12) Cancer Heterogeneity

Question 1

How has next generation sequencing been useful in cancer research?

Answer 1

Provided us with an insight into tumour heterogeneity by multi-regional sequencing

Question 2

What can whole genome sequencing be used to look for?

Answer 2

Structural variants, point mutations and copy number variations

Question 3

What are the benefits of exome sequencing?

Answer 3

Only looks at coding regions

Targeted sequence can be focused in a selected target gene panel associated with malignancy

Question 4

Why is there inter-patient cancer heterogeneity?

Answer 4

Some cancers have more mutations due to increased exposure to mutagens and due to to defects in DNA repair functions

Question 5

What are the consequences of inter-patient heterogeneity for therapy?

Answer 5

Targeted therapies will only work in some individuals with the specific mutations that are being treated against

Question 6

What is intra-patient cancer heterogeneity?

Answer 6

Different regions within the same tumour have different mutations

Question 7

What are trunk mutations?

Answer 7

Are clonal mutations present in the initial tumour (founder clone)

Question 8

What are branch mutations?

Answer 8

Are regional and represent secondary and local mutations

Question 9

Describe the branched evolution of a tumour:

Answer 9

Start with trunk that contains the original initiator clonal events, then get internal branches that are subclones with heterogeneity. Also have terminal branches which are current active subclones

Question 10

What is temporal heterogeneity?

Answer 10

Looking back to how the new mutations have developed from the original mutations

Question 11

What is spatial heterogeneity?

Answer 11

Refers to the uneven distribution of various mutations across the tumour

Question 12

What are actionable mutations?

Answer 12

Refers to a DNA change that, if detected in a patient’s tumour, would be expected to affect a patient’s response to treatment

Question 13

What are driver mutations?

Answer 13

Confer growth advantage on the cancer cell - needed at some point during cancer development

Question 14

How can heterogeneity contribute to therapeutic resistance?

Answer 14

Targeted therapy removes most cells but mutant subclones survive and replicate creating a population with resistant gene

Question 15

What are deleterious mutations?

Answer 15

Mutations that impair cells survival, negatively selected in cancer genome

Question 16

What is the issue with making clinical decisions from biopsy?

Answer 16

Usually based on a single biopsy that doesn’t account for regional mutations (heterogeneity)

Question 17

How can resistance through heterogeneity be prevented?

Answer 17

Combinational therapy targeting more than one mutation