Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer

Yuanhui Jia; Pishun Li; Lan Fang; Haijun Zhu; Liangliang Xu; Hao Cheng; Junying Zhang; Fei Li; Yan Feng; Yan Li; Jialun Li; Ruiping Wang; James X. Du; Jiwen Li; Taiping Chen; Hongbin Ji; Jackie Han; Wenqiang Yu; Qihan Wu; Jiemin Wong

doi:10.1038/celldisc.2016.7

Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer

Yuanhui Jia, Pishun Li, Lan Fang, Haijun Zhu, Liangliang Xu, Hao Cheng, Junying Zhang, Fei Li, Yan Feng, Yan Li, Jialun Li, Ruiping Wang, James X. Du, Jiwen Li, Taiping Chen, Hongbin Ji, Jackie Han, Wenqiang Yu, Qihan Wu, Jiemin Wong

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

71 Scopus citations

Abstract

Global DNA hypomethylation is a most common epigenetic alteration in cancer, but the mechanism remains elusive. Previous studies demonstrate that UHRF1 but not UHRF2 is required for mediating DNA maintenance methylation by DNMT1. Here we report unexpectedly a conserved function for UHRF1 and UHRF2: inhibiting de novo DNA methylation by functioning as E3 ligases promoting DNMT3A degradation. UHRF1/2 are frequently overexpressed in cancers and we present evidence that UHRF1/2 overexpression downregulates DNMT3A proteins and consequently leads to DNA hypomethylation. Abrogating this negative regulation on DNMT3A or overexpression of DNMT3A leads to increased DNA methylation and impaired tumor growth. We propose a working model that UHRF1/2 safeguards the fidelity of DNA methylation and suggests that UHRF1/2 overexpression is likely a causal factor for widespread DNA hypomethylation in cancer via suppressing DNMT3A.

Original language	English (US)
Article number	16007
Journal	Cell Discovery
Volume	2
DOIs	https://doi.org/10.1038/celldisc.2016.7
State	Published - Apr 12 2016
Externally published	Yes

Keywords

DNA
DNMT1
DNMT3A
UHRF1
UHRF2
cancer
hypomethylation

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Genetics
Cell Biology

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Jia, Y., Li, P., Fang, L., Zhu, H., Xu, L., Cheng, H., Zhang, J., Li, F., Feng, Y., Li, Y., Li, J., Wang, R., Du, J. X., Li, J., Chen, T., Ji, H., Han, J., Yu, W., Wu, Q., & Wong, J. (2016). Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer. Cell Discovery, 2, Article 16007. https://doi.org/10.1038/celldisc.2016.7

Jia, Y, Li, P, Fang, L, Zhu, H, Xu, L, Cheng, H, Zhang, J, Li, F, Feng, Y, Li, Y, Li, J, Wang, R, Du, JX, Li, J, Chen, T, Ji, H, Han, J, Yu, W, Wu, Q & Wong, J 2016, 'Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer', Cell Discovery, vol. 2, 16007. https://doi.org/10.1038/celldisc.2016.7

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title = "Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer",

abstract = "Global DNA hypomethylation is a most common epigenetic alteration in cancer, but the mechanism remains elusive. Previous studies demonstrate that UHRF1 but not UHRF2 is required for mediating DNA maintenance methylation by DNMT1. Here we report unexpectedly a conserved function for UHRF1 and UHRF2: inhibiting de novo DNA methylation by functioning as E3 ligases promoting DNMT3A degradation. UHRF1/2 are frequently overexpressed in cancers and we present evidence that UHRF1/2 overexpression downregulates DNMT3A proteins and consequently leads to DNA hypomethylation. Abrogating this negative regulation on DNMT3A or overexpression of DNMT3A leads to increased DNA methylation and impaired tumor growth. We propose a working model that UHRF1/2 safeguards the fidelity of DNA methylation and suggests that UHRF1/2 overexpression is likely a causal factor for widespread DNA hypomethylation in cancer via suppressing DNMT3A.",

