05
the last cell junction that we got to
00:38:07
talk about here is gap junctions these
00:38:09
are really cool junctions now the
00:38:11
biggest thing to remember is that these
00:38:13
aren't really for
00:38:14
blocking the movement they're not really
00:38:15
a diffusion barrier like tight junctions
00:38:17
they're not really designed to be able
00:38:19
to resist kind of abrasive and shearing
00:38:21
forces like the adherence junctions and
00:38:23
like the desmosomes and they're not
00:38:25
really anything that's connecting
00:38:27
another cell to a connective tissue
00:38:29
these are primarily allowing for cell to
00:38:31
cell communication which is so cool now
00:38:33
what are the different components in the
00:38:34
structures and proteins involved here so
00:38:37
this whole thing here is called a gap
00:38:38
junction but a gap junction is actually
00:38:41
made up of two particular types of
00:38:43
proteins so when we take a gap junction
00:38:46
it's actually made up of what's called
00:38:48
conexons
00:38:51
connexons and there's two of them
00:38:53
basically so two connexons make up a gap
00:38:57
junction so imagine here this whole
00:38:59
thing here
00:39:01
this whole component so here's cell one
00:39:04
and here's cell two if you look right
00:39:06
here this right here
00:39:08
is one connexon
00:39:11
so this is one connexon and then right
00:39:14
here to this component right here this
00:39:16
is a another connexon
00:39:19
these two together are what make up a
00:39:23
gap
00:39:24
junction
00:39:25
now what's really interesting about this
00:39:29
is that when you actually zoom in on a
00:39:30
connexon
00:39:32
a connexon just one of these connexons
00:39:35
is made up of six this is so annoying
00:39:37
right two three four five six connexins
00:39:43
so when we talk about what a connexin is
00:39:46
so here we have what's called a connexin
00:39:50
it's made up of what's called connects
00:39:54
ends and how many six of them so let's
00:39:57
kind of recap this
00:39:58
a gap junction is connexons two of them
00:40:03
and a connexon
00:40:05
is actually what six connexins together
00:40:08
that make this big protein
00:40:10
so if you want to think about how many
00:40:12
total connections would make up a gap
00:40:14
junction 12 right because you need one
00:40:16
connexon another connexon and each one
00:40:18
of them is six
00:40:20
so what is the whole purpose to know out
00:40:23
of this
00:40:24
well these gap junctions which are made
00:40:26
up of two connexons and one connexon is
00:40:28
made of six connexins
00:40:30
is allowing for cell
00:40:33
to cell communication
00:40:35
and that is what's so cool about these
00:40:38
so if you have for example you have a
00:40:41
cation like sodium
00:40:42
or calcium these ions can move from this
00:40:46
cell to the next cell
00:40:48
and allow for that ion
00:40:50
transfer and that can be important in
00:40:52
certain types of cells that are
00:40:53
excitable so what kind of cells would
00:40:55
this be really really important in where
00:40:58
it's going to be cells where i want them
00:40:59
to be really excitable right and i want
00:41:01
them to be able to propagate those
00:41:03
electrical potentials onto other cells
00:41:05
nearby
00:41:06
so that would be a big deal in cardiac
00:41:08
tissue
00:41:09
in smooth muscle tissue or even in
00:41:11
certain types of neurons those are
00:41:13
excitable cells and we need that
00:41:15
propagation of electrical activity which
00:41:17
can be made via these gap junctions or
00:41:20
cell to cell communications so tissues
00:41:22
where this can be important in
00:41:24
is going to be your cardiac tissue
00:41:28
lots of gap junctions there but again
00:41:30
what do we call those because remember
00:41:32
cardiac tissue actually has what's
00:41:33
called intercollated discs which are
00:41:36
desmosomes and gap junctions
00:41:39
the other tissue would be your smooth
00:41:41
muscle tissue
00:41:44
so you know smooth muscle tissue
00:41:45
obviously a good example of this is your
00:41:47
gastrointestinal tract but you also have
00:41:49
smooth muscle within the respiratory
00:41:51
tract
00:41:53
and you also have smooth muscle within
00:41:54
the euro genital tract
00:41:57
so any type of smooth muscle even in
