Direct interaction of FANCD2 with BRCA2 in DNA damage response pathways

Hussain, Shobbir; Wilson, James B.; Medhurst, Annette L.; Hejna, James; Witt, Emily; Ananth, Sahana; Davies, Adelina A.; Masson, Jean‐Yves; Moses, Robb E.; West, Stephen C.; Winter, Johan P. de; Ashworth, Alan; Jones, Nigel J.; Mathew, Christopher G.

doi:10.1093/hmg/ddh135

Cited by 189 publications

(178 citation statements)

References 57 publications

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“…However, it is possible that USP1 may regulate the levels of other monoubiquitinated substrates in DNA repair pathways. Recent studies by our group and others have found that FANCD2 and PCNA colocalize at DNA repair foci during certain conditions of replication stress 17,18 (and data not shown). Therefore, we explored whether USP1 can deubiquitinate PCNA -a monoubiquitinated protein that localizes and functions at the DNA replication fork after UV damage or replication arrest.…”

mentioning

confidence: 64%

Regulation of monoubiquitinated PCNA by DUB autocleavage

et al. 2006

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Monoubiquitination is a reversible post-translational protein modification that has an important regulatory function in many biological processes, including DNA repair. Deubiquitinating enzymes (DUBs) are proteases that are negative regulators of monoubiquitination, but little is known about their regulation and contribution to the control of conjugated-substrate levels. Here, we show that the DUB ubiquitin specific protease 1 (USP1) deubiquitinates the DNA replication processivity factor, PCNA, as a safeguard against error-prone translesion synthesis (TLS) of DNA. Ultraviolet (UV) irradiation inactivates USP1 through an autocleavage event, thus enabling monoubiquitinated PCNA to accumulate and to activate TLS. Significantly, the site of USP1 cleavage is immediately after a conserved internal ubiquitin-like diglycine (Gly-Gly) motif. This mechanism is reminiscent of the processing of precursors of ubiquitin and ubiquitin-like modifiers by DUBs. Our results define a regulatory mechanism for protein ubiquitination that involves the signal-induced degradation of an inhibitory DUB.Monoubiquitination is a highly regulated process that is conserved in all eukaryotes 1,2 and controls a broad range of cellular functions, including DNA repair. Protein monoubiquitination is a reversible post-translational event that can be influenced by the opposing activities of a ubiquitin E3 ligase and a deubiquitinating enzyme (DUB), similar to the regulation of protein phosphorylation by kinases and phosphatases 3,4 . Protein monoubiquitination regulates the rescue of stalled DNA replication forks -an important cellular process required for cell survival 5 . The E2 ubiquitin conjugating enzyme RAD6 and the E3 ligase RAD18 are conserved in both yeast and human and they coordinate and activate the monoubiquitination of PCNA in response to UV damage or stalled replication forks [6][7][8] . Recent studies have shown that polη, a specialized TLS polymerase, is recruited to the replication fork through a specific interaction with monoubiquitinated PCNA 7 . The deployment of TLS polymerases during replication ensures timely bypass of the diverse DNA lesions encountered by the replication fork. Although many TLS polymerases are intrinsically mutagenic, polη allows replication past UV-damaged bases with high fidelity 9-11 . Thus, a model has emerged in which polη binds to monoubiquitinated PCNA and ensures accurate (error-free) replicative bypass of UV lesions. However, other (error-prone) TLS polymerases (such as polι and Rev1) have recently been shown to rely on monoubiquitinated PCNA for their function 12,13 . How cells limit PCNA monoubiquitination and the unwanted deployment of polη and/or other error-prone TLS polymerases in the absence or presence of extrinsic DNA damage during the synthesis of DNA in S phase is not known.In humans, protein deubiquitination is controlled by a family of approximately 95 distinct DUB enzymes 14,15 but the function of most of these proteins is unknown. DUBs are cysteine proteases that cleave ubiquitin fro...

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confidence: 64%

Regulation of monoubiquitinated PCNA by DUB autocleavage

et al. 2006

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“…Complex 1 is also essential for the inducible monoubiquitination of FANCD2 following cellular exposure to DNA damaging agents, such as MMC, ultraviolet (UV), or ionizing radiation (IR) and deoxynucleotide depletion due to hydroxyurea (Garcia-Higuera et al 2001;Gregory et al 2003). Following monoubiquitination, FANCD2 relocalizes from a soluble nuclear compartment to the chromatin fraction (Wang et al 2004) where it colocalizes in nuclear foci with other DNA damage response proteins, including FANCD1/BRCA2 (Hussain et al 2004;Wang et al 2004) BRCA1 (Garcia-Higuera et al 2001), RAD51 (Taniguchi et al 2002a;Hussain et al 2004), Proliferating Cell Nuclear Antigen (PCNA) (Hussain et al 2004), and Nijmegen Breakage Syndrome (NBS1) (Nakanishi et al 2002). Following relocalization to chromatin, monoubiquinated FANCD2 (FANCD2-Ub) promotes chromatin loading of the FANCD1/BRCA2 protein, forming a second complex (complex 2), where it may facilitate the formation of nuclear foci containing the homologous recombination (HR) DNA repair protein RAD51 (Wang et al 2004).…”

