IDTH 201 Epithelia PDF

Summary

These notes cover epithelial cell characteristics, classification (simple and stratified), cell shapes (squamous, cuboidal, columnar), and special categories (pseudostratified, endothelium, mesothelium). It also examines the structure-function relationship of epithelia, including secretion, absorption, transportation, protection, and receptors. The document details cell polarity (apical, lateral, basal) and surface modifications like microvilli, stereocilia, and cilia.

Full Transcript

**IDTH 201 -- Exam 3 Material**

**Epithelium**

Epithelia lines body surfaces and cavities and constitutes the secretory
portion of glands (parenchyma) and their ducts.

It is a tightly cohesive sheet of cells, and it is avascular.

There are specialized epithelial cells that are receptors for special
senses.

I. **Epithelial Cell Characteristics:**

1. Closely adhering to one another by means of specific cell-to-cell
adhesion molecules (junctions).

2. They exhibit functional and morphological polarity.

Different functions are associated with 3 distinct morphological
surface domains:

a. Free surface domain or apical domain open towards lumen.

b. Lateral domain.

c. Basal domain attached to BM a non-cellular protein polysaccharide
layer.

The properties of each domain are determined by specific lipid surface
membrane proteins.

Example of **thick ascending limb** and **distal convoluted tubule**:
the apical domain contains different transporters and channels. The
thick ascending limb has different distribution of transporters and
channels compared to the distal convoluted tubule.

In the same nephron, we can see two different distributions of cells
which means two different functions.

3. Epithelia can be classified as simple or stratified.

A single layer Used for exchange mainly.

Multiple layers More involved in protection.

Note epithelia has high innervation, high mitotic rate, and lies on BM.

II. **We can classify cells based on:**

1. Number of cell layers (simple or stratified)

2. Shape of the cell (Squamous, Cuboidal, or Columnar)

Cells in some exocrine glands are more or less pyramidal.

Their apical side (apsis) is directed toward the lumen.

However, these cells are still classified as either cuboidal or columnar
depending on their height relative to their width at the base of the
cell.

In some instances, there is specialization of the apical cell surface
domain.

Simple: one layer.

Columnar: there are the lateral sides which are longer than the apical
and basal side. If they have cilia or not.

Simple columnar ciliated when the apical domain has cilia.

Same principle applies to stratified squamous epithelium, in which the
surface cells can be keratinized or non-keratinized.

Stratified squamous keratinized epithelium because keratinized cells are
on the apical side.

Stratified columnar has two layers, a basement membrane another cuboidal
layer then another columnar layer. **It is the last layer towards the
apical side or the lumen that will dictate the name of the epithelium.**
Here the last layer towards the lumen is the columnar stratified
columnar.


**Some special categories of epithelia:**

**Pseudostratified epithelium:** Simple epithelium that appears
stratified. All of the cells rest on the basement membrane, yet some of
them will not reach the lumen. The distribution of pseudostratified
epithelium is limited in the body. It is often difficult to distinguish
whether all of the cells contact the lumen. Identification of
pseudostratified epithelium will depend on where it is normally found.

**Specific classes of epithelium:**

Endothelium: Epithelium lining the blood and lymphatic vessels.

Endocardium: Epithelium lining ventricles and atria of heart.

Mesothelium: Epithelium lining walls and covering content of closed
cavities of the body.

These are almost always simple squamous epithelia; an exception is the
postcapillary venules of certain lymphatic venules which have cuboidal
endothelium.

III. **Structure-Function Relationship:**

An epithelium may serve one or more function depending on the activity
of the cell type that are present.

**Secretion**: as in the **columnar epithelium of the stomach and the
gastric glands**.

**Absorption**: **columnar epithelium of the intestines and proximal
convoluted tubules** in the kidney.

**Transportation**: transport of materials or cells along the surface of
the epithelium by motile cilia or in the transport of materials across
an epithelium to and from the connective tissues.

**Protection**: several layers, **stratified squamous epithelium of the
skin** (epidermis) and the **transitional epithelium of the urinary
bladder** because urine contains all the toxins of our body.

**Receptors**: epithelium receives and transduces external stimuli as in
the taste buds of the tongue, olfactory epithelium of the nasal mucosa
and the retina of the eye.

Epithelia involved in secretion or absorption are typically simple, in
some cases they are pseudostratified which is also simple.

