Lecture 12 - p53 and Apoptosis

Question 1

What is p53 and what can it trigger? What does the loss of apoptosis allow [in relation to cancer]?

Why is it interesting?

Answer 1

p53 is a transcription factor that can trigger cell cycle arrest and apoptosis.

The loss of apoptosis allows cancer cells to survive under normally lethal pathological stresses. Cancer cells have learned how to avoid apoptosis.

p53 is interesting because it is the most common mutated gene found in all forms of cancer. It even has a higher frequency of mutation than Rb. It is almost always lost eventually (at some point) in every form of cancer.

Question 2

Why was p53 originally thought to be an oncogene? Why was this false?

Answer 2

p53 was originally thought to be an oncogene as p53 cDNA transformed rodent cells. However, it was found that the p52 used in that experiment was a mutated form and therefore cause injected rodents to develop cancer. (promotes proliferation).

Regular Wild Type p53 suppresses proliferation and is a tumor suppressor gene.

Question 3

What is the relationship between p53 and many tumor viruses?

Answer 3

p53 is a target for many tumor viruses.

Question 4

How is p53 different from other tumor suppressor genes?

Answer 4

p53’s function is different from other tumor suppressor genes as it specifically prevents the proliferation of abnormal cells.

Question 5

What is the most common form of a p53 mutation? Why is this form the most detrimental form of p53 mutation?

Answer 5

The most common p53 mutation is a “missense mutation” where one Amino Acid has been switched for another.

This is the most detrimental mutation as it is similar enough in shape to allow p53 to stay in the cell and in the game, so to speak, but powerful enough to prevent the protein from performing its proper function.

Question 6

Explain the statement: “p53 is a dominant negative mutant”.

Answer 6

p53 is a protein that functions as a homotetramer. This means it is made up of four smaller subunits that all need to be functional in order for the overall protein to function.

Therefore, only 1 out of every 16 p53 proteins is truly +/+/+/+ or simply +/+ which means that the mutated version are more common, favoured, and will naturally out-compete the small amount of +/+ in the cell.

Question 7

What is so significant about p53 levels? Explain the futile cycle.

Answer 7

p53 shows nuclear localization and levels differ between cells. Furthermore, levels of p53 increase in response to stress and p53 has a ~20 minute half life.

The cycle of p53 production is therefore futile because it will continously degrade/die-off.

Question 8

What are the 6 most common activating signals of p53 release? What are the 4 most common response effects by p53 to these signals?

Answer 8

Activating signals of p53:
1 - lack of nucleotides
2 - UV radiation
3 - Ionizing radiation
4 - Oncogene signalling
5 - Hypoxia
6 - Blockage of transcription

Effects of p53:
1 - Cell cycle arrest
2 - DNA repair
3 - Block of angiogenesis
4 - Apoptosis

Question 9

What are the two subcategories to the cell cycle arrest response of p53? What do they mean?

What role do activating signals play over a prolonged period of time? What is the main role of p53?

Answer 9

1 - Senescence: cell goes into a Go style stage where it cannot proliferate and remains static. It is still functioning, but stagnant. Cell may or may not go back into the cell cycle down the road (pretty doubtful though)

2 - Return to proliferation: basically, instead of going into the Go stage, you just let the cell go to do its thing.

Over an extended period of time, activating signals usually prevent p53 breakdown: the transcription levels will remain relatively constant.

Question 10

What is Mdm2 and what is its relationship to p53?

Answer 10

Mdm2 is an oncoprotein that binds to all four domains of the p53 tetramer (1 Mdm2 per subunit). It then initiates the ubiquitylation (3 Ubi per subunit) of p53 and its degradation bia proteasomes.

Essentially, Mdm2 acts to inhibit p53 and thereby inhibit apoptosis and/or senescence.

Question 11

How is the relationship between p53 and Mdm2 transcription levels a negative feedback loop? Describe this process.

Answer 11

p53 transcribes certain genes to perform its various functions. At increased levels, it will transcribe Mdm2 which then acts to reduce the levels of p53 and subsequently reduce its own levels.

Question 12

Can p53 be protected from Mdm2? How does this occur?

Answer 12

p53 can be phosphorylated in response to DNA damage. This prevents Mdm2 from binding and furhter prevents ubiquitylation and degradation via proteasomes.

Question 13

Aside from phosphorylation, what is the other way p53 can be protected from Mdm2?

Answer 13

Mdm2 can be phosphorylated or broken down/degraded itself by Chk1 and/or Chk2 kinases.

Question 14

What is the relationship between ARF and Mdm2? What does the ARF molecule look like?

Answer 14

ARF bind to Mdm2 NOT for breakdown, but rather for sequesteration. It mobes Mdm2 into the nucleus for storage until it is needed.

