Endoplasmic Reticulum (ER) PDF

Summary

This document provides an overview of the endoplasmic reticulum (ER). It covers the endomembrane system, the different functions of rough and smooth ER, and the pathways involved in protein synthesis. It also discusses the roles of chaperones and the unfolded protein response. Includes topics such as protein transport, glycosylation, and lipid metabolism.

Full Transcript

BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

TOPIC 7: THE ENDOPLASMIC RETICULUM (ER)
1. THE ENDOMEMBRANE SYSTEM

2. THE ENDOPLASMIC RETICULUM (ER)
2.1. Rough Endoplasmic Reticulum (RER)
2.2. Smooth Endoplasmic Reticulum (SER)

3. SECRETORY AND CYTOSOLIC PATHWAYS FOR PROTEIN SYNTHESIS 3.1. Cytosolic
pathway 3.2. Secretory pathway

4. RER: THE START OF THE SECRETORY PATHWAY

5. CYTOSOLIC vs. RER POLYRIBOSOMES
5.1. Characteristics

6. TRANSLOCATION OF PROTEINS
6.1. Synthesis of water soluble proteins
6.2. Synthesis of transmembrane proteins
6.3. Glycosylation

7. FOLDING AND QUALITY PROTEINS
7.1. Chaperons and protein folding
7.2. The unfolded protein response (UPR)

8. SMOOTH ENDOPLASMIC RETICULUM (SER)
8.1. Cytochrome p450 system
8.2. Membrane lipid biosynthesis in the SER

9. INTEREXCHANGE OF LIPIDS BETWEEN THE ER AND OTHER ORGANELLES

10. OTHER ER FUNCTIONS: STORAGE OF Ca2+

1. THE ENDOMEMBRANE SYSTEM

The endomembrane system consists of a group of
organelles which are interconnected through transport
vesicles and work together to modify, package and
transport lipids and proteins. They are independent but
work together.

- These organelles are the endoplasmic Reticulum,
(nuclear envelope), the golgi apparatus, endosomes,
phagosomes, autophagosomes, lysosomes and
transport
vesicles. → these communicate with each other
through
vesicles.
- It is extremely important to remember that peroxisomes, mitochondria and chloroplast do NOT belong to the
 endomembrane system, because they don’t receive vesicles from the other organelles.

BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

2. THE ENDOPLASMIC RETICULUM (extension of the nuclear envelope)

It is a continuous membrane system that forms a series of flattened sacs within the cytoplasm of
eukaryotic cells and serves multiple functions, being important particularly in the synthesis, folding,
modification, and transport of proteins and lipids too. It is a complex membrane organelle, and they
have a very variable development in the cell depending on the cell type/activity (especially abundant
in protein and lipid secreting cells). It’s presence is depending on the cell type, especially cells that
have to secrete proteins or lipids will have a big ER.

2.1. RER: ROUGH ENDOPLASMIC
RETICULUM

- It has ribosomes attached to the
membrane.
- Cisterns are aligned in parallel.
- Main function → involved in protein
metabolism:
- Protein synthesis: beginning of
secretory pathway.
- Protein sorting: It sorts the
proteins.
- Protein glycosylation: The amino acids have sugar molecules attached to them.
- Protein folding: There is a high amount of chaperons. Proteins need to be properly folded so they have a
specific fufunction
- Synthesized proteins are stored in the lumen of the ER and will reach the Golgi apparatus and other organelles
through vesicles.

2.2. SER: SMOOTH ENDOPLASMIC RETICULUM

- It does not have ribosomes attached to it
- Cisterns are more twisted, they look more disorganized. It is more irregular (in cross section it looks like there is
an accumulation of vesicles).
- Main function → lipid metabolism
- Membrane lipid synthesis (when the lipids are reduced they are send to other organelles by means of
vesicles or other translocators).
- Interexchange of lipids between organelles ( through vesicles or specific cytosolic transporters) -
Phospholipids, sphingolipids, cholesterol and Steroid hormones (cortisol…) synthesis
- Detoxification of toxic organic compounds through oxidation (enzymes of the cytochrome P450)

!!! RER/SER ratio depends on the cell type and its physiological function. For example, cells synthesizing
large amounts of proteins will have a very developed RER and cells having a very high lipid metabolism
will contain a very developed SER.
There is continuity between the SER and the RER, they are arranged differently but they are
communicated.

