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Cancer and Metastasis Reviews
Erschienen in: Cancer and Metastasis Reviews 4/2014

01.12.2014

MTA family of proteins in DNA damage response: mechanistic insights and potential applications

verfasst von: Da-Qiang Li, Yinlong Yang, Rakesh Kumar

Erschienen in: Cancer and Metastasis Reviews | Ausgabe 4/2014

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Abstract

The DNA damage, most notably DNA double-strand breaks, poses a serious threat to the stability of mammalian genome. Maintenance of genomic integrity is largely dependent on an efficient, accurate, and timely DNA damage response in the context of chromatin. Consequently, dysregulation of the DNA damage response machinery is fundamentally linked to the genomic instability and a likely predisposition to cancer. In turn, aberrant activation of DNA damage response pathways in human cancers enables tumor cells to survive DNA damages, thus, leading to the development of resistance of tumor cells to DNA damaging radio- and chemotherapies. A substantial body of experimental evidence has established that ATP-dependent chromatin remodeling and histone modifications play a central role in the DNA damage response. As a component of the nucleosome remodeling and histone deacetylase (NuRD) complex that couples both ATP-dependent chromatin remodeling and histone deacetylase activities, the metastasis-associated protein (MTA) family proteins have been recently shown to participate in the DNA damage response beyond its well-established roles in gene transcription. In this thematic review, we will focus on our current understandings of the role of the MTA family proteins in the DNA damage response and their potential implications in DNA damaging anticancer therapy.
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Metadaten
Titel
MTA family of proteins in DNA damage response: mechanistic insights and potential applications
verfasst von
Da-Qiang Li
Yinlong Yang
Rakesh Kumar
Publikationsdatum
01.12.2014
Verlag
Springer US
Erschienen in
Cancer and Metastasis Reviews / Ausgabe 4/2014
Print ISSN: 0167-7659
Elektronische ISSN: 1573-7233
DOI
https://doi.org/10.1007/s10555-014-9524-2

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