Genetics 4 - Cancer

Question 1

What are the hallmarks of cancer?

Answer 1

• Disregulated growth
• Evasion of apoptosis
• Limitless replication
• Metastisis
• IMPORTANT: genome instability and mutation

Question 2

Why is cancer a polyclonal disease?

Answer 2

Cumulative changes result in cancer, meaning that there are many different cells with different mutations in one tumour.

Question 3

What are driver mutations in cancer?

Answer 3

An initial mutation that occurs in either oncogenes or tumour supressor genes. This first hit is usually a point mutation which cant produce a phenotypic effect.

Question 4

Summarise the two hit hypothesis.

Answer 4

Hit 1 is a point mutation, which reduces protein level but doesnt cause phenotypic effect. Therefore, inactivation of a second allele is required - this is hit 2, causes total loss of transcription.
This is required in tumour suppressor genes.

Question 5

What is the function of proto-oncogenes? Give some examples.

Answer 5

They promote growth and proliferation, overriding apoptosis:

• Growth factors
• Transcription factors
• Tyrosine kinases

Question 6

What is the function of tumour suppressors?

Answer 6

These regulate cell division at the DNA damage checkpoints. They can cause apoptosis and DNA repair.

Question 7

How can cancers be identified in the genetics?

Answer 7

They can be identified by a loss of heterogenity due to mutations.

Question 8

What is the difference between familial retinoblastoma and a sporadic retinoblastoma?

Answer 8

Familial - first hit is inherited, second hit is a somatic mutation
Sporadic - two somatic mutations occur in the same cell (hit 1 & hit 2)

Question 9

What inherited mutation is linked to breast and ovarian cancer?

Answer 9

Germline mutations in BRCA1 and BRCA2, DNA repair genes. They give rise to a 60% risk of cancer by age 90. BRCA2 mutations also predispose risk of breast cancer in men.

Question 10

What two diseases result in an inherited predisposition to colorectal cancer?

Answer 10

• Familial adenomatous polyposis (FAP)

- Lynch syndrome (HNPCC)

Question 11

What are the colorectal cancer risks in patients with familial adenomatous polyposis?

Answer 11

Almost a 100% lifetime risk of cancer.

Responsible for >1% of colorectal cancers.

Question 12

What is the risk of colorectal cancer in patients with lynch syndrome?

Answer 12

Responsible for 3% of cancer cases, and 90% of familial cases.
The lifetime risk for cancer is around 80%.

Question 13

How are patients treated if a inherited cancer syndrome is detected?

Answer 13

• If a patient has positive family history then they will recieve genetic screening/counseling.
• If they are mutation positive then they recieve surveillance, chemoprevention and family work-up

Question 14

How may the causes of polygenic cancer be studied?

Answer 14

• Using genome wide association studies to look for SNPs.
• Using transcriptome chips/mRNA arrays to identify differently expressed transcripts (compares expression between malignant and normal tissue)

Question 15

What are cytogenetic changes in cancer?

Answer 15

These are visible changes in chromosome structure or number, which accumulate during disease progression. (Eg. Fusion genes, macroduplications or macrodeletions, aneuploidy)

Question 16

What is the cause of chronic myeloid leukaemias?

Answer 16

It is a clonal myeloproliferative disorder, where there is an overproduction of mature granulocytes.

Question 17

What are the three phases of chronic myeloid leukaemia?

Answer 17

Chronic (beningn), accelerated (ominous) and then blast crisis (acute leukaemic, fatal)

Question 18

What is the philadelphia chromosome?

Answer 18

A fusion protein which acts as the marker for CML. This allows CML to be treated by blocking the ATP binding site of the protein (BCR-ABL1)

Question 19

What are the two lines of treatment of CML and why are they needed?

Answer 19

First line is imantib, and eventually patients lose their response and require second line tyrosine kinase inhibitors.

Question 20

How is acute myeloid leukaemia divided?

Answer 20

Into FAB M0 to FAB M7.

• FAB M3 is a medical emergency
• FAB M5 is not

Question 21

What is pharmacogenetics?

Answer 21

A branch of pharmacology which deals with the influence of genetic variation in drug response.

Question 22

How can pharmacogenetics be used in cancer?

Answer 22

• To plan chemotherapy
• To identify which patients are likely to respond to certain cancer drugs
• To assay particular somatic mutations

Question 23

How many mutations are required in oncogenes to cause cancer?

Answer 23

Only one gain of function mutation.

Question 24

How many mutatiosn are required in tumour suppressor genes to cause cancer?

Answer 24

Two mutations causing loss of function.

Question 25

How are chromosome translocations used to quantify residual disease in leukaemia?

Answer 25

• The response to treatment over the first 3-12 months defines long term response to tyrosine kinase inibitors, which guides clonical management.
• Absense of a cytogenetic response by 12 months results in change of therapy
• Loss of RT-qPCR negativity is a indicator is relapse results in change of therapy.