Deck 16: The Genetics of Cancer

Define cancer at the anatomical level.

Cancer is the uncontrolled proliferation of cells and the ability of cells to metastasize or migrate to other sites to form secondary growths.

Which three stages or transitions in the cell cycle seem to serve as points of control (checkpoints)?

Why do cancer researchers study molecular events associated with mitosis?

Although mitosis is a basic process related to genetic and general biological studies,it is also a significant event in the cell cycle.The cell cycle is regulated by a variety of gene products,which,when altered by mutation,may lead to cancer.

Describe two classes of proteins known to be involved in the regulation of the cell cycle.

Describe the general relationship that may exist between mutations and cancer.

Name two classes of proteins that combine to directly control progression through the cell cycle.

Chronic myelogenous leukemia appears to be associated with a chromosomal rearrangement.Which chromosome(s)is(are)involved,and what is the name of the rearrangement?

What functional differences exist between various cyclins?

Describe the major cellular and molecular events that mark the entry of mitosis from G2.

What is the significance of CDK?

Chronic myelogenous leukemia appears to be associated with a chromosomal rearrangement.How would a chromosomal rearrangement be responsible for this disease?

Define cancer at the genetic level.

What is the name of a normal gene that serves to promote cellular division?

What two properties do various types of cancer cells share?

Provide a simple definition of a carcinogen.

Describe the cellular and molecular function of the ras gene family and the consequences of mutations in ras.

As more is learned about cancer,it has become clear that cancer,with few exceptions,has no genetic basis.

What is retinoblastoma,and what is its supposed genetic basis?

If someone has a predisposition to cancer,what genetic circumstance likely exists?

The familial form of retinoblastoma is characterized by cancer appearing in both eyes relatively early in life.In contrast,the sporadic form is usually unilateral and appears later.What accounts for the difference?

The genome of humans is remarkably stable,so much so that there are no cancers known to result from genomic instability.

Describe the molecular nature of mutation,as related to cancer,in a ras gene.

Much has been written about p53 in terms of cancer biology.What is p53,and what is its significance?

Describe three genetic mechanisms whereby proto-oncogenes can become overexpressed.

List at least three environmental agents or factors that are known to cause cancer.

In what way might a virus contribute to cancer formation?

List three general categories of genetic changes that lead to the formation of oncogenes.

The genetic difference between familial retinoblastoma and sporadic retinoblastoma appears to be based on those with the familial form starting out being ________,whereas those with the sporadic form start out being ________.

In what way can loss of heterozygosity lead to cancer?

Name three human cancers with a genetic predisposition.What appears to be the genetic cause of each?

(a)What is a tumor-suppressor gene?
(b)What are oncogenes?
(c)What is the normal (nonmutant)cellular version of an oncogene called?

Differentiate among the following types of genes: tumor-suppressor gene,proto-oncogene,and oncogene.

When referring to tumor-suppressor genes and cancer,loss of heterozygosity is likely to suppress cancer formation.

A retrovirus uses reverse transcriptase to make a DNA copy of RNA.

There are two types of retinoblastoma,familial and sporadic.In the familial form,a defective gene is generally inherited from one parent.

The gene p53 is called the "guardian of the genome" because it corrects mutations in the spindle apparatus before nondisjunction can occur.

There are several checkpoints in the mitotic cell cycle.All occur in the S phase.

Any agent that causes damage to DNA is a potential carcinogen.

When the normal retinoblastoma protein is dephosphorylated,it acts to suppress cell division by binding to and inactivating the E2F transcription factor.

A tumor-suppressor gene normally functions to suppress cell division.