The height of the cells often reflects the level of secretory or
absorptive activity.

Simple squamous small distance between the basal and the apical side are
compatible with high rate of transepithelial transport.

Stratification of the epithelium usually correlates with transepithelial
impermeability.

In some pseudostratified epithelia, basal cells are the stem cells that
give rise to the mature functional cells of the epithelium thus
balancing cell turn-over.

IV. **Cell Polarity: Apical Domain**

- Apical domain (towards lumen).

- Lateral domain communicates with adjacent cells and it is
characterized by specialized attachment areas **tight junction**
which is always towards the apical side and the lumen.

It can be used to distinguish whether we are on the apical side or
not.

Also, there are **gap junctions** that allow communication between
cytoplasm of the epithelium which allows calcium to move for example
between one cytoplasm to the other.

- Basal domain rests on the basal lamina anchoring the cell to the
connective tissue.

Specific biochemical characteristics are associated with each cell
surface.

Toward the lumen on the apical domain there are special structure
surface modifications, and any structural change is going to be
transducing a functional change.

These structural changes are:

A. **Microvilli**: cytoplasmic processes containing a core of **actin
filaments**.

B. **Stereocilia** or stereovilli: microvilli of unusual length.

C. **Cilia**: cytoplasmic processes containing bundle of
**microtubules**.

A. **Microvilli**


They are fingerlike cytoplasmic projections which are found on the
apical surface of most epithelial cells. Microvilli vary widely in
appearance:

The number and shape of microvilli correlate with the absorptive state
of the cell.

When they are uniform, numerous, tall and regularly arranged their main
goal is to increase the free cell surface area for absorption.

Cells that transport fluid and absorb metabolites have many closely
packed tall microvilli intestine cells are absorptive cells and
microvilli play a major role in exchange.

Cells in which transepithelial transport is less active have smaller
more irregular shaped microvilli.

Microvilli that are uniform, numerous, and regularly arranged form a
straited border or a brush border.

A cell cannot increase in size except when it undergoes hypertrophy so
to increase the surface of exchange they have microvilli.


20-30 actin filaments, anchored to **villin** on the top.

Actin bundles extend down into the apical cytoplasm, and they interact
with a horizontal network of actin filaments called the **terminal
web**.

They are cross-linked by ABP like **espin** and **fimbrin**.

This cross-linkage provides support and give rigidity to the microvilli.
In addition, the core of actin filaments is associated with **myosin
I**, a molecule that binds the actin filaments to the plasma membrane of
the microvillus.

The addition of villin to epithelial cells growing in culture induces
formation of microvilli on the free apical surface.

The terminal web is composed of actin filament stabilized by
**spectrin**.

The presence of **myosin II and tropomyosin** in the terminal web
explain the contractile ability of the microvilli. These proteins
decrease the diameter of the apex of the cell causing the microvilli to
spread apart and increase the inter-microvillus space allowing more
exchange.

B. **Stereocilia**

They are long, non-motile microvilli.

They are not widely distributed through epithelia, they mostly belong to
the **epididymis**, the **proximal part of the ductus deferens** of the
male reproductive system and the **sensory cells of the inner ear**.

They extend from the apical surfaces of the cell and in some cases, they
facilitate absorption.

They are supported by internal bundles of actin
filaments, crosslinked by **fimbrin**. They are bound to the membrane by
ABP **ezrin**, and they **do not have villin**!

They are anchored to the apical site of cytoplasm by **alpha actinin**
in the terminal web.

Microvilli are present in many epithelial cells, they increase
absorptive surface of the cells, they are visible in light microscopy as
**straited borders or brush borders**. Stereocilia have limited
distribution, they are found in the male reproductive system and in
sensory hair cells in the inner ear and they function as
mechanoreceptors.

C. **Cilia**

Common surface modification present on nearly every cell in the body.
They are hair-like extensions of the apical plasma membrane, and contain
an **axoneme**, a **MT**- based internal structure.

They are much longer and different in structure than microvilli.


Axoneme of cilium extends from the basal body MTOC. Basal bodies are
associated with several accessory structures that help them in
anchoring.

Functions of cilia:

Based on functional characteristics, we can classify cilia into:

1. Motile cilia

Found in large numbers and have a 9+2 axonemal arrangement.

2. Primary cilia

Immotile solitary projections found on almost all eukaryotic cells. They
function as chemosensors, osmosensors, and mechanosensors.