3. SECRETORY AND CYTOSOLIC PATHWAYS FOR PROTEIN SYNTHESIS
 Ribosomes initiate translation in the cytosol, after that, there are two routes that proteins use to
reach their destination within the cell::
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

3.1. CYTOSOLIC PATHWAY: Direct translation of the mRNA. The ribosome can continue being a
free ribosome and the synthesis of the protein is going to finish in the cytoplasm. Proteins
following this route are synthesized by free ribosomes in the cytosol. These proteins usually
remain in the cytoplasm or are directed to organelles like mitochondria, nucleus or peroxisomes
(none of them is an organelle of the endomembrane system), were they perform specific
functions. The proteins are released to the cytosol and need to be exported to the organelles by
different mechanisms. This pathway is common for proteins that do not require extensive
post-translational modifications.

3.2. SECRETORY PATHWAY: The translation of mRNA starts on the surface of the ER, followed by
transport through vesicles to the Golgi apparatus. Here, proteins are modified and packaged into
secretory vesicles, which will fuse with the plasma membrane to release the proteins outside the
cell. This pathway is typical for proteins that need to be secreted, sent to specific organelles or
targeted to lysosomes. This proteins have specific signals:

- GLYCOSYLATIONS. All proteins will have sugars residues attached to them (it is their main
characteristic). These glycosylations will start in the ER and they will be finished in the
Golgi apparatus.

4. RER: THE START OF THE SECRETORY
PATHWAY
Ribosomes attached to its surface (electron dense spots) will be translocated to the RER lumen
(cistern inside), which will contain newly synthesized proteins along with chaperons. The RER
consists of highly aligned cisterns charged, visualized in parallel and they have electrodense spots
(ribosomes).
 Synthesis starts in the cytosol, the ribosome and the mRNA bind in the cytosol, (the first amino
acids are translated by cytosolic ribosomes), but the ribosome is immediately translocated to RER
thanks to an HYDROPHOBIC SIGNAL PEPTIDE (8-10 hydrophobic amino acids) → (this will be the
ER import signal) →if anything has this signal, it will be translocated to the ER.
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

5. CYTOSOLIC vs. RER POLYRIBOSOMES

Many ribosomes read one mRNA molecule at a time.

In the secretory pathway, in order for the mRNA-ribosome complex to be translocated to the ER, the
protein needs to have one specific signal (SRP) which bounded to the signal peptide creates the RER
import signal (close to NH2 protein end).

5.1. CHARACTERISTICS

- 8 to 10 hydrophobic amino acids in a row (Leu, Ile, Phe, Trp, Val, Met, Ala): hydrophobic block - It’s
a consensus sequence (not fixed: relative changes are allowed as long as they are hydrophobic
amino acids.)
- If you remove it from a gene → block translocation (it shows that sequences are fundamental to
immediate translocations). Proteins rely on this system to reach the ER.
- A special protein (SRP, signal recognition particles) recognises and binds to these hydrophobic
peptide sequences. So thanks to this movement of the SRP molecule, we are going to have
ribosomes attached to the rough endoplasmic reticulum (RER).

6. TRANSLOCATION OF PROTEINS

Shortly after the initiation of translation the signal peptide, which has to be hydrophobic, will appear.
Typically, this peptide will have a consensus sequence created by 8-10 amino acids (ex:
Leu-Leu-Leu-Val-Gly-Ile-Leu-Phe-Trp-Tyr). This will be recognized by the Signal Recognition Particle (SRP).
This protein, first of all, recognizes the signal sequence of the nascent newborn protein, it gets in touch
with it, and also with the ribosome that is free in the cytosol. Finally, it is going to transport both the
nascent protein with the ribosome and the mRNA molecule towards an SRP receptor, and this receptor is
located in the RER. So, in other words, SRP binds the peptide and brings the mRNA-ribosome complex to
the RER surface.