It looks like a circle with a rectangular slot for the square end of the Mdm2 rectangle.

Question 15

What can p53 do in emergency situations.

Ex: when there is massive genomic damage

Where is the p53 apoptotic pathway commonly seen in development?

Answer 15

In emergency situations, p53 can trigger apoptosis, but Cell Cycle arrest is still the primary response.

p53 apoptotic activity is commonly observed in the separation of digits, etc…

Question 16

What is one of the major reasons p53 is so interesting for research? [in relation to proteins]

Answer 16

There is much we still don’t know about the function of p53. Proteins transcribed by the p53 pathway undergo a wide range of post translational modifications before reaching their specific targets or performing their specific roles.

Question 17

What does the apoptotic program often depend on? Which gene in particular is of interest here? Why?

Answer 17

The apoptotic program often depends on the mitochondria. Here, the bcl-2 oncogene is of interest since apoptosis requires the proper functioning of this gene, even though it is anti-apoptotic.

Question 18

What is Bcl-2? What role does it play in apoptosis?

Answer 18

Bcl-2 is an anti-apoptotic protein that localizes to the outer membrane of the mitochondria. Here, it controls the flow of cytochrome c, which is extremely important in controlling apoptosis [wheel of death].

During apoptosis, the mitochondrial outer membrane becomes depolarized and cytochrome c spills out into the cytosol. There, it interacts with proteins to trigger cell death.

Question 19

What does cytochrome c like to target [typically].

Answer 19

Cytochrome C typically likes to target organelles such as the nucleus. Incredibly high levels of cytochrome c can be found in the nucleus during apoptosis.

Question 20

What happens if bcl-2 is mutated or lost?

What is the observed balance in the study of the struggle between pro/anti-apoptotic proteins?

Give three examples of pro-apoptotic proteins.

Answer 20

If bcl-2 is mutated or lost, the cell can no longer release cytochrome c meaning that apoptosis has been avoided. This in turn is a proliferative, pro-survival adaptation.

If bcl-2 wild type was present there was no change. If absent, proliferation and apoptosis avoidance ensued. If absent and combined with a pro-apoptotic protein, cells appeared similar to wild type.

Ex: Bax, Bim, Bad

Question 21

What are pro-apoptotic signals?

Give three examples of pro-apoptotic proteins.

Answer 21

Pro-apoptotic signals are bcl-2 related pro-apoptotic proteins that are relased by bcl-2.
Ex: Bax, Bim, Bad

Question 22

Describe the Apoptotic Caspase Cascade. Include and describe caspase 9, cytochrome c, wheel of death, executioner caspases 3,6,7.

Where does this all occur? What is it called?

Answer 22

1 - Pro-apoptotic (death) signals enter mitochondria and cause bcl-2 to release cytochrome c in the cytosol (inner cell environment) as well as Smac/DIABLO

2 - Cytochrome C binds with Apaf-1 and caspase 9 [previously inactivated as procaspase 9] to form the “wheel of death”

3 - The Wheel of Death causes the activation of executioner caspases 3, 6, 7

4 - The executioner caspases 3, 6, 7 cause the cleavage of death substrates –> cell death via DNA destruction

5 - Smac/DIABLO also released from mitochondria activate inhibitors of apoptosis which can block the executioner caspases from cleaving the death substrates.

Fighting cycle.
THIS OCCURS INSIDE THE CELL –> Intrinsic apoptosis

Question 23

How does apoptosis proceed outside the cell? What is this called? How does this occur?

Answer 23

Extrinsic apoptosis (outside the cell) occurs when signals initiated outside the cell (TNF-alpha, TRAIL, Fas L) bind to their specific receptors.

This triggers the DISC apoptotic response through FADD, which leads to the inactivation of caspases from their inactive procaspase form.

Finally, it triggers the executionary caspases and the rest is all the same.

Question 24

How are the extrinsic and intrinsic pathways related?

Answer 24

Extrinsic can initiate the triggering of the intrinsic pathway through executionary caspases that cause Bid to be cleaved and activated –> releasing Smac/DIABLO and starting a strong apoptotic signal in the cell.

Question 25

How is apoptosis activated by p53? Describe the 4 ways this is possible.

Answer 25

1 - p53 can sensitize a cell to pro apoptotic signals by increasing the production of FAS receptors (more likely to trigger)

2 - p53 can inhibit pro-survival pathways such as the IGF1/2 pathways (constant, ubiquitous, normal). Here it produces an IGF binding inhibitor that blocks IGF1/2 from binding properly.

3 - p53 can activate Bax which opens mitochondrial channels for cytochrome c and causes cell death cycle

4 - p53 can activate FOXO3 mitogenic pathway. This is pro-proliferative, pro-division, pro-survival.