3. Nodal cilia

Found on embryo bilaminar disk at gastrulation, area around primitive
node. They have similar axonemal architecture as primary cilia, but they
can also rotate!

1. *Motile Cilia*

- Motile cilia possess an internal structure that allows them to move
fluid and particles along epithelial surfaces (i.e. trachea,
bronchi, oviduct).

- Motile cilia appear as short, thin hair like structures and in the
middle we see a thin dark staining band which is known as the
**basal body**.

- Internal core of microtubule is called axoneme.

- A cross sectional view will reveal a characteristic configuration of
motile cilia made of nine pairs or doublets of circular arranged
microtubules surrounding two central microtubules.

- The wall of one MT (B) appears incomplete because it shares a
portion of the wall of MT (A).

- Elastic band of **nexin** links A to B.

- The central MTs are enclosed partially by an **inner sheath**, and
the **radial spoke** extends from each doublet to the central MTs.

- Cilia movement originates from the sliding of microtubule doublets
which is generated by the ATPase activity of the **outer and inner
dynein arms** that go from A to B. Cilia beat in a synchronous
pattern, they display a precise and synchronous movement.

2. *Primary Cilia*

- Immotile, move passively by fluid motion.

- Have an arrangement of 9+0 no central MTs.

- Lack microtubules-associated motor proteins needed to generate
motile force.

- The axoneme originates from a basal body that ressembles a
mature centriol positioned orthogonally in relation to its
immature counterpart.

- Primary cilium formation is **synchronized with cell cycle
progression** and centrosome duplication events.

- Found in epithelial cells of the biliary tract, kidney tubules,
etc.

- Function as receptors sensing fluid flow.

- Function in secretory organs (kidney, liver, pancreas) as
sensors of body flow.

3. *Nodal Cilia*

- Motile.

- 9+0 pattern of microtubules.

- Play a role in early embryonic development since they generate the
left-right asymmetry of internal organs.

- Contain motor proteins and capable of rotational movement.

Correlate structure with function of human cilliary disease genes.

D. **Flagella**

They are present in human body only in spermatozoa.

They are similar in structure to cilia, longer, and are limited to one
per cell.

V. **Cell Polarity: Lateral Domain**

Lateral domain of epithelial cells is in close contact with other
lateral domain of adjacent cells.

Characterized by presence of specific cell adhesion molecules CAMs.

The molecular composition of lipids and proteins forming the cell
membrane of the lateral domain are significantly different from those
that form the apical cell membrane.

 Lateral cell surface may form folds and
processes, invaginations and evaginations that create interdigitating
and interleaving tongue-and-groove margins between neighboring cells.

Junctional complex:

Zonula occludens or tight junction

Zonula adherens or belt desmosomes

Macula adherens or desmosomes

Hemidesmosomes

Note that occluding or tight junctions indicate polarity of the cell.

A. **Occluding Junctions**

In some places of the body, they are permeable and allow cells to
function as a barrier leaky.

Form the primary intercellular diffusion barrier between adjacent cells.

Main functions:

- Form a tight seal and prevent migration of lipids and specialized
membrane proteins between the apical and lateral surfaces = they
prevent the paracellular route of transport maintaining the
integrity of these two domains + they mantain physiochemical
seperation of tissue compartments.

- Recruit signaling molecules to the cell surface and link them to the
actin filaments of the cell cytoskeleton.

Tight junctions in EM: you will see a region in the plasma membrane of
adjoining cells that come in close contact to seal off intercellular
space.

The zonula occludens appear not as a continuous series but as a series
of focal fusion between the cell. This focal fusion are created by
transmembrane proteins of adjoining cells that join in the intercellular
space.

The presence of the tight junction and its ability to create a diffusion
barrier will create two distinct pathways:

Transcellular: Exchange goes through the apical and basal sides. It
requires energy. Example of active transporter Na+/K+ pump on
basolateral membrane.

Paracellular: Capable of diffusing ions based on the tightness of zonula
occludens.

B. **Zonula Adherens and Macula Adherens**

Anchoring junctions provide lateral adhesions between epithelial cells,
using proteins that link into the cytoskeleton of adjacent cells:

Zonula adherens: Interact with actin filaments.

Macula Adherens: Interact with IF.

Other anchoring junctions where epithelial cells rest on CT are focal
adhesions and hemidesmosomes.

