Eukaryotic cell

Question 1

What occurs in the nucleolus?

Answer 1

partial ribosome synthesis in which RNA pol 1 synthesizes rRNA. Note, the nucleolus is not separated from the nucleus, it is just in a polarized region of it.

Question 2

what is a nuclear localization sequence?

Answer 2

proteins destined to be used in the nucleus will contain an AA sequence that signals for them to be transported back to the nucleus after cytoplasmic translation

Question 3

What are the functions of the RER and SER?

Answer 3

RER –> it is studded with ribosomes. It is mainly responsible for synthesizing and processing proteins which are apart of the secretory pathway.

SER –> steroid synthesis and detoxification in the liver and calcium storage in muscle.

Question 4

proteins that are translated in the cytoplasmic ribosomes are likely to appear where?

Answer 4

they may appear in the

• nucleus
• cytoplasm
• mitochondria
• peroxisome

Question 5

Proteins synthesized by the RER are likely to end up where?

Answer 5

in any part of the secretory pathway. 
Therefore they can end up in 
1. the RER
2. the Golgi apparatus 
3. the plasma membrane
4. ECF
5. inside of lysosome which have degrading functions

Question 6

how do secretory proteins go from the RER to the Golgi to etc.

Answer 6

They travel through vesicles (never touching the cytoplasm). This vesicle transport makes the secretory pathway “contiguous” (means to share a common border)

Question 7

Explain what an N-terminal signal sequence is and a signal recognition particle (SRP) is.

Answer 7

An N-terminal signal sequence is the sequence of amino acids on the mRNA. This signal sequence is recognized by the SRP. The SRP binds the RER ribosome Orients the translating peptide so that as its being made it enters the RER lumen.

Question 8

What is a signal peptide?

Answer 8

the signal peptide is the amino acid sequence that came from the signal sequence translation. The peptide sequence enters the RER lumen first and is cleaved by a signal peptidase inside the lumen. (its only job was to get the protein into the secretory pathway)

Question 9

true or false, the signal sequence / SRP / signal peptide mechanism is only used for proteins destined for the ECF or a lysosome.

Answer 9

true, proteins destined for the plasma membrane and such have another mechanism

however, all secretory pathway proteins contain a signal sequence + some other signal

PM - transmembrane domain
Golgi - targeting sequence

Question 10

integral membrane proteins contain regions called transmembrane domains. Explain these and the secretory pathway involved for them

Answer 10

The transmembrane domains are series of hydrophobic amino acids which end up within the membrane. they are derived from interior signal sequences of the mRNA. During translation, these domains are threaded through the ER membrane which then buds off to the Golgi inside a vesicle.

Question 11

what is the difference between a targeting sequence and a localization signal?

Answer 11

A targeting sequence is a sequence on a peptide that is in the secretory pathway but not destined to be secreted or in the plasma membrane.

A localization signal is sequence on a peptide that is made in the cytoplasm and is destined to go to an organelle that is not apart of the secretory pathway.

Question 12

for the following peptides, state the signal sequence, if any, that they have for transport.

1. secreted peptide
2. PM peptide
3. lysosome
4. RER
5. SER
6. Golgi
7. Cytoplasm
8. Nucleus
9. mitochondria

Answer 12

1. secreted = signal sequence with SRP
2. PM = signal sequence + transmembrane domains
3. lysosome = signal peptide + targeting signal
4. RER = signal P + targeting sequence
5. SER = signal P + targeting sequence
6. Golgi = signal + targeting sequence
7. Cytoplasm = nothing
8. nucleus = localization
9. mito = localization

Question 13

true or false, the Golgi is very uni-directional

Answer 13

true, proteins enter the cis side and leave the trans side

Question 14

Autophagy, phagocytosis, and crinophagy are all done by this organelle… Explain each process.

Answer 14

Autophagy = self eating (eating damaged organelle) 
Phagocytosis = cell eating ECF content 
Crinophagy = the digestion of excess material 

this is performed by lysosomes which contain acid hydrolase’s

Question 15

what do peroxisomes do?

Answer 15

a variety of metabolic tasks. They have bi-product that is peroxy acid but this is degraded by catalase (an enzyme)

Question 16

true or false, weaker intermolecular forces means higher vapour pressure of the substance.

Answer 16

true, vapour pressure is the measured pressure of a gas phase substance back down on a liquid. The easier it evaporates, the more gas form there is, the more vapour pressure.

easier evaporation = weak IMF’s

Question 17

how does dissolving a solute in a solvent effect the solvents vapour pressure?

Answer 17

the solute dissociates and forms ionic interactions with the solvent making it more difficult for the solvent to enter the gas phase. Therefore adding a solute will decrease vapour pressure.

Question 18

what is the Van Hoft factor (i)

Answer 18

i represents the amount of particles in solution when something dissolves.

glucose (C6H12O6), i = 1
NaCl, i = 2

Question 19

what is a colligative process?

Answer 19

a process that depends on the number of solute particles more than the kind of particle. Vapour pressure decrease due to solute addition is a colligative process (the amt of solute added)

Question 20

t or f, the addition of any solute to a solvent will result in the colligative processes vapour pressure depression, boiling point elevation, and freezing-point depression.

Answer 20

true

Question 21

what is osmosis and osmotic pressure? What is hydrostatic pressure?

Answer 21

osmosis is the diffusion of water. Osmotic pressure is the pressure required to stop osmosis from occurring.

hydrostatic pressure is the pressure exerted by a fluid at equilibrium

Question 22

why is simple diffusions curve (force of diffusion vs. flux) linear and facilitated curved and levels off?

note: flux = rate of diffusion

Answer 22

facilitated diffusion is subject to saturation kinetics (all carrier / channels are taken up)

Question 23

microtubules, intermediate filaments, and microfilaments. Explain each.