Thanks to this movement of the SRP molecule, and to the
interaction of the SRP with the protein translocation
machinery in the ER, we are going to have ribosomes attached
to the rough endoplasmic reticulum. Translation will be
transiently stopped until the whole complex gets bound to the
ER membrane. Once the ribosome together with the nascent
protein is attached to the rough ER, there is a cross membrane
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

protein called translocon (which will catalyze translocation of the new protein to the ER lumen) is going
to open. Once this protein opens, the synthesis of the protein is not going to happen anymore in the
cytosol, but inside the lumen of the endoplasmic reticulum. → In the process, there could be different
situations depending on the protein.

6.1. SYNTHESIS OF WATER SOLUBLE PROTEINS

Ribosome is going to be bound to the ER. Then, the signal peptide will interact with the translocon in a
way that the edge of the protein will be sticking facing the cytosolic side. Meanwhile the ribosome will
resume translation so new amino acids will be added to the newborn protein and after a while, signal
peptides will come and cleave the protein by the signal peptide depart. Like this, it will remove the signal
peptide from the new protein (is always removed). In the process, the signal peptide will remain bound
to the translocator, but the protein will be released free in the ER lumen.

6.2. SYNTHESIS OF TRANSMEMBRANE PROTEINS

Transmembrane proteins are those who are permanently attached to the membrane by hydrophobic domains
but cross to the lipid bilayer. Transmembrane proteins are different, because apart from the first hydrophobic
block (there are several), they have other internal signal sequences: the start and stop transfer sequences.

The stop signals bind to the proteins too and the part that has been synthesized stays inside and the part
that is going to be done gets out.
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM
Single Stop sequence: The single-pass transmembrane protein will cross through the membrane only
one time.

The process is the following one:

- SRP (signal recognition particles) recognize the sequence and get in touch with the ribosome. -
Transport the ribosome towards the membrane of the ERER.
- Translation continues and when the protein is burning inside the lumen, the peptidase is gonna cut
the signal sequence.
- When the protein is finished the translocon closes again and we will have the protein. Also, the
hydrophobic peptides will be transferred to the lipid bilayer.

Alternating the hydrophobic sequences (start and stop) there is a possibility to generate multiple
multipass of transmembrane protein. So the internal hydrophobic parts of the protein will constitute the
transmembrane domains of the future protein. Hydrophobic amino acids tend to arrange alpha-helix 3D
(most stable form of arrangement), which interact with the lipid bilayer (the amino acids are not
repealed by the bilayer because they are hydrophobic, so they are able to integrate well in the lipid
bilayer).

*Non-well folded proteins can suppose a danger for the protein itself. If chaperons fail their function,
then the protein won’t complete its function (not functional). (The function of each proteins relays on
the 3D configuration of the protein)

*These signal sequences get their name (start/stop) because the first sequence, which is the signal
peptide, starts the translocation of the protein. But then, when there is another one, it will stop because
the amino acid that is next to it will be sticking out of the membrane.

6.3. GLYCOSYLATION (No ha dicho todo)

This process is specific for proteins taking the secretory synthesis
pathway (RER-Golgi). It starts in the ER and it takes place simultaneously
with the translocation.
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM
During the translation of the protein some specific carbohydrates are added to it, because cytosolic
proteins have no sugar residues attached. Those needed sugars are transferred from the main molecule
used in this process: dolichol (phosphate). It is located in the ER membrane and has two functions:
anchoring molecules and carrying molecules. As the proteins get synthesized, some specific amino acids
of the proteins’ structure bind to the dolichol oligosaccharide, like this, the oligosaccharide is transferred
from dolichol phosphate to asparagine amino acids in the new protein. This process is called
N-glycosylation (carried out on the top in a nitrogen atom).

