A YY1–INO80 complex regulates genomic stability through homologous recombination–based repair

Wu, Su; Shi, Yujiang Geno; Mulligan, Peter; Landry, Joseph W.; Liu, Huifei; Lu, J; Qi, Hank H.; Wang, Weijia; Nickoloff, Jac A.; Wu, Carl; Shi, Yang

doi:10.1038/nsmb1332

Cited by 187 publications

(239 citation statements)

References 47 publications

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“…IR-and UV-induced DNA damages persist in mIno80 ∆/∆ MEFs, suggesting that mIno80 is required for their efficient repair (Figure 3). In addition, we found that mIno80 is required for the generation of ssDNA to mediate HDR at sites of DSBs (Figure 4), in agreement with previous results showing that siRNA-mediated depletion of hIno80 impairs HDR [20,23].…”

Section: Discussionsupporting

confidence: 80%

“…As mIno80 promotes DNA repair and represses genome instability, we postulate that the mIno80 complex also plays a role in tumor prevention. This notion is supported by the observation that hIno80 and its associated protein YY-1 are required to maintain genome stability by promoting proper chromosome segregation [20,22]. We found that deletion of mIno80 severely compromised the tumorigenic potential of transformed mouse cell lines by reducing cellular proliferative capacity and the ability to form soft agar colonies in culture ( Figure 6).…”

Section: Discussionsupporting

confidence: 71%

“…Recent studies of mammalian INO80 functions by siRNA-mediated knockdown approaches revealed that this complex plays critical roles in the repair of DSBs and maintenance of genome stability [20][21][22][23][24]. However, little is known about INO80's function at mammalian telomeres.…”

Section: Introductionmentioning

confidence: 99%

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The mINO80 chromatin remodeling complex is required for efficient telomere replication and maintenance of genome stability

et al. 2013

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The INO80 (inositol requiring mutant 80) chromatin remodeling complex plays important roles in transcriptional regulation and DNA replication and repair, and consists of several functional protein subunits, including the critical Ino80 ATPase catalytic subunit. While the function of INO80 has been studied in yeast and mammalian cell lines, we do not know how mIno80 contributes to the maintenance of genome stability to prevent cancer development in mice. Here, we use a conditional knockout approach to explore the cellular and organismal functions of mIno80. Deletion of mIno80 results in profound cellular proliferative defects and activation of p21-dependent cellular senescence. While mIno80 is required for efficient repair of DNA double strand breaks, its depletion did not impact upon the formation of γ-H2AX and 53BP1 DNA damage foci, or the activation of the ATM-CHK2-dependent DNA damage response. mIno80 deletion inhibited the generation of single-strand DNA, resulting in defects in homology-directed DNA repair (HDR) at telomeres. Fragile telomeres were prominent in mIno80 ∆/∆ MEFs, suggesting that chromatin remodeling is required for efficient telomere replication. mIno80 −/− mouse embryos die early during embryogenesis, while conditional deletion of mIno80 in adult mice results in weight loss and premature death. In a p53 −/− tumorprone background, mIno80 haploinsufficiency favored the development of sarcomas. Our studies suggest that the mIno80 chromatin remodeling complex plays important roles in telomere replication, HDR-mediated repair of dysfunctional telomeres, and maintenance of genome stability.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionsupporting

confidence: 71%

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The mINO80 chromatin remodeling complex is required for efficient telomere replication and maintenance of genome stability

et al. 2013

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“…At the molecular level, it has been demonstrated that regulation of nucleosome deposition is essential for transcriptional activation or repression, 28 -30 DNA replication, 31,32 DNA damage repair, 4,33,34 and cell cycle progression. [35][36][37] Chromatin remodeling factors that control DNA winding/unwinding cycles are therefore believed to be involved in these processes.…”

Section: Discussionmentioning

confidence: 99%

Overexpression of a Chromatin Remodeling Factor, RSF-1/HBXAP, Correlates with Aggressive Oral Squamous Cell Carcinoma