keywords = "DNA, DNMT1, DNMT3A, UHRF1, UHRF2, cancer, hypomethylation",

author = "Yuanhui Jia and Pishun Li and Lan Fang and Haijun Zhu and Liangliang Xu and Hao Cheng and Junying Zhang and Fei Li and Yan Feng and Yan Li and Jialun Li and Ruiping Wang and Du, {James X.} and Jiwen Li and Taiping Chen and Hongbin Ji and Jackie Han and Wenqiang Yu and Qihan Wu and Jiemin Wong",

note = "Funding Information: We thank Drs David Stewart and Christian Zwieb for critical reading of the manuscript and Drs Guoliang Xu and Yanhui Xu for reagents. We also thank Dr Xiufeng Peng for technical help in the mouse xenograft model. This study was supported by grants from the National Natural Science Foundation of China (91419303, and 81530078), The National Science and Technology (2014ZX09507-002 and 2015CB910402) and the Science Technology Commission of Shanghai Municipality (14xD1401700 and 11DZ2260300).",

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doi = "10.1038/celldisc.2016.7",

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AU - Jia, Yuanhui

AU - Li, Pishun

AU - Fang, Lan

AU - Zhu, Haijun

AU - Xu, Liangliang

AU - Cheng, Hao

AU - Zhang, Junying

AU - Li, Fei

AU - Feng, Yan

AU - Li, Yan

AU - Li, Jialun

AU - Wang, Ruiping

AU - Du, James X.

AU - Li, Jiwen

AU - Chen, Taiping

AU - Ji, Hongbin

AU - Han, Jackie

AU - Yu, Wenqiang

AU - Wu, Qihan

AU - Wong, Jiemin

N1 - Funding Information: We thank Drs David Stewart and Christian Zwieb for critical reading of the manuscript and Drs Guoliang Xu and Yanhui Xu for reagents. We also thank Dr Xiufeng Peng for technical help in the mouse xenograft model. This study was supported by grants from the National Natural Science Foundation of China (91419303, and 81530078), The National Science and Technology (2014ZX09507-002 and 2015CB910402) and the Science Technology Commission of Shanghai Municipality (14xD1401700 and 11DZ2260300).

PY - 2016/4/12

Y1 - 2016/4/12

N2 - Global DNA hypomethylation is a most common epigenetic alteration in cancer, but the mechanism remains elusive. Previous studies demonstrate that UHRF1 but not UHRF2 is required for mediating DNA maintenance methylation by DNMT1. Here we report unexpectedly a conserved function for UHRF1 and UHRF2: inhibiting de novo DNA methylation by functioning as E3 ligases promoting DNMT3A degradation. UHRF1/2 are frequently overexpressed in cancers and we present evidence that UHRF1/2 overexpression downregulates DNMT3A proteins and consequently leads to DNA hypomethylation. Abrogating this negative regulation on DNMT3A or overexpression of DNMT3A leads to increased DNA methylation and impaired tumor growth. We propose a working model that UHRF1/2 safeguards the fidelity of DNA methylation and suggests that UHRF1/2 overexpression is likely a causal factor for widespread DNA hypomethylation in cancer via suppressing DNMT3A.

AB - Global DNA hypomethylation is a most common epigenetic alteration in cancer, but the mechanism remains elusive. Previous studies demonstrate that UHRF1 but not UHRF2 is required for mediating DNA maintenance methylation by DNMT1. Here we report unexpectedly a conserved function for UHRF1 and UHRF2: inhibiting de novo DNA methylation by functioning as E3 ligases promoting DNMT3A degradation. UHRF1/2 are frequently overexpressed in cancers and we present evidence that UHRF1/2 overexpression downregulates DNMT3A proteins and consequently leads to DNA hypomethylation. Abrogating this negative regulation on DNMT3A or overexpression of DNMT3A leads to increased DNA methylation and impaired tumor growth. We propose a working model that UHRF1/2 safeguards the fidelity of DNA methylation and suggests that UHRF1/2 overexpression is likely a causal factor for widespread DNA hypomethylation in cancer via suppressing DNMT3A.

KW - DNA

KW - DNMT1

KW - DNMT3A

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KW - UHRF2

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Negative regulation of DNMT3A de novo DNA methylation by frequently overexpressed UHRF family proteins as a mechanism for widespread DNA hypomethylation in cancer

Abstract

Keywords

ASJC Scopus subject areas

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