**Zonula** **Adherens**

An adherens junction is defined as a cell junction whose cytoplasmic
face is linked to the **actin cytoskeleton**. They can appear as bands
encircling the cell (zonula adherens) or as spots of attachment to the
extracellular matrix (adhesion plaques). 

The cell adhesion molecules form an essential part of every anchoring
junction on both lateral and basal cell surfaces. The extracellular
domain of cell adhesion molecules interact with similar domains
belonging to the cell adhesion molecules of neighboring cells.

If the binding occurs between different types of CAMs it is described as
heterotypic binding. When the binding occurs between the same type of
CAMs it is described as homotypic binding.

CAM have a selective adhesive characteristic of relatively low strength
which will allow cells to easily join and dissociate. The cytoplasmic
domains are linked through a variety of intracellular proteins to
components of the cell cytoskeleton. Through the cytoskeleton
connections, CAMs are able to control and regulate diverse intracellular
processes associated with:

- Cell adhesion

- Cell proliferation

- Cell migration

The three CAMs are integrated in many cellular functions such as:

- Intercellular and intracellular communication

- Cell recognition

- Regulation of intercellular diffusion barrier

- Generation of immune response

- Apoptosis

**CAMs are divided into four major factors:**

1. **Cadherins**: Transmembrane calcium dependent CAMs localized mainly
within the zonula adherens. At this site they maintain homotypic
interactions with similar protein from the neighboring cells. They
are associated with a group of proteins **catenin** that links
cadherin molecules to actin filaments of the cell cytoskeleton.
Through this interaction, cadherins convey signals that regulate
mechanism of growth and cell differentiation. Cadherins control cell
to cell interaction, they participate in cell recognition and
embryonic cell migration. E-cadherin is the most studied member of
this family, it maintains the zonula adheren junction between
epithelial cells. It also acts as an important suppressor of
epithelial tumor cells.

2. **Integrins**: Represented by two transmembrane glycoprotein
subunits consisting of 15 alpha and 9 beta chains. This composition
allows for the formation of different combination of integrin
molecules that are able to interact with various proteins. Integrin
interacts with EM molecules and with actin and intermediate
filaments of the cell cytoskeleton. By these interactions, integrin
regulates: cell adhesion, control cell movement and shape,
participate in cell growth and differentiation.

3. **Selectins**: Expressed on white blood cells and endothelial cells.
They mediate neutrophil endothelial cell recognition. This
heterotypic binding initiates neutrophil migration through the
endothelium of blood vessel into the extracellular matrix. They are
also involved in directing lymphocytes into accumulation in
lymphatic tissues.

4. **Immunoglobin Superfamily**: many molecules involved in immune
reactions share a common precursor element in their structure. Yet,
several other molecules with no known immunological function also
share the same repeat element. Together the genes encoding these
related molecules have been defined as the immunoglobulin gene
family. It is the largest gene families in the human genome and its
glycoproteins perform a wide variety of important biological
functions.

**Macula Adherens or Spot Desmosomes**

They represent a major anchoring cell-to-cell junction that provides a
particularly strong attachment.

The macula adherence was originally described in epidermal cells where
we start calling them desmosomes. These junctions localize on the
lateral domain of the cells. They are much like a series of spot wells
and they mediate direct cell-to-cell contact by providing anchoring site
for **intermediate filaments.**

They are distributed in patches along cell lateral membrane of most
epithelial cells.

Also called anchoring junctions, we have cell-to-extracellular-matrix
junction.

They maintain the **morphological integrity** of the epithelium
connective tissue interface. You have the **focal adhesions** that
anchor actin filament of the cytoskeleton into the basement membrane,
and you have **hemidesmosomes** that anchor intermediate filaments of
the cytoskeleton into the basement membrane.

C. **Communicating Junctions or Gap Junctions**

Gap junctions are the only known cellular structure that permits a
**direct passage of signaling molecules from one cell to another**.

Calcium can go from one cytosol to the other cytosol using gap junction.
They are present in a wide variety of tissues, including **epithelia**,
**smooth and cardiac muscle**, and **nerves**.

Cardiac junction are important tissue in which activity in adjacent cell
must be coordinated very tightly. The gap junction consists of an
accumulation of transmembrane channels or pores in a tightly packed
area. It allows cells to exchange ions, regulatory molecules, and small
metabolites through the pores.

