Haploinsufficiency of <i>RAD51B</i> Causes Centrosome Fragmentation and Aneuploidy in Human Cells

Date, Osamu; Katsura, Mari; Ishida, Mari; Yoshihara, Takashi; Kinomura, Aiko; Sueda, Taijiro; Miyagawa, Kiyoshi

doi:10.1158/0008-5472.can-05-2803

Cited by 47 publications

(36 citation statements)

References 45 publications

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“…1). Consistent with previous studies (39,44), the RAD51B knockdown MCF7 cells exhibited a comparable reduction in RAD51 foci formation on the DSB sites after ionizing radiation (Fig. 1, B and C).…”

Section: Resultssupporting

confidence: 91%

“…RAD51B-deficient cells are hypersensitive to DSB-inducing agents, such as cisplatin, mitomycin C (MMC), and ␥-rays, indicating that the RAD51B protein is involved in the HRR pathway (39 -44). Genetic experiments revealed that RAD51B-deficient cells exhibited impaired RAD51 assembly onto DSB sites (39,44), suggesting that the RAD51B protein functions in the early stage of the HRR pathway. Biochemical experiments also suggested that the RAD51B protein participates in the early to late stages of the HRR pathway (45)(46)(47).…”

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confidence: 99%

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Recombination Activator Function of the Novel RAD51- and RAD51B-binding Protein, Human EVL

Takaku

Machida

Hosoya

et al. 2009

Journal of Biological Chemistry

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The RAD51 protein is a central player in homologous recombinational repair. The RAD51B protein is one of five RAD51 paralogs that function in the homologous recombinational repair pathway in higher eukaryotes. In the present study, we found that the human EVL (Ena/Vasp-like) protein, which is suggested to be involved in actin-remodeling processes, unexpectedly binds to the RAD51 and RAD51B proteins and stimulates the RAD51-mediated homologous pairing and strand exchange. The EVL knockdown cells impaired RAD51 assembly onto damaged DNA after ionizing radiation or mitomycin C treatment. The EVL protein alone promotes single-stranded DNA annealing, and the recombination activities of the EVL protein are further enhanced by the RAD51B protein. The expression of the EVL protein is not ubiquitous, but it is significantly expressed in breast cancer-derived MCF7 cells. These results suggest that the EVL protein is a novel recombination factor that may be required for repairing specific DNA lesions, and that may cause tumor malignancy by its inappropriate expression.Chromosomal DNA double strand breaks (DSBs) 2 are potential inducers of chromosomal aberrations and tumorigenesis, and they are accurately repaired by the homologous recombinational repair (HRR) pathway, without base substitutions, deletions, and insertions (1-3). In the HRR pathway (4, 5), single-stranded DNA (ssDNA) tails are produced at the DSB sites. The RAD51 protein, a eukaryotic homologue of the bacterial RecA protein, binds to the ssDNA tail and forms a helical nucleoprotein filament. The RAD51-ssDNA filament then binds to the intact double-stranded DNA (dsDNA) to form a threecomponent complex, containing ssDNA, dsDNA, and the RAD51 protein. In this three-component complex, the RAD51 protein promotes recombination reactions, such as homologous pairing and strand exchange (6 -9).The RAD51 protein requires auxiliary proteins to promote the homologous pairing and strand exchange reactions efficiently in cells (10 -12). In humans, the RAD52, RAD54, and RAD54B proteins directly interact with the RAD51 protein (13-17) and stimulate the RAD51-mediated homologous pairing and/or strand exchange reactions in vitro (18 -21). The human RAD51AP1 protein, which directly binds to the RAD51 protein (22), was also found to stimulate RAD51-mediated homologous pairing in vitro (23, 24). The BRCA2 protein contains ssDNA-binding, dsDNA-binding, and RAD51-binding motifs (25)(26)(27)(28)(29)(30)(31)(32)(33), and the Ustilago maydis BRCA2 ortholog, Brh2, reportedly stimulated RAD51-mediated strand exchange (34,35). Most of these RAD51-interacting factors are known to be required for efficient RAD51 assembly onto DSB sites in cells treated with ionizing radiation (10 -12).The RAD51B (RAD51L1, Rec2) protein is a member of the RAD51 paralogs, which share about 20 -30% amino acid sequence similarity with the RAD51 protein (36 -38). RAD51B-deficient cells are hypersensitive to DSB-inducing agents, such as cisplatin, mitomycin C (MMC), and ␥-rays, indicating that the RAD51B protei...

