Path Book: Chapter 5 Neoplasia pg. 173-177 Flashcards
What is the genetic hypothesis of cancer?
implies that a tumor mass results from the clonal expansion of a single progenitor cell that has incurred genetic damage (i.e., tumors are monoclonal).
What are the main normal regulatory genes that are targets of DNA damage for cancer formation?
1) growth-promoting proto-oncogenes,
2) growth-inhibiting tumor suppressor genes,
3) genes that regulate programmed cell death (i.e., apoptosis), and
4) genes involved in DNA repair
What are oncogenes?
Genes that induce a transformed phenotype when expressed in cells. A major discovery in cancer was the realization that most oncogenes are mutated or over expressed versions of normal cellular genes, which are called proto-oncogenes. Most known oncogenes encode transcription factors, growth regulating proteins, or proteins involved in cell survival and cell–cell and cell–matrix interactions.
They are considered dominant because mutation of a single allele can lead to cellular transformation.
T or F. Usually both normal alleles of tumor suppressor genes must be damaged for transformation to occur.
T. However, recent work has clearly shown that, in some cases, loss of a single allele of a tumor suppressor gene can promote transformation.
Tumor suppressor genes are usefully placed into two general groups:
“governors” and “guardians.”
What are governors?
“Governors” are classic tumor suppressor genes, such as RB, where mutation of the gene leads to transformation by removing an important brake on cellular proliferation.
What are guardians?
“Guardian” genes are responsible for sensing genomic damage. Some of these genes initiate and choreograph a complex “damage control response.” This response leads to the cessation of proliferation or, if the damage is too great to be repaired, the induction of apoptosis.
What is TP53?
“guardian of the genome,” is a prototypic tumor suppressor gene of this type. Other guard- ian genes are directly involved in recognizing and repairing specific kinds of DNA damage; these are the genes that are mutated in the autosomal recessive syndromes of DNA repair.
What is a mutator phenotype?
Mutation of TP53 or other sensors of genomic damage does not directly transform cells, as loss of guardian function has no direct effect on cellular proliferation or apoptosis. Instead, loss of the guardian genes permits and accelerates the acquisition of mutations in oncogenes and tumor suppressor genes that can lead to the development of cancer. This increase in mutation rate is often referred to as a mutator phenotype.
The genetic changes that characterize cancer-associated mutations may be subtle (e.g., point mutations or inser- tions and deletions) or large enough to produce karyotypic changes.
The genetic changes that characterize cancer-associated mutations may be subtle (e.g., point mutations or inser- tions and deletions) or large enough to produce karyotypic changes.
What do point mutations typically manifest as?
Point mutations can either activate or inactivate the resulting protein products. For example, point mutations in proto-oncogenes, such as RAS or EGFR, frequently result in overactivity of the protein, usually by altering an internal regulatory amino acid and producing a constitu- tively active protein. However, point mutations in tumor suppressors, such as those affecting RB or TP53 genes, reduce or disable the function of the encoded protein.
The common types of nonrandom structural abnormalities in tumor cells are:
(1) balanced translocations,
(2) deletions, and
(3) cytogenetic manifestations of gene amplification.
Balanced translocations are highly associated with certain malignancies, particularly specific kinds of ___ and ___ neoplasms.
hematopoietic and mesenchymal neoplasms.
Translocations can activate proto-oncogenes in two ways:
1) Some translocations result in overexpression of proto- oncogenes by removing them from their normal regulatory elements and placing them under control of an inappropriate, highly active promoter.
2) Other oncogenic translocations create fusion genes encoding novel chimeric proteins.
What are two examples of how translocations result in overexertion of porto-oncogenes by removing them from their normal regulatory elements and placing them under control of an inappropriate promoter?
two kinds of B cell lymphoma
1) In more than 90% of cases of Burkitt lymphoma the cells have a translocation, usually between chromosomes 8 and 14, which leads to overexpression of the MYC gene on chromosome 8 by juxtaposition with immunoglobulin heavy chain gene regulatory elements on chromosome 14.
2) In follicular B cell lymphomas, a reciprocal translocation between chromosomes 14 and 18 leads to overexpression of the antiapoptotic gene, BCL2, on chromosome 18, also driven by immunoglobulin gene elements.
