Plasticity of BRCA2 Function in Homologous Recombination: Genetic Interactions of the PALB2 and DNA Binding Domains

Siaud, Nicolas; Barbera, Maria; Egashira, Akinori; Lam, Isabel; Christ, Nicole; Schlacher, Katharina; Xia, Bing; Jasin, Maria

doi:10.1371/journal.pgen.1002409

Cited by 74 publications

(94 citation statements)

References 54 publications

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“…Consistent with the conclusion that HR is not restored, CHD4 depletion did not enhance break-induced HR in the BRCA2 mutant VC-8 hamster cell line that includes an integrated SCE-1 break-inducible DR-GFP reporter, (Pierce et al 1999), but GFP-positive cells were recovered, as expected, by introduction of a functional BRCA2 ( Fig. 3D; Siaud et al 2011).…”

Section: Resultssupporting

confidence: 86%

Resistance to therapy in BRCA2 mutant cells due to loss of the nucleosome remodeling factor CHD4

et al. 2015

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Hereditary cancers derive from gene defects that often compromise DNA repair. Thus, BRCA-associated cancers are sensitive to DNA-damaging agents such as cisplatin. The efficacy of cisplatin is limited, however, by the development of resistance. One cisplatin resistance mechanism is restoration of homologous recombination (HR), which can result from BRCA reversion mutations. However, in BRCA2 mutant cancers, cisplatin resistance can occur independently of restored HR by a mechanism that remains unknown. Here we performed a genome-wide shRNA screen and found that loss of the nucleosome remodeling factor CHD4 confers cisplatin resistance. Restoration of cisplatin resistance is independent of HR but correlates with restored cell cycle progression, reduced chromosomal aberrations, and enhanced DNA damage tolerance. Suggesting clinical relevance, cisplatin-resistant clones lacking genetic reversion of BRCA2 show de novo loss of CHD4 expression in vitro. Moreover, BRCA2 mutant ovarian cancers with reduced CHD4 expression significantly correlate with shorter progression-free survival and shorter overall survival. Collectively, our findings indicate that CHD4 modulates therapeutic response in BRCA2 mutant cancer cells.

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Section: Resultssupporting

confidence: 86%

Resistance to therapy in BRCA2 mutant cells due to loss of the nucleosome remodeling factor CHD4

et al. 2015

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“…There is no evidence as yet to suggest that there is a second cryptic DNA-binding domain in the N-terminal region of BRCA2 as in the case with Brh2 and the NBD. But a similar kind of dualistic behavior as noted with Brh2 seems apparent from the studies with the synthetic BRCA2 fusions [29]. HR is functional in the absence of the DBD so long as there is PALB2 interaction, and conversely, HR is functional when PALB2 is removed so long as the DBD remains.…”

Section: Discussionmentioning

confidence: 60%

“…A similar situation prevails in the mammalian system where it was found using synthetic BRCA2 constructs prepared by fusing different domains that abolishing the DBD had little impact on HR so long as the ability to associate with PALB2 was maintained [29]. PALB2 is a partner of BRCA2 that physically interacts with the N-terminal region of BRCA2 and that has its own intrinsic DNA binding domain [30].…”

Section: Discussionmentioning

confidence: 92%

Dual DNA-binding domains shape the interaction of Brh2 with DNA

Zhou¹,

Holloman²

2014

DNA Repair

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Brh2, the BRCA2 ortholog in the fungus Ustilago maydis, harbors two different DNA-binding domains, one located in the N-terminal region and the other located in the C-terminal region. Here we were interested in comparing the biochemical properties of Brh2 fragments, Brh2NT and Brh2CT, respectively, harboring the two different DNA-binding regions to understand the mechanistic purpose of dual DNA-interaction domains. With oligonucleotide substrates to model different DNA conformations, it was found that the substrate specificity of Brh2NT and Brh2CT was almost indistinguishable although avidity was different depending on salt concentration. DNA annealing activity inherent in Brh2 was found to be attributable to Brh2NT. Likewise, activity responsible for a second-end capture reaction modeling a later step in repair of DNA double-strand breaks was found attributable to Brh2NT. Efficient annealing of DNA strands coated with RPA required full length Brh2 rather than Brh2NT suggesting Brh2CT contributes to the activity when RPA is present. Brh2NT and Brh2CT were both found capable of physically interacting with RPA. The results suggest that while the two DNA-binding regions of Brh2 appear functionally redundant in certain aspects of DNA repair, they differ in fundamental properties, and likely contribute in different ways to repair processes involving or arising from stalled DNA replication forks.

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“…Prior work using BRC repeat regions shows that they also (less efficiently) specifically promote the formation of ssDNA-RAD51 complexes by blocking the ATPase activity of RAD51, which promotes disassembly [1171][1172][1173]. Genetic analysis in V79 hamster cells suggests functional redundancy within this complex HRR protein [1174].…”

Section: Brca2 and Associated Factors In Dynamic Regulation Of Rad51 mentioning

confidence: 99%

Recognition, signaling, and repair of DNA double-strand breaks produced by ionizing radiation in mammalian cells: The molecular choreography

Thompson

2012

Mutation Research/Reviews in Mutation Research

318

283

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Plasticity of BRCA2 Function in Homologous Recombination: Genetic Interactions of the PALB2 and DNA Binding Domains

Cited by 74 publications

References 54 publications

Resistance to therapy in BRCA2 mutant cells due to loss of the nucleosome remodeling factor CHD4

Resistance to therapy in BRCA2 mutant cells due to loss of the nucleosome remodeling factor CHD4

Dual DNA-binding domains shape the interaction of Brh2 with DNA

Recognition, signaling, and repair of DNA double-strand breaks produced by ionizing radiation in mammalian cells: The molecular choreography

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