ZNF365 promotes stability of fragile sites and telomeres

Yuqing Zhang; Sandra J. Shin; Debra Liu; Elena Ivanova; Friedrich Foerster; Haoqiang Ying; Hongwu Zheng; Yonghong Xiao; Zhengming Chen; Alexei Protopopov; Ronald A. DePinho; Ji Hye Paik

doi:10.1158/2159-8290.CD-12-0536

ZNF365 promotes stability of fragile sites and telomeres

Yuqing Zhang, Sandra J. Shin, Debra Liu, Elena Ivanova, Friedrich Foerster, Haoqiang Ying, Hongwu Zheng, Yonghong Xiao, Zhengming Chen, Alexei Protopopov, Ronald A. DePinho, Ji Hye Paik

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

17 Scopus citations

Abstract

Critically short telomeres activate cellular senescence or apoptosis, as mediated by the tumor suppressor p53, but in the absence of this checkpoint response, telomere dysfunction engenders chromosomal aberrations and cancer. Here, analysis of p53-regulated genes activated in the setting of telomere dysfunction identified Zfp365 (ZNF365 in humans) as a direct p53 target that promotes genome stability. Germline polymorphisms in the ZNF365 locus are associated with increased cancer risk, including those associated with telomere dysfunction. On the mechanistic level, ZNF365 suppresses expression of a subset of common fragile sites, including telomeres. In the absence of ZNF365, defective telomeres engage in aberrant recombination of telomere ends, leading to increased telomere sister chromatid exchange and formation of anaphase DNA bridges, including ultra-fine DNA bridges, and ultimately increased cytokinesis failure and aneuploidy. Thus, the p53-ZNF365 axis contributes to genomic stability in the setting of telomere dysfunction. Significance: The contribution of the p53-ZNF365-telomere axis in the suppression of genomic instability illuminates how alterations in this pathway may confer increased cancer risk for individuals harboring germline alterations in the ZNF365 locus.

Original language	English (US)
Pages (from-to)	798-811
Number of pages	14
Journal	Cancer discovery
Volume	3
Issue number	7
DOIs	https://doi.org/10.1158/2159-8290.CD-12-0536
State	Published - Jul 2013

ASJC Scopus subject areas

Oncology

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Cytogenetics and Cell Authentication Core

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10.1158/2159-8290.CD-12-0536

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title = "ZNF365 promotes stability of fragile sites and telomeres",

abstract = "Critically short telomeres activate cellular senescence or apoptosis, as mediated by the tumor suppressor p53, but in the absence of this checkpoint response, telomere dysfunction engenders chromosomal aberrations and cancer. Here, analysis of p53-regulated genes activated in the setting of telomere dysfunction identified Zfp365 (ZNF365 in humans) as a direct p53 target that promotes genome stability. Germline polymorphisms in the ZNF365 locus are associated with increased cancer risk, including those associated with telomere dysfunction. On the mechanistic level, ZNF365 suppresses expression of a subset of common fragile sites, including telomeres. In the absence of ZNF365, defective telomeres engage in aberrant recombination of telomere ends, leading to increased telomere sister chromatid exchange and formation of anaphase DNA bridges, including ultra-fine DNA bridges, and ultimately increased cytokinesis failure and aneuploidy. Thus, the p53-ZNF365 axis contributes to genomic stability in the setting of telomere dysfunction. Significance: The contribution of the p53-ZNF365-telomere axis in the suppression of genomic instability illuminates how alterations in this pathway may confer increased cancer risk for individuals harboring germline alterations in the ZNF365 locus.",

author = "Yuqing Zhang and Shin, {Sandra J.} and Debra Liu and Elena Ivanova and Friedrich Foerster and Haoqiang Ying and Hongwu Zheng and Yonghong Xiao and Zhengming Chen and Alexei Protopopov and DePinho, {Ronald A.} and Paik, {Ji Hye}",

year = "2013",

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doi = "10.1158/2159-8290.CD-12-0536",

language = "English (US)",

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T1 - ZNF365 promotes stability of fragile sites and telomeres

AU - Zhang, Yuqing

AU - Shin, Sandra J.

AU - Liu, Debra

AU - Ivanova, Elena

AU - Foerster, Friedrich

AU - Ying, Haoqiang

AU - Zheng, Hongwu

AU - Xiao, Yonghong

AU - Chen, Zhengming

AU - Protopopov, Alexei

AU - DePinho, Ronald A.

AU - Paik, Ji Hye

PY - 2013/7

Y1 - 2013/7

N2 - Critically short telomeres activate cellular senescence or apoptosis, as mediated by the tumor suppressor p53, but in the absence of this checkpoint response, telomere dysfunction engenders chromosomal aberrations and cancer. Here, analysis of p53-regulated genes activated in the setting of telomere dysfunction identified Zfp365 (ZNF365 in humans) as a direct p53 target that promotes genome stability. Germline polymorphisms in the ZNF365 locus are associated with increased cancer risk, including those associated with telomere dysfunction. On the mechanistic level, ZNF365 suppresses expression of a subset of common fragile sites, including telomeres. In the absence of ZNF365, defective telomeres engage in aberrant recombination of telomere ends, leading to increased telomere sister chromatid exchange and formation of anaphase DNA bridges, including ultra-fine DNA bridges, and ultimately increased cytokinesis failure and aneuploidy. Thus, the p53-ZNF365 axis contributes to genomic stability in the setting of telomere dysfunction. Significance: The contribution of the p53-ZNF365-telomere axis in the suppression of genomic instability illuminates how alterations in this pathway may confer increased cancer risk for individuals harboring germline alterations in the ZNF365 locus.

AB - Critically short telomeres activate cellular senescence or apoptosis, as mediated by the tumor suppressor p53, but in the absence of this checkpoint response, telomere dysfunction engenders chromosomal aberrations and cancer. Here, analysis of p53-regulated genes activated in the setting of telomere dysfunction identified Zfp365 (ZNF365 in humans) as a direct p53 target that promotes genome stability. Germline polymorphisms in the ZNF365 locus are associated with increased cancer risk, including those associated with telomere dysfunction. On the mechanistic level, ZNF365 suppresses expression of a subset of common fragile sites, including telomeres. In the absence of ZNF365, defective telomeres engage in aberrant recombination of telomere ends, leading to increased telomere sister chromatid exchange and formation of anaphase DNA bridges, including ultra-fine DNA bridges, and ultimately increased cytokinesis failure and aneuploidy. Thus, the p53-ZNF365 axis contributes to genomic stability in the setting of telomere dysfunction. Significance: The contribution of the p53-ZNF365-telomere axis in the suppression of genomic instability illuminates how alterations in this pathway may confer increased cancer risk for individuals harboring germline alterations in the ZNF365 locus.

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ZNF365 promotes stability of fragile sites and telomeres

Abstract

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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