Alway every oligosaccharides that take part contain the same elements (they are the same
oligosaccharide): 14 sugar residues, 2 NAG (N acetylglucosamine), 9 mannose and 3 galactose. Apart
from that, all the proteins that enter in the ER are glycosylated in the same way, initially. Particularly
important in the golgi apparatus for tagging different proteins, due to the compounds taking different
directions.

7. FOLDING AND QUALITY PROTEINS

7.1.CHAPERONS AND PROTEIN
FOLDING

Chaperons are proteins that help other
proteins fold
correctly, whether the type of the protein they all
have to be
fond correctly. Proteins that aren’t correctly folded
are
useless, and even dangerous for the cell (they
become a
problem for the cell). Due to that, and to help new proteins
get their final 3D conformation, ER is very rich in chaperones.
If chaperones fail, the new synthesized protein will likely be
non-functional.

One example of complex folding processes requiring the aid of
chaperones is heteromeric protein assembly (antibodies), that need BIP chaperone. IgGs (a type of
antibodies) contain two light and two heavy chains, so they are a protein containing four different
protein chains. Here, BiP chaperones help them to stabilize, before they get bound to the rest. So this
process takes place gradually.

Another example is the case of the disulfide bond formation
(covalent bond), in which the protein disulfide isomerase (PDI) has
an important role: it participates in the creation of these specific
unions by oxidizing amino acids with a sulfide group to create a
covalent bond that brings polypeptide chains together. This is very
typical in heteromeric proteins.

*There are four main proteins that control the proper folding of
proteins to manage to get that 3D structure, which are different
types of chaperons:
The following molecular chaperons are very abundant in the RER lumen. Calnexin and Calreticulin bind to
glycosylated protein moieties, binding those oligosaccharides.
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

- BiP; It is hydrosoluble. It is a resident protein and it is found in the lumen in the ER. It stabilizes and
checks the proper folding of the protein.
- Calnexin; It is liposoluble because it is a transmembrane protein but it is facing the lumen so it can
interact with the protein. It controls the proper folding of the protein by adding or removing
sugars.
- Calreticulin: It shares the function with the previous one but in this case it is hydrosoluble.

PDI: It is hydrosoluble. It is found in the lumen of the ER and its main function is to create disulfide
bonds.

If a new proten is not well folded, it gets retained by chaperons inside the ER.

7.2 THE UNFOLDED PROTEIN RESPONSE (UPR) - ER STRESS: Folding and Quality
control in the ER

If chaperones manage to get proteins folded it happens what is called the unfolded protein
response UPR. This is a situation of ER stress.

Proteins need to be properly folded
within the
ER and if many unfolded proteins
accumulate,
that may compromise cell viability.
There are
some stress sensors (PERK, IRE1, ATF6)
that
are present in the ER membrane that
can
detect these situations. If you have a
situation,
for instance, when cells are subjected to high
temperatures, many unfolded proteins are
 obtained so there is a higher demand for
chaperones. Chaperones instead of being free,
they will be all occupied to fold the proteins.

There are some transmembrane proteins
(stress sensors) in the ER membrane which can be either bound to chaperones or unbound to
them. When the chaperone demand is low, these proteins will be bound to chaperones in an
inactive form. However, if there is a higher demand for chaperones, then those sensors will lose
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

the chaperon binding, and chaperones will bond to unfolded proteins. If there are a lot of
unfolded proteins, the ER sensors don't have any chaperons bound to them and they activate the
relay stress signals to the cell nucleus. This is what is called the UPR or the unfolded protein
response.

The important idea is that they all culminate in the activation of specific transcription factors
that may affect gene expression. The gene expression response that is activated is usually to
increase the chaperones synthesis as chaperones are very needed in the case of accumulation of
unfolded proteins. Then, autophagy pathways will be activated as well. If this situation of ER
stress persists, this will lead to the suicide of the cell, what we call as cellular apoptosis. This is
usually created by the accumulation of unfolded proteins.