Fang

Huang

et al. 2011

The American Journal of Pathology

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RSF-1, also known as hepatitis B X-antigen associated protein (HBXAP), is a subunit of an ISWI chromatin remodeling complex, remodeling and spacing factor (RSF). Recent studies have provided new evidence that chromatin remodeling participates in the pathogenesis of neoplastic diseases by altering cell cycle regulation and gene expression. In this report, we studied the biological roles of RSF-1 in oral squamous cell carcinoma (OSCC), a highly invasive neoplastic disease. Based on IHC and quantitative real-time PCR, we demonstrated that RSF-1 expression could be detected in the majority of OSCC cases, and the levels were significantly higher in OSCC cells than in their normal counterparts. Moreover, expression levels of RSF-1 significantly correlated with the presence of angiolymphatic invasion, abnormal mitoses, metastasis, tumor recurrence, and advanced stage disease at presentation. Univariate and multivariate analyses showed a significant association of RSF-1 overexpression and worse overall survival in OSCC patients. RSF-1 knockdown remarkably decreased cellular proliferation and induced apoptosis in OSCC cells with high RSF-1 expression levels, but not in those without. Taken together, our results suggest that RSF-1 up-regulation is associated with several clinicopathological features of disease aggressiveness in OSCC patients, and RSF-1 plays an important role in maintaining cellular growth and survival in OSCC.

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“…Yeast INO80 and SWR1 chromatin remodeling complexes interact with γ-H2A and facilitate DSB repair (van Attikum et al, 2007;Park et al, 2009). Wu and colleagues showed that knockdown models of human INO80, or of its binding partner YY1, increased cellular sensitivity toward DNAdamaging agents, and in their study they highlighted the essentiality of both INO80 and YY1 for HR repair (Wu, S. et al, 2007). However, a recent report indicated that H2A phosphorylation is dispensable for recruitment of the chromatin remodelers INO80 and SNF6 (a component of SWI/SNF) to DSB sites in yeast (Bennett et al, 2013), suggesting that the interaction with γ-H2AX may not be essential for directing the accumulation of histone remodelers at DSB damage sites.…”

Section: Introductionmentioning

confidence: 99%

Chromatin modification and NBS1: their relationship in DNA double-strand break repair

2015

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The importance of chromatin modification, including histone modification and chromatin remodeling, for DNA double-strand break (DSB) repair, as well as transcription and replication, has been elucidated. Phosphorylation of H2AX to γ-H2AX is one of the first responses following DSB detection, and this histone modification is important for the DSB damage response by triggering several events, including the accumulation of DNA damage response-related proteins and subsequent homologous recombination (HR) repair. The roles of other histone modifications such as acetylation, methylation and ubiquitination have also been recently clarified, particularly in the context of HR repair. NBS1 is a multifunctional protein that is involved in various DNA damage responses. Its recently identified binding partner RNF20 is an E3 ubiquitin ligase that facilitates the monoubiquitination of histone H2B, a process that is crucial for recruitment of the chromatin remodeler SNF2h to DSB damage sites. Evidence suggests that SNF2h functions in HR repair, probably through regulation of end-resection. Moreover, several recent reports have indicated that SNF2h can function in HR repair pathways as a histone remodeler and that other known histone remodelers can also participate in DSB damage responses. On the other hand, information about the roles of such chromatin modifications and NBS1 in non-homologous end joining (NHEJ) repair of DSBs and stalled fork-related damage responses is very limited; therefore, these aspects and processes need to be further studied to advance our understanding of the mechanisms and molecular players involved.

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A YY1–INO80 complex regulates genomic stability through homologous recombination–based repair

Cited by 187 publications

References 47 publications

The mINO80 chromatin remodeling complex is required for efficient telomere replication and maintenance of genome stability

The mINO80 chromatin remodeling complex is required for efficient telomere replication and maintenance of genome stability

Overexpression of a Chromatin Remodeling Factor, RSF-1/HBXAP, Correlates with Aggressive Oral Squamous Cell Carcinoma

Chromatin modification and NBS1: their relationship in DNA double-strand break repair

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