Section: The Basic Fa Pathwaymentioning

confidence: 99%

“…Accumulating evidence suggests a major function of complex 1 is to generate monoubiquitinated FANCD2 (FANCD2-Ub), required for the assembly of the FANCD2-Ub/BRCA2 chromatin complex (complex 2). Following monoubiquitination, FANCD2 relocalizes to DNA damage-induced S-phase foci where it associates with the DNA repair proteins BRCA2/FANCD1 (Wang (Nakanishi et al 2002), RAD51 (Hussain et al 2004), and PCNA (Howlett et al 2005). The formation of these DNA damage-induced FANCD2 foci is dependent on the presence of functional BRCA1 (Garcia-Higuera et al 2001), thereby linking this DNA repair protein to the FA pathway.…”

Section: The Structure Of the Fa Complexmentioning

confidence: 99%

The Fanconi Anemia/BRCA pathway: new faces in the crowd

Kennedy¹,

D’Andrea²

2005

Genes Dev.

362

345

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Over the past few years, study of the rare inherited chromosome instability disorder, Fanconi Anemia (FA), has uncovered a novel DNA damage response pathway. Through the cooperation of multiple proteins, this pathway regulates a complicated cellular response to DNA cross-linking agents and other genotoxic stresses. In this article we review recent data identifying new components of the FA pathway that implicate it in several aspects of the DNA damage response, including the direct processing of DNA, translesion synthesis, homologous recombination, and cell cycle regulation. We also discuss new findings that explain how the FA pathway is regulated through the processes of ubiquitination and deubiquitination. We then consider the clinical implications of our current understanding of the FA pathway, particularly in the development and treatment of malignancy in heterozygous carriers of FA mutations or in patients with sporadic cancers. We consider how recent studies of p53-mediated apoptosis and loss of p53 function in models of FA may help explain the clinical features of the disease and finally present a hypothesis to account for the specificity of the FA pathway in the response to DNA cross-links.

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“…FANCD2S+/FANCD2L+ phenotype in patients with a positive chromosome breakage test and FA clinical features suggests deleterious mutation on any of the genes functioning downstream of FANCD2 monoubiquitination. Three complementation groups corresponding to downstream proteins, that play their role after FANCD2 activation, have been identified (FANCD1/ BRCA2, FANCJ and FANCN) (9,15,19,28). Western blots for BRCA2 were performed on FANCD2S+/FANCD2L+ patients and all of them showed normal expression of this protein.…”

Section: Chromosome Breakage Test -Diepoxybutanementioning

confidence: 99%

“…The activation of this complex induced by DNA replication or by DNA-damage results in monoubiquitination of FANCD2, which moves into areas of damaged chromatin to interact with downstream FA members (FANCD1/BRCA2, FANCJ, FANCN) and other DNA-repair proteins such as BRCA1 and RAD51. FANCD2 is the central protein that connects the FA/BRCA pathway to the homologous recombination-mediated DNA repair (18,19,23,(25)(26)(27)(28). The recently identified FANCI protein associates with FANCD2 and is the second monoubiquitinated component of the FA pathway (14,29).…”

Section: Introductionmentioning

confidence: 99%

FANCD2 Western blot as a diagnostic tool for Brazilian patients with Fanconi anemia

Pilonetto

Pereira

Bitencourt

et al. 2009

Braz J Med Biol Res

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Fanconi anemia is a rare hereditary disease showing genetic heterogeneity due to a variety of mutations in genes involved in DNA repair pathways, which may lead to different clinical manifestations. Phenotypic variability makes diagnosis difficult based only on clinical manifestations, therefore laboratory tests are necessary. New advances in molecular pathogenesis of this disease led researchers to develop a diagnostic test based on Western blot for FANCD2. The objective of the present study was to determine the efficacy of this method for the diagnosis of 84 Brazilian patients with Fanconi anemia, all of whom tested positive for the diepoxybutane test, and 98 healthy controls. The FANCD2 monoubiquitinated isoform (FANCDS+/FANCD2L-) was not detected in 77 patients (91.7%). In 2 patients (2.4%), there was an absence of both the monoubiquitinated and the non-ubiquitinated proteins (FANCD2S-/FANCD2L-) and 5 patients (5.9%) had both isoforms (FANCD2S+/FANCD2L+). This last phenotype suggests downstream subtypes or mosaicism. All controls were diepoxybutane negative and were also negative on the FANCD2 Western blot. The Western blot for FANCD2 presented a sensitivity of 94% (79/84) and specificity of 100% (98/98). This method was confirmed as an efficient approach to screen Brazilian patients with deleterious mutations on FANCD2 (FANCD2S-/FANCD2L-) or other upstream genes of the FA/BRCA pathway (FANCDS+/FANCD2L-), to confirm the chromosome breakage test and to classify patients according to the level of FA/BRCA pathway defects. However, patients showing both FANCD2 isoforms (FANCD2S+/FANCD2L+) require additional studies to confirm mutations on downstream Fanconi anemia genes or the presence of mosaicism.

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Direct interaction of FANCD2 with BRCA2 in DNA damage response pathways

Cited by 189 publications

References 57 publications

Regulation of monoubiquitinated PCNA by DUB autocleavage

Regulation of monoubiquitinated PCNA by DUB autocleavage

The Fanconi Anemia/BRCA pathway: new faces in the crowd

FANCD2 Western blot as a diagnostic tool for Brazilian patients with Fanconi anemia

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