8. SMOOTH ENDOPLASMIC RETICULUM (SER)

The SER is continuous with the
RER
and they both belong to the
same
organelle but the structure is
completely different. In the SER
there
are not any attached
ribosomes, so
they cannot synthesize proteins.
However, it is very important in lipid
metabolism. Most cellular
membrane lipids are synthesized
here so they can then be transferred
to other cellular compartments by
means of vesicles or specific transporters. The SER also plays an important role in the clearance
of toxic hydrophobic compounds (xenobiotics) by oxidating them. This is catalyzed by the p450
cytochrome system (redox enzyme system). They are very often hydrophobic so they need to be
modified.

Cells containing a very developed SER are usually involved in lipid metabolism and in the
clearance of toxic substances in our organism. For example, liver hepatocytes (which are
involved in the clearance of toxins or hydrophobic toxins from the blood, like in the drug
clearance). Adrenal gland cells also have a very developed SER but in this case they are involved
in steroid hormone synthesis.

8.1. CYTOCHROME P450 SYSTEM
 Carries out the oxidation of the toxic compound

Is a very powerful system to metabolize
non-water
soluble toxic organic compounds.

Cytochrome p450 system retains a lot of
mitochondrial
reticulum transport chains. It is a set of redox
enzymes
present in the ER membrane with the function
of
oxidizing of organic components. There are electron
donors (NADPH will be the primary donor) which
transfer electrons to the chain of proteins to transport
them from one another. This is used to metabolize
organic compounds. These compounds are usually
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

hydrophobic toxins and in order to be eliminated/secreted they have to be oxidized. Those
enzymes manage to combine the ‘R’ (this will refer to the toxin) to make it water soluble (more
“manageable” for secretion/elimination). Similarly to mitochondria, this system consumes O2
that combines with the toxin so it gets oxidized and oxygen gets reduced to water.

8.2. MEMBRANE LIPID BIOSYNTHESIS IN THE SER

The SER is also fundamental for lipid biosynthesis. This takes place in the cytosolic hemilayer of
the SER membrane. New lipids will be added to the cytosolic hemilayer of the SER.

In the image we can see the process of phospholipid synthesis (the most abundant lipid in our
membranes). This is formed by the esterification of fatty acids with glycerol thanks to acid
transferases which are present in the SER membrane. These acid transferases generate
phosphatidic acid at the beginning, then the phosphate group gets removed and the
diacylglycerol, which is the product of the removal, can then be combined with nonpolar groups
in different types of phospholipids. In the case of the choline combination, you get
phosphatidylcholine.

9. INTEREXCHANGE OF LIPIDS BETWEEN THE ER AND OTHER ORGANELLES
 We know that phospholipids can flip to the
opposite hemilayer and then they can
diffuse laterally; they can travel.
Phospholipids in the ER get transported
to
the GA by means of vesicles (this is the
typical way of transport).

The addition of new phospholipids
takes
place only in the cytosolic hemilayer
of
the SER membrane, but some of them
will then move to the luminar part
hemilayer, to equilibrate both sides. Those phospholipids will flip (flip-flop movement) inside.
Once synthesized they can transfer to other organelles by means of vesicles or transporters.

Sphingolipids, however, are a bit different because the basic block of sphingolipids is ceramide
and it doesn’t travel in vesicles. This is transferred through specific translocators which bring
these ceramides directly from the SER membrane to the golgi apparatus. They get sphingolipids
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

such as sphingomyelin and once they have mature sphingomyelin, this goes together with
phospholipids in secretion vesicles to reach the plasma membrane.