The number of pores in gap junction can vary widely, as can the number
of gap junction between adjacent cells.

They are pores, and these pores are formed by 12 subunits of the
connexin protein family to form the connexins.

So when you view gap junction under electron microscope, they appear as
an area of contact between the plasma membrane of adjacent cells, and
they reveal groups of tightly packed channels, each formed by two half
channels called connexins embedded in the facing membrane.

The connexin in one cell membrane is precisely aligned to dock with the
corresponding connexin on the membrane of an adjacent cell. Each
connexin contains six symmetrical subunits of membrane proteins called
connexins.

VI. **Basal Domains**

It is characterized by several features. The basement membrane is a
specialized structure located next to the basal domain of epithelial
cells and the underlying connective tissues. Cell-to-extracellular
matrix junction anchors the cell to the extracellular matrix.

They are represented by **focal adhesions** and **hemi-desmosomes**.

Basal cell membrane enfolding that increase the cell surface area and
facilitate morphologic interaction between adjacent cells and
extracellular matrix proteins.

The term basement membrane is used to specify a **periodic acid shift
positive layer** visible with light microscope beneath epithelial. The
basement membrane is usually formed by the **fusion of either two basal
laminas or a basal lamina and a reticular lamina/lamina lucida**.


The basement membrane is defined by two layers, a **basal lamina**
containing **laminin**, **fibronectin**, **type IV collagen**,
**heparensulfate** **proteoglycans**, and a **reticular lamina**
containing **type III collagen**, or reticular fibers.

The components of these two lamina are **glycoproteins**, and they are
**periodic acid shift positive**.

VII. **Glandular Epithelia**

Glands are classified into two major groups and this classification is
based on how their products are released.

Glandular epithelia are cells that produce **fluid** secretion.

They produce a fluid that is different than the extracellular fluid
blood.

They produce a fluid that is different than the intracellular fluid.

They are characterized by presence of **secretory granules** inside the
cell.

They may synthesize, store, and secrete:

Proteins like the pancreas.

Lipid like the adrenal gland.

Complexes of carbohydrate plus protein like salivary gland.

Also they can secrete proteins, lipids, and complexes of carbohydrates
and protein like the mammary gland.

Some other epithelial cells are ion-transporting cells, example the
striated duct.

The types of glandular epithelia are:

- Exocrine glands.

- The exocrine secrete their products onto a surface directly or
through epithelial ducts or tube that are connected to a surface.
The ducts convey the secreted material in a unilateral form or may
modify the secretion by concentrating it or adding or reabsorbing
constituents substances.

- Endocrine glands.

- The endocrine glands, they lack a duct system. They secrete their
product into the connective tissue from which they enter the
bloodstream to reach their target cells. The products that you know
is called hormones.

- Mixed.

The liver is one of the best examples.

The cells of exocrine gland exhibit different mechanism of secretion:

1. **Merocrine** **secretion**: This secretory product is delivered in
**membrane-bounded vesicles** to the apical surface of the cell. The
vesicles here fuse with the plasma membrane and extrude their
content by exocytosis. This is the most common mechanism of
secretion and it is found for example in the **pancreatic acinar
cells**.

2. **Apocrine secretion**: The secretory product is released in the
apical portion of the cell surrounded by **a thin layer of
cytoplasm** within an envelope of plasma membrane. This mechanism of
secretion is found in the lactating **mammary gland** where it is
responsible for releasing large lipid droplets into the milk. It
also occurs in the **apocrine glands of skin**, **ciliary glands of
the eyelid** and other places.

3. **Holocrine** secretion: The **secretory product accumulates within
the maturing cell** which simultaneously undergoes programmed cell
death. Both secreted product and cell debris are discharged into the
**lumen of the gland**. This mechanism is found in the **sebaceous
gland of skin** and in the **glands of the eyelid**.

VIII. **Epithelial Cell Renewal**

Most epithelial cells have a finite lifespan.

The rate of cell turnover is different, it can be fast like in the
intestinal epithelium or slow like in the pancreas.

Also it should be emphasized that some cells like special epithelial
cells are hard to be renewed like podocyte.

Metaplasia is when one type of epithelia transforms into another type
(reversible):

- In smokers (heavy), the pseudostratified becomes stratified squamous
epithelia.

- In chronic Vit A deficiency, the epithelium of bronchi or urinary
bladder becomes stratified squamous epithelia.