DNMT1 and DNMT3b cooperate to silence genes in human cancer cells

Ina Rhee; Kurtis E. Bachman; Ben Ho Park; Kam Wing Jair; Ray Whay Chiu Yen; Kornel E. Schuebel; Hengmi Cui; Andrew P. Feinberg; Christoph Lengauer; Kenneth W. Kinzler; Stephen B. Baylin; Bert Vogelstein

doi:10.1038/416552a

DNMT1 and DNMT3b cooperate to silence genes in human cancer cells

Ina Rhee, Kurtis E. Bachman, Ben Ho Park, Kam Wing Jair, Ray Whay Chiu Yen, Kornel E. Schuebel, Hengmi Cui, Andrew P. Feinberg, Christoph Lengauer, Kenneth W. Kinzler, Stephen B. Baylin, Bert Vogelstein

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Abstract

Inactivation of tumour suppressor genes is central to the development of all common forms of human cancer. This inactivation often results from epigenetic silencing associated with hypermethylation rather than intragenic mutations. In human cells, the mechanisms underlying locus-specific or global methylation patterns remain unclear. The prototypic DNA methyltransferase, Dnmt1, accounts for most methylation in mouse cells, but human cancer cells lacking DNMT1 retain significant genomic methylation and associated gene silencing. We disrupted the human DNMT3b gene in a colorectal cancer cell line. This deletion reduced global DNA methylation by less than 3%. Surprisingly, however, genetic disruption of both DNMT1 and DNMT3b nearly eliminated methyltransferase activity, and reduced genomic DNA methylation by greater than 95%. These marked changes resulted in demethylation of repeated sequences, loss of insulin-like growth factor II (IGF2) imprinting, abrogation of silencing of the tumour suppressor gene p16^INK4a, and growth suppression. Here we demonstrate that two enzymes cooperatively maintain DNA methylation and gene silencing in human cancer cells, and provide compelling evidence that such methylation is essential for optimal neoplastic proliferation.

Original language	English (US)
Pages (from-to)	552-556
Number of pages	5
Journal	Nature
Volume	416
Issue number	6880
DOIs	https://doi.org/10.1038/416552a
State	Published - Apr 8 2002

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@article{60bf9db184c84f9b9f6e74a5b997bd4d,

title = "DNMT1 and DNMT3b cooperate to silence genes in human cancer cells",

abstract = "Inactivation of tumour suppressor genes is central to the development of all common forms of human cancer. This inactivation often results from epigenetic silencing associated with hypermethylation rather than intragenic mutations. In human cells, the mechanisms underlying locus-specific or global methylation patterns remain unclear. The prototypic DNA methyltransferase, Dnmt1, accounts for most methylation in mouse cells, but human cancer cells lacking DNMT1 retain significant genomic methylation and associated gene silencing. We disrupted the human DNMT3b gene in a colorectal cancer cell line. This deletion reduced global DNA methylation by less than 3%. Surprisingly, however, genetic disruption of both DNMT1 and DNMT3b nearly eliminated methyltransferase activity, and reduced genomic DNA methylation by greater than 95%. These marked changes resulted in demethylation of repeated sequences, loss of insulin-like growth factor II (IGF2) imprinting, abrogation of silencing of the tumour suppressor gene p16INK4a, and growth suppression. Here we demonstrate that two enzymes cooperatively maintain DNA methylation and gene silencing in human cancer cells, and provide compelling evidence that such methylation is essential for optimal neoplastic proliferation.",

author = "Ina Rhee and Bachman, {Kurtis E.} and Park, {Ben Ho} and Jair, {Kam Wing} and Yen, {Ray Whay Chiu} and Schuebel, {Kornel E.} and Hengmi Cui and Feinberg, {Andrew P.} and Christoph Lengauer and Kinzler, {Kenneth W.} and Baylin, {Stephen B.} and Bert Vogelstein",

note = "Funding Information: We thank G. Struhl, D. Kalderon, R. Holmgren, S. Cohen, T. Kornberg and M. Peifer for reagents; and G. Struhl, K. Wharton and L. Parada for comments. This work was supported by the National Institutes of Health. J.J. is a Searle Scholar supported by the Chicago Community Trust, a Eugene McDermott Endowed Scholar in Biomedical Research, and a Leukemia and Lymphoma Society Special Fellow. Funding Information: We thank S. R. Lee and S. G. Rhee for assistance with the HPLC analysis. This work was supported by the Clayton Fund, the V Foundation, and by grants from the National Institutes of Health.",

year = "2002",

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day = "8",

doi = "10.1038/416552a",

language = "English (US)",

volume = "416",

pages = "552--556",

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T1 - DNMT1 and DNMT3b cooperate to silence genes in human cancer cells