Answer 23

microtubules are made of tubulin and are used in mitosis to move chromosomes. They are hollow and the largest filament in the cytoskeleton. Microtubules also act as railroad for transport such as nerve axon transport.

intermediate filaments - middle size

microfilaments - smallest, made of actin, involved with amoeboid movement

Question 24

t or f, both eukaryotic and prokaryotic flagella have a basal structure, hook, and filament organization.

Answer 24

false, only prokaryotes have this set up. Eukaryotes have an microtubule arrangement that differs.

Question 25

dynein is a motor protein found where?

Answer 25

in the microtubule tracks which facilitate transport of intracellular material

Question 26

Mitosis: What is the difference between sister chromatids and homologous chromosomes?

Answer 26

sister chromatids –> are identical copies of a chromosome that result after DNA replication

Homologous chromosomes –> are non-identical copies of the same chromosome

e.g. You have two copies of chromosome 1 (one from mom, one from dad). These are homologous chromosomes. Then after DNA replication you have two copies of paternal chromosome 1 and 2 copies of maternal chromosome 1.

each pair are sister chromatids to each other

Question 27

Explain the cell cycle.

Answer 27

The Cycle begins with mitosis (prophase, metaphase, anaphase, telophase) and cytokinesis. This is the actual division of one cell into two

then G1 phase occurs: growth and development

then S phase occurs: DNA replication

then G2 occurs: more growth

then mitosis again

Question 28

what occurs during Prophase of mitosis? (3)

Answer 28

1. chromosomes condense tightly and sister chromatids are joined by centromeres.
2. nucleolus disappears
3. Centrioles move to opposite sides of the cell
4. nuclear envelope begins to degrade

Question 29

what are centrioles and the microtubule organization centre (MCOT)

Answer 29

MCOT is in every cell and it coordinates microtubule cytoskeleton development. Centrioles are apart of it and they form the spindle fibres in mitosis.

Question 30

what is the difference between the kintechore and the centromere?

Answer 30

The centromere links sister chromatids together

The Kinetochore links each sister chromatid to a spindle fibre

Question 31

What occurs during metaphase of mitosis?

Answer 31

The chromosomes line up along the metaphase plate. This is achieved because the kinetochores of each chromosome is connected to the centriole spindle fibres.

Note: polar centrioles / MCOTs are also referred to as asters since they look like (a) stars

Question 32

what occurs during anaphase of mitosis?

Answer 32

the spindle fibres shorten towards the centrioles which separates the sister chromatids. The cell begins to elongate and develop the cleavage furrow.

Question 33

What occurs during telophase?

Answer 33

essentially the opposite of prophase.

1. nuclear envelope forms around polarized chromosomes (ex-sister chromatids)
2. nucleolus appears in each
3. chromosomes re-condense

cytokinesis occurs in which the cells actually separate.

Question 34

what are capsase enzymes

Answer 34

Capsase enzymes are the main enzyme involved in apoptosis

Question 35

what are initiation capsase’s and effector capsase’s?

Answer 35

upon an external (cytokine / toxin / etc.) signal or internal signal (accumulation of a tumour suppressor protein) initiation capsase’s clump together which activates effector capsase’s which cleave many proteins for apoptosis.

Question 36

what is an alpha-beta tubulin dimer?

Answer 36

this is the monomer unit for the microtubule cytoskeleton of the cell (which is a hollow rod)

Question 37

t or f, the MTOC is a pair of centrioles which duplicate and then move to each end of the cell upon mitosis.

Answer 37

true

Question 38

t or f, the kinetochore is a part of the chromosome centromere and is the location where the spindle fibres attach which extend from polarized centrioles.

Answer 38

true

Question 39

what is a microfilament and what are they made from?

Answer 39

the smallest filament in the cell. they are made from actin and are used in small gross movements.

Question 40

what are microtubules made out of?

Answer 40

alpha tubulin and beta tubulin dimers. many dimers non-covalently form a hollow tube

Question 41

t or f, all cytoskeleton structures are made from non-covalent interactions of many proteins

Answer 41

true, cytoskeleton is a great example of quaternary structure.

Question 42

microtubules elongate from one end, what is the other end?

Answer 42

microtubule organization centre MTOC located near the nucleus.

Question 43

what is within the MTOC?

Answer 43

a pair of centrioles which control cell division via splitting chromosomes

therefore microtubules are responsible for mitosis / meiosis

Question 44

what is the miotic spindle

Answer 44

the centrioles + their expanding microtubules

Question 45

t or f, the centromere of each Xm has a kinetchore which the mitoic spindle attaches too

Answer 45

true

Question 46

what else do microtubules do other than mitosis?

Answer 46

they mediate transport of substances within the cell (e.g. in axons)

cilia and flagella are also made from microtubules

Question 47

what do microfilaments do? what are they made from?

Answer 47

they are made out of actin (thin filament)

actin / microfilaments are responsible for gross movement of the cell and contractile processes in muscle cells

they perform cytokinesis too

Question 48

what are intermediate filaments made from and what do they do?

Answer 48

these are heterogenous being composed of many proteins.

these simply create cell structure and are less dynamic than microfilaments and microtubules (they don’t grow and shrink repeatedly)

Question 49

what is a desmosome?

Answer 49

do not form seals but merely hold cells together (tight junctions hold cells in a seal)