00:41:59
your blood vessels you actually have
00:42:00
again smooth muscle
00:42:02
so again all of these would be
00:42:03
particular is cardiac muscle smooth
00:42:05
muscle what else
00:42:06
neurons
00:42:07
certain types of neurons is also going
00:42:09
to be a big one so some specific types
00:42:12
of neurons actually do communicate via
00:42:16
gap junctions now
00:42:19
not only does it allow for ions to move
00:42:22
from cell to cell but it can also allow
00:42:24
for certain types of proteins or second
00:42:26
messenger molecules to move from cell to
00:42:28
cell you notice uh there's other things
00:42:30
you know it's called cyclic amp you guys
00:42:33
have heard that right cyclic amp it
00:42:35
activates things like protein kinase a
00:42:37
there's another molecule called ip3
00:42:41
all of these different types of
00:42:42
molecules these are like cell signaling
00:42:44
molecules right and basically if they're
00:42:46
let's say that you have some type of
00:42:48
stimulus let's say here's some type of
00:42:49
molecule
00:42:50
and it acts on a receptor on this cell
00:42:53
so here's a receptor on this cell
00:42:56
when this molecule stimulates this it
00:42:58
can activate these particular molecules
00:43:00
exciting this cell
00:43:02
well maybe this cell would want to let
00:43:04
the other cell know and so not only can
00:43:07
ions move from cell to cell but we can
00:43:09
also have certain types of
00:43:11
signaling molecules like cyclic amp ip3
00:43:13
other types of cytokines
00:43:15
which can alert the cells nearby
00:43:18
why would that be important let's say
00:43:20
for example
00:43:22
let's say you had a cell here and let's
00:43:23
say here's a
00:43:24
pathogen here's a pathogen
00:43:27
and this actual cell gets infected by
00:43:29
this pathogen alright so now this cell
00:43:32
is infected
00:43:33
what this cell could do
00:43:35
is it could do a couple things it could
00:43:37
tell the cell nearby hey go ahead and
00:43:39
make some specific anti-microbial
00:43:41
proteins against this pathogen and it
00:43:44
very well could do that
00:43:46
but it also could say to the nearby cell
00:43:47
hey man there's a virus nearby there's a
00:43:49
pathogen nearby you just need to go
00:43:51
ahead and kill yourself
00:43:53
and it may actually trigger that cell to
00:43:55
undergo a programmed cell death to
00:43:57
prevent it from being infected by that
00:43:59
pathogen
00:44:00
and so what it can do is it can signal
00:44:02
certain types of molecules nearby
00:44:05
maybe certain types of cytokines and
00:44:07
tell them hey
00:44:08
time to trigger
00:44:10
what's called
00:44:12
apoptosis
00:44:15
which is that programmed cell death
00:44:17
process to be able to protect that cell
00:44:20
and say hey we don't want this cell to
00:44:21
have another reservoir for this virus to
00:44:24
continue to keep populating and making
00:44:25
more and more viruses just go ahead and
00:44:27
die so that we can prevent that actual
00:44:29
virus from being able to have cells as a
00:44:31
reservoir to continue to keep making
00:44:33
viruses
00:44:34
and that may be a process that occurs
00:44:36
and that can happen not only
00:44:38
by certain types of molecules being
00:44:40
released extracellularly
00:44:42
things like interferons and letting
00:44:44
these cells know but it can happen via
00:44:46
these gap junctions communicating with
00:44:48
the nearby cells saying hey some stuff's
00:44:50
going on go ahead and prepare yourself
00:44:51
for that
00:44:52
and so not only is the function of gap
00:44:54
junctions allowing for ions to move from
00:44:56
cell to cell allowing for electrical
00:44:57
communication
00:44:59
but also it's important for being able
00:45:01
to allow for cell to cell communication
00:45:02
to trigger apoptosis to trigger maybe
00:45:04
certain cellular adaptive processes to
00:45:07
undergo hypertrophy atrophy maybe
00:45:10
whatever it may be but allows for that
00:45:11
cell to cell communication and it's a
00:45:13
very cool protective response and that
00:45:15
my friends finishes our lecture on cell
00:45:18
junctions i hope it made sense i hope
00:45:19
that you guys enjoyed it and as always
00:45:21
ninja nerds until next time
00:45:27
[Music]
00:45:43
you