AU - Rhee, Ina

AU - Bachman, Kurtis E.

AU - Park, Ben Ho

AU - Jair, Kam Wing

AU - Yen, Ray Whay Chiu

AU - Schuebel, Kornel E.

AU - Cui, Hengmi

AU - Feinberg, Andrew P.

AU - Lengauer, Christoph

AU - Kinzler, Kenneth W.

AU - Baylin, Stephen B.

AU - Vogelstein, Bert

N1 - Funding Information: We thank G. Struhl, D. Kalderon, R. Holmgren, S. Cohen, T. Kornberg and M. Peifer for reagents; and G. Struhl, K. Wharton and L. Parada for comments. This work was supported by the National Institutes of Health. J.J. is a Searle Scholar supported by the Chicago Community Trust, a Eugene McDermott Endowed Scholar in Biomedical Research, and a Leukemia and Lymphoma Society Special Fellow. Funding Information: We thank S. R. Lee and S. G. Rhee for assistance with the HPLC analysis. This work was supported by the Clayton Fund, the V Foundation, and by grants from the National Institutes of Health.

PY - 2002/4/8

Y1 - 2002/4/8

N2 - Inactivation of tumour suppressor genes is central to the development of all common forms of human cancer. This inactivation often results from epigenetic silencing associated with hypermethylation rather than intragenic mutations. In human cells, the mechanisms underlying locus-specific or global methylation patterns remain unclear. The prototypic DNA methyltransferase, Dnmt1, accounts for most methylation in mouse cells, but human cancer cells lacking DNMT1 retain significant genomic methylation and associated gene silencing. We disrupted the human DNMT3b gene in a colorectal cancer cell line. This deletion reduced global DNA methylation by less than 3%. Surprisingly, however, genetic disruption of both DNMT1 and DNMT3b nearly eliminated methyltransferase activity, and reduced genomic DNA methylation by greater than 95%. These marked changes resulted in demethylation of repeated sequences, loss of insulin-like growth factor II (IGF2) imprinting, abrogation of silencing of the tumour suppressor gene p16INK4a, and growth suppression. Here we demonstrate that two enzymes cooperatively maintain DNA methylation and gene silencing in human cancer cells, and provide compelling evidence that such methylation is essential for optimal neoplastic proliferation.

AB - Inactivation of tumour suppressor genes is central to the development of all common forms of human cancer. This inactivation often results from epigenetic silencing associated with hypermethylation rather than intragenic mutations. In human cells, the mechanisms underlying locus-specific or global methylation patterns remain unclear. The prototypic DNA methyltransferase, Dnmt1, accounts for most methylation in mouse cells, but human cancer cells lacking DNMT1 retain significant genomic methylation and associated gene silencing. We disrupted the human DNMT3b gene in a colorectal cancer cell line. This deletion reduced global DNA methylation by less than 3%. Surprisingly, however, genetic disruption of both DNMT1 and DNMT3b nearly eliminated methyltransferase activity, and reduced genomic DNA methylation by greater than 95%. These marked changes resulted in demethylation of repeated sequences, loss of insulin-like growth factor II (IGF2) imprinting, abrogation of silencing of the tumour suppressor gene p16INK4a, and growth suppression. Here we demonstrate that two enzymes cooperatively maintain DNA methylation and gene silencing in human cancer cells, and provide compelling evidence that such methylation is essential for optimal neoplastic proliferation.

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VL - 416

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JO - Nature

JF - Nature

IS - 6880

ER -

DNMT1 and DNMT3b cooperate to silence genes in human cancer cells

Abstract

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