ER may transfer lipids directly to other membrane organelles like mitochondria and
peroxisomes, even the plasma membrane. They are lipids of the nuclear envelope, which can
diffuse laterally. Since the nuclear envelope is continuous with the ER, the destination is
reached. As you can see, there are many ways to transfer lipids from the ser to different
membrane compartments: direct, through vesicles, specific translocators…

10. OTHER ER FUNCTIONS: STORAGE OF Ca2+

The endoplasmic reticulum can also store Ca2+ from the cytosol and release it in response to
specific signals. It is able to transport it against gradients (active transport, calcium pump).

When looking at the calcium concentration in the intracellular and extracellular medium, we can
see that the extracellular medium contains high concentration of calcium. The cytosol, in
contrast, contains a very low one. But the lumen of ER is very rich in calcium as well, and this is
so because in the membrane of the ER we have some transmembrane proteins which hydrolyze
ATP to keep calcium released from the ER. This regulates a lot of physiological processes, for
example, muscle contraction.

Many signaling pathways culminate in the release of
calcium from the ER. This is the case of skeleton
muscles.
Most of the calcium that overwhelms the cytosol
upon
muscle fiber contraction comes from the ER, and not
from
 the intracellular space. This is just one example of the many
different processes that can be regulated by calcium
released from this organelle.

KNOWLEDGE TEST:

1. Why is the ER divided into smooth and rough ER (SER, RER)?

Because the rough one has ribosomes attached to it and the smooth has not.

2. Which are the main functions of each two parts?

The RER is involved in protein metabolism: protein synthesis (beginning of secretory pathway), protein
sorting, protein glycosilation and protein folding while SER is involved in lipid metabolism: membrane
lipid synthesis, interexchange of lipids between organelles, cholesterol and steroid hormone synthesis
and detoxification of organic compounds.

3. Proteins synthesized in the ER have a keysignature/specific characteristic that is not found in
proteins synthesized in the cytosol. Which is it?

Glycosylations, which involve adding sugar molecules. This process distinguishes them from cytosolic
proteins, which do not undergo glycosylation.
BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

4. What is it needed for a protein to be translocated to the ER?

A protein needs a signal peptide, which is a sequence of 8-10 hydrophobic amino acids near the start, to
be moved to the ER. This signal starts the process and is recognized and attached by the Signal
Recognition Particle (SRP). SRP is located in the citosol, in the very beggining of the protein.

5. The lumen of the RER is very rich in molecular chaperones. What is the function of those
proteins? Can you name some examples of them?

Chaperons are proteins that assist in the correct folding of other proteins so they get their final 3D
configuration. For example, BIP proteins.

6. What is the ER stress respone?

Is the reaction that the ER transmit to the nucleus if there are too many misfolded proteins accumulated
in the ER. This response can lead to block the expression of more proteins or even be the cause of the
suicide of the cell.

7. How does the SER participate in the clearence of toxic compounds?

By the cytochrome p450 system, who metabolizes non-water soluble toxic organic compounds by
oxidating them so they become non polar.

8. The SER can transfer membrane lipids to other eukaryotic cell compartments. Can you briefly
describe the different mechanism to do that?
They can travel to the membrane through vesicles and by specific trannsolcator (those mainly when the
molecules have to be transported to the GA)

9. How does the ER sequester Ca+2 to attain a higher concentration of this ion inside the ER
lumen?

ER collects Ca2+ from the cytosol, increasing its levels inside. It can release this Ca2+ when signaled to
do so. This is due to the presence of pumps that pump calcium against the gradient concentration. Ca2+
in the cytosol is important for many cell functions, including muscle contraction.

10. What is the main function of signal sequences and SPR in rotein synthesis on the ER?

Facilitate ribosome binding to the ER membrane

11. Membrane-bound proteins are integrated into the ER membrane because they posses:

Transmembrane hydrophobic domains.

12. The Unfolded Protein Response (UPR) aims to restore ER homeostasis by:

Enhancing protein synthesis

BIOCELL BOCK 4: ENDOMEMBRANE SYSTEM

13. In addition to lipid synthesis the smooth endoplasmic erreticullum is also involved in the
metabolism of which type of molecule?

Xenobiotics (foreign organic compounds)