BBAP Monoubiquitylates Histone H4 at Lysine 91 and Selectively Modulates the DNA Damage Response

Yan, Qingsheng; Dutt, Shilpee; Xu, Rong; Graves, Katherine; Juszczyński, Przemysław; Manis, John P.; Shipp, Margaret A.

doi:10.1016/j.molcel.2009.08.019

Cited by 138 publications

(160 citation statements)

References 53 publications

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“…ADIPOR1 is the cognate receptor for adiponectin, which stimulates proliferation of hematopoietic stem cells (48). Although the precise function of the ubiquitin ligase DTX3L is not defined, recent work suggests that DTX3L monoubiquitylates histone H4 lysine 91 and thereby protects DNA from ROS (39). Here, we show that these genes are highly inducible by ROS and regulated by STAT1.…”

Section: Discussionmentioning

confidence: 62%

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STEAP1 Is Associated with the Invasive and Oxidative Stress Phenotype of Ewing Tumors

Grünewald

Diebold

Espósito

et al. 2012

Molecular Cancer Research

111

131

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Ewing tumors comprise the second most common type of bone-associated cancer in children and are characterized by oncogenic EWS/FLI1 fusion proteins and early metastasis. Compelling evidence suggests that elevated levels of intracellular oxidative stress contribute to enhanced aggressiveness of numerous cancers, possibly including Ewing tumors. Using comprehensive microarray analyses and RNA interference, we identified the six-transmembrane epithelial antigen of the prostate 1 (STEAP1)-a membrane-bound mesenchymal stem cell marker of unknown function-as a highly expressed protein in Ewing tumors compared with benign tissues and show its regulation by EWS/FLI1. In addition, we show that STEAP1 knockdown reduces Ewing tumor proliferation, anchorage-independent colony formation as well as invasion in vitro and decreases growth and metastasis of Ewing tumor xenografts in vivo. Moreover, transcriptome and proteome analyses as well as functional studies revealed that STEAP1 expression correlates with oxidative stress responses and elevated levels of reactive oxygen species that in turn are able to regulate redox-sensitive and proinvasive genes. In synopsis, our data suggest that STEAP1 is associated with the invasive behavior and oxidative stress phenotype of Ewing tumors and point to a hitherto unanticipated oncogenic function of STEAP1. Mol Cancer Res; 10(1); 52-65. Ó2011 AACR.

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Section: Discussionmentioning

confidence: 62%

“…We choose MMP-1, ADIPOR1, and DTX3L for follow-up due to their high expression in Ewing tumors and their involvement in oxidative stress responses (34,38,39). Notably, (Fig.…”

Section: Ros Are Critical For Ewing Tumor Proliferation and Invasivenessmentioning

confidence: 99%

STEAP1 Is Associated with the Invasive and Oxidative Stress Phenotype of Ewing Tumors

Grünewald

Diebold

Espósito

et al. 2012

Molecular Cancer Research

111

131

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“…Furthermore, Skp2 was shown to be responsible for PR-Set7 degradation after UV damage, outside the chromatin context (Oda et al 2010). BBAP, another E3 ligase, also regulates PR-Set7 protein levels (Yan et al 2009). However, neither Skp2 nor BBAP have been shown to directly ubiquitinate PR-Set7.…”

Section: Post-translational Regulation Of Pr-set7mentioning

confidence: 99%

PR-Set7 and H4K20me1: at the crossroads of genome integrity, cell cycle, chromosome condensation, and transcription

et al. 2012

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Histone post-translational modifications impact many aspects of chromatin and nuclear function. Histone H4 Lys 20 methylation (H4K20me) has been implicated in regulating diverse processes ranging from the DNA damage response, mitotic condensation, and DNA replication to gene regulation. PR-Set7/Set8/KMT5a is the sole enzyme that catalyzes monomethylation of H4K20 (H4K20me1). It is required for maintenance of all levels of H4K20me, and, importantly, loss of PR-Set7 is catastrophic for the earliest stages of mouse embryonic development. These findings have placed PR-Set7, H4K20me, and proteins that recognize this modification as central nodes of many important pathways. In this review, we discuss the mechanisms required for regulation of PR-Set7 and H4K20me1 levels and attempt to unravel the many functions attributed to these proteins.

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“…H4K20 methyltransferase MMSET (Wolf-Hirschhorn syndrome candidate 1) regulates the induction of H4K20 methylation on histones around double-strand breaks, which in turn facilitates 53BP1 recruitment (Hajdu et al, 2011;Pei et al, 2011). In addition to MMSET, another two H4K20 methyltransferases Set8 and Set9 are also responsible for H4K20 methylation and the recruitment of 53BP1 (Dulev et al, 2014;Greeson et al, 2008;Oda et al, 2010;Sanders et al, 2004;Yan et al, 2009). Similar to H3K79 methylation, H4K20 methylation recruits 53BP1 via its tandem Tudor domain as well (Botuyan et al, 2006).…”

Section: Methylationmentioning

confidence: 99%

“…However, the relationship between H2A/H2AX ubiquitination and H2AX is not clear. Moreover, some other ubiquitin E3 ligases, such as B-lymphoma and BAL-associated protein (BBAP) (Yan et al, 2009), RNF20-RNF40 heterodimer (Moyal et al, 2011;Nakamura et al, 2011), Cul4-DDBRoc1 and checkpoint with forkheadassociated (FHA) and RING finger domain protein (CHFR) , have been shown to be involved in his-tone ubiquitination in response to DNA damage as well.…”

Section: Ubiquitinationmentioning

confidence: 99%

Histone modifications in DNA damage response

Cao

Shen

Zhu

2016

Sci. China Life Sci.

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DNA damage is a relatively common event in eukaryotic cell and may lead to genetic mutation and even cancer. DNA damage induces cellular responses that enable the cell either to repair the damaged DNA or cope with the damage in an appropriate way. Histone proteins are also the fundamental building blocks of eukaryotic chromatin besides DNA, and many types of post-translational modifications often occur on tails of histones. Although the function of these modifications has remained elusive, there is ever-growing studies suggest that histone modifications play vital roles in several chromatin-based processes, such as DNA damage response. In this review, we will discuss the main histone modifications, and their functions in DNA damage response.DNA damage response, histone modifications, chromatin, DNA repair Citation:

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BBAP Monoubiquitylates Histone H4 at Lysine 91 and Selectively Modulates the DNA Damage Response

Cited by 138 publications

References 53 publications

STEAP1 Is Associated with the Invasive and Oxidative Stress Phenotype of Ewing Tumors

STEAP1 Is Associated with the Invasive and Oxidative Stress Phenotype of Ewing Tumors

PR-Set7 and H4K20me1: at the crossroads of genome integrity, cell cycle, chromosome condensation, and transcription

Histone modifications in DNA damage response

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