Modeling chromosomal instability and epithelial carcinogenesis in the telomerase-deficient mouse

Sandy Chang; Christine Khoo; Ronald A. DePinho

doi:10.1006/scbi.2000.0374

Modeling chromosomal instability and epithelial carcinogenesis in the telomerase-deficient mouse

Sandy Chang, Christine Khoo, Ronald A. DePinho

Research output: Contribution to journal › Article › peer-review

51 Scopus citations

Abstract

Human carcinomas are intimately linked to advancing age. These cancers have complex cytogenetic profiles, including aneuploidy and chromosomal structural aberrations. While aged humans sustain a high rate of carcinomas, mice bearing common tumor suppressor gene mutations typically develop soft tissue sarcomas and lymphomas. One marked species distinction between human and mouse that bears on the predisposition to carcinogenesis lies in the radical differences in length and regulation of the telomere, nucleoprotein complexes that cap the ends of eukaryotic chromosomes. Recent cancer modeling studies in the telomerase knockout p53 mutant mice revealed that telomere dynamics might be relevant to carcinogenesis. In these mice, there is a shift in the tumor spectrum towards epithelial carcinomas, and these cancers emerge with complex cytogenetic profiles classical for human carcinomas. In this review, we suggest that the mechanism of fusion-bridge-breakage-translocation, triggered by critically short telomeres, may be one of the generators of genomic instability commonly seen in human carcinomas.

Original language	English (US)
Pages (from-to)	227-238
Number of pages	12
Journal	Seminars in cancer biology
Volume	11
Issue number	3
DOIs	https://doi.org/10.1006/scbi.2000.0374
State	Published - 2001
Externally published	Yes

Keywords

Cancer
Carcinoma
Fusion-bridge-breakage translocation
Genomic instability
Mouse models
Non-reciprocal translocations
Telomerase
Telomere
p53

ASJC Scopus subject areas

Cancer Research

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10.1006/scbi.2000.0374

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title = "Modeling chromosomal instability and epithelial carcinogenesis in the telomerase-deficient mouse",

abstract = "Human carcinomas are intimately linked to advancing age. These cancers have complex cytogenetic profiles, including aneuploidy and chromosomal structural aberrations. While aged humans sustain a high rate of carcinomas, mice bearing common tumor suppressor gene mutations typically develop soft tissue sarcomas and lymphomas. One marked species distinction between human and mouse that bears on the predisposition to carcinogenesis lies in the radical differences in length and regulation of the telomere, nucleoprotein complexes that cap the ends of eukaryotic chromosomes. Recent cancer modeling studies in the telomerase knockout p53 mutant mice revealed that telomere dynamics might be relevant to carcinogenesis. In these mice, there is a shift in the tumor spectrum towards epithelial carcinomas, and these cancers emerge with complex cytogenetic profiles classical for human carcinomas. In this review, we suggest that the mechanism of fusion-bridge-breakage-translocation, triggered by critically short telomeres, may be one of the generators of genomic instability commonly seen in human carcinomas.",

keywords = "Cancer, Carcinoma, Fusion-bridge-breakage translocation, Genomic instability, Mouse models, Non-reciprocal translocations, Telomerase, Telomere, p53",

author = "Sandy Chang and Christine Khoo and DePinho, {Ronald A.}",

note = "Funding Information: The authors would like to thank S. Alson, M. Bosen-berg, L. Chin, K. Senechal, N. Sharpless, and K. Wong for a critical review of the manuscript. S. C. is a Howard Hughes Medical Institute Physician Postdoctoral Fellow. R. A. D. is supported by the National Institutes of Health and is an American Cancer Society Research Professor and a Steven and Michele Kirsch Foundation Investigator.",

year = "2001",

doi = "10.1006/scbi.2000.0374",

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AU - Khoo, Christine

AU - DePinho, Ronald A.

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PY - 2001

Y1 - 2001

N2 - Human carcinomas are intimately linked to advancing age. These cancers have complex cytogenetic profiles, including aneuploidy and chromosomal structural aberrations. While aged humans sustain a high rate of carcinomas, mice bearing common tumor suppressor gene mutations typically develop soft tissue sarcomas and lymphomas. One marked species distinction between human and mouse that bears on the predisposition to carcinogenesis lies in the radical differences in length and regulation of the telomere, nucleoprotein complexes that cap the ends of eukaryotic chromosomes. Recent cancer modeling studies in the telomerase knockout p53 mutant mice revealed that telomere dynamics might be relevant to carcinogenesis. In these mice, there is a shift in the tumor spectrum towards epithelial carcinomas, and these cancers emerge with complex cytogenetic profiles classical for human carcinomas. In this review, we suggest that the mechanism of fusion-bridge-breakage-translocation, triggered by critically short telomeres, may be one of the generators of genomic instability commonly seen in human carcinomas.

AB - Human carcinomas are intimately linked to advancing age. These cancers have complex cytogenetic profiles, including aneuploidy and chromosomal structural aberrations. While aged humans sustain a high rate of carcinomas, mice bearing common tumor suppressor gene mutations typically develop soft tissue sarcomas and lymphomas. One marked species distinction between human and mouse that bears on the predisposition to carcinogenesis lies in the radical differences in length and regulation of the telomere, nucleoprotein complexes that cap the ends of eukaryotic chromosomes. Recent cancer modeling studies in the telomerase knockout p53 mutant mice revealed that telomere dynamics might be relevant to carcinogenesis. In these mice, there is a shift in the tumor spectrum towards epithelial carcinomas, and these cancers emerge with complex cytogenetic profiles classical for human carcinomas. In this review, we suggest that the mechanism of fusion-bridge-breakage-translocation, triggered by critically short telomeres, may be one of the generators of genomic instability commonly seen in human carcinomas.

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KW - Fusion-bridge-breakage translocation

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KW - Mouse models

KW - Non-reciprocal translocations

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KW - Telomere

KW - p53

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Modeling chromosomal instability and epithelial carcinogenesis in the telomerase-deficient mouse

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