Mismatch repair gene defects in sporadic colorectal cancers with microsatellite instability

B. Liu; N. C. Nicolaides; S. Markowitz; J. K V Willson; R. E. Parsons; J. Jen; N. Papadopolous; P. Peltomaki; A. De la Chapelle; S. R. Hamilton; K. W. Kinzler; B. Vogelstein

doi:10.1038/ng0195-48

Mismatch repair gene defects in sporadic colorectal cancers with microsatellite instability

B. Liu, N. C. Nicolaides, S. Markowitz, J. K V Willson, R. E. Parsons, J. Jen, N. Papadopolous, P. Peltomaki, A. De la Chapelle, S. R. Hamilton, K. W. Kinzler, B. Vogelstein

Simmons Comprehensive Cancer Center

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

759 Scopus citations

Abstract

Microsatellite instability has been observed in both sporadic and hereditary forms of colorectal cancer. In the hereditary form, this instability is generally due to germline mutations in mismatch repair (MMR) genes. However, only one in ten patients with sporadic tumours exhibiting microsatellite instability had a detectable germline mutation. Moreover, only three of seven sporadic tumour cell lines with microsatellite instability had mutations in a MMR gene, and these mutations could occur somatically. These results demonstrate that tumours can acquire somatic mutations that presumably do not directly affect cell growth but result only in genetic instability. They also suggest that many sporadic tumours with microsatellite instability have alterations in genes other than the four now known to participate in MMR.

Original language	English (US)
Pages (from-to)	48-55
Number of pages	8
Journal	Nature genetics
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/ng0195-48
State	Published - Jan 1995

ASJC Scopus subject areas

Genetics

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abstract = "Microsatellite instability has been observed in both sporadic and hereditary forms of colorectal cancer. In the hereditary form, this instability is generally due to germline mutations in mismatch repair (MMR) genes. However, only one in ten patients with sporadic tumours exhibiting microsatellite instability had a detectable germline mutation. Moreover, only three of seven sporadic tumour cell lines with microsatellite instability had mutations in a MMR gene, and these mutations could occur somatically. These results demonstrate that tumours can acquire somatic mutations that presumably do not directly affect cell growth but result only in genetic instability. They also suggest that many sporadic tumours with microsatellite instability have alterations in genes other than the four now known to participate in MMR.",

author = "B. Liu and Nicolaides, {N. C.} and S. Markowitz and Willson, {J. K V} and Parsons, {R. E.} and J. Jen and N. Papadopolous and P. Peltomaki and {De la Chapelle}, A. and Hamilton, {S. R.} and Kinzler, {K. W.} and B. Vogelstein",

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AU - Liu, B.

AU - Nicolaides, N. C.

AU - Markowitz, S.

AU - Willson, J. K V

AU - Parsons, R. E.

AU - Jen, J.

AU - Papadopolous, N.

AU - Peltomaki, P.

AU - De la Chapelle, A.

AU - Hamilton, S. R.

AU - Kinzler, K. W.

AU - Vogelstein, B.

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N2 - Microsatellite instability has been observed in both sporadic and hereditary forms of colorectal cancer. In the hereditary form, this instability is generally due to germline mutations in mismatch repair (MMR) genes. However, only one in ten patients with sporadic tumours exhibiting microsatellite instability had a detectable germline mutation. Moreover, only three of seven sporadic tumour cell lines with microsatellite instability had mutations in a MMR gene, and these mutations could occur somatically. These results demonstrate that tumours can acquire somatic mutations that presumably do not directly affect cell growth but result only in genetic instability. They also suggest that many sporadic tumours with microsatellite instability have alterations in genes other than the four now known to participate in MMR.

AB - Microsatellite instability has been observed in both sporadic and hereditary forms of colorectal cancer. In the hereditary form, this instability is generally due to germline mutations in mismatch repair (MMR) genes. However, only one in ten patients with sporadic tumours exhibiting microsatellite instability had a detectable germline mutation. Moreover, only three of seven sporadic tumour cell lines with microsatellite instability had mutations in a MMR gene, and these mutations could occur somatically. These results demonstrate that tumours can acquire somatic mutations that presumably do not directly affect cell growth but result only in genetic instability. They also suggest that many sporadic tumours with microsatellite instability have alterations in genes other than the four now known to participate in MMR.

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Mismatch repair gene defects in sporadic colorectal cancers with microsatellite instability

Abstract

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