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Section: Resultssupporting

confidence: 91%

mentioning

confidence: 99%

Recombination Activator Function of the Novel RAD51- and RAD51B-binding Protein, Human EVL

Takaku

Machida

Hosoya

et al. 2009

Journal of Biological Chemistry

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“…However, 48 hours after irradiation, the proportion of cells with fragmented centrosomes was similar to the level observed for both unirradiated cell lines. Taken together, these results indicate that depletion of PARG exacerbates the centrosome amplification and fragmentation that has been already described in irradiated cells, in cells deficient in proteins involved in DSB repair or in cells overexpressing PARP3 and treated with an alkylating agent (Augustin et al, 2003;Date et al, 2006;Griffin et al, 2000).…”

Section: Irradiated Parg Kd Cells Display Centrosomal Abnormalitiessupporting

confidence: 77%

Radiation-induced mitotic catastrophe in PARG-deficient cells

Amé

Fouquerel

Gauthier

et al. 2009

Journal of Cell Science

110

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“…A growing body of evidence suggests that aneuploidy is often caused by chromosomal instability during mitosis (3,4), which may result from an improper duplication of centrosomes. The centrosome organizes the spindles for the separation of chromosomes during mitosis, and the presence of more than two centrosomes in a cell can result in lost chromosomes or in an excess number of chromosomes (2,5).…”

Section: Introductionmentioning

confidence: 99%

Inactivation of the Nijmegen Breakage Syndrome Gene Leads to Excess Centrosome Duplication via the ATR/BRCA1 Pathway

et al. 2009

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Nijmegen breakage syndrome is characterized by genomic instability and a predisposition for lymphoma and solid tumors. Nijmegen breakage syndrome 1 (NBS1), the protein which is mutated in these patients, functions in association with BRCA1 and ATR as part of the cellular response to DNA double-strand breaks. We show here that NBS1 forms foci at the centrosomes via an interaction with ;-tubulin. Down-regulation of NBS1 by small interfering RNA induces supernumerary centrosomes, and this was confirmed with experiments using Nbs1 knockout mouse cells; the introduction of wild-type NBS1 (wt-NBS1) cDNA into these knockout mouse cells reduced the number of supernumerary centrosomes to normal levels. This phenotype in NBS1-deficient cells is caused by both centrosome duplication and impaired separation of centrioles, which have been observed in BRCA1-inhibited cells. In fact, supernumerary centrosomes were observed in Brca1 knockout mouse cells, and the frequency was not affected by NBS1 down-regulation, suggesting that NBS1 maintains centrosomes via a common pathway with BRCA1. This is consistent with findings that NBS1 physically interacts with BRCA1 at the centrosomes and is required for BRCA1-mediated ubiquitination of ;-tubulin. Moreover, the ubiquitination of ;-tubulin is compromised by either ATR depletion or an NBS1 mutation in the ATR interacting (FHA) domain, which is essential for ATR activation. These results suggest that, although centrosomes lack DNA, the NBS1/ATR/ BRCA1 repair machinery affects centrosome behavior, and this might be a crucial role in the prevention of malignances.

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Haploinsufficiency of RAD51B Causes Centrosome Fragmentation and Aneuploidy in Human Cells

Cited by 47 publications

References 45 publications

Recombination Activator Function of the Novel RAD51- and RAD51B-binding Protein, Human EVL

Recombination Activator Function of the Novel RAD51- and RAD51B-binding Protein, Human EVL

Radiation-induced mitotic catastrophe in PARG-deficient cells

Inactivation of the Nijmegen Breakage Syndrome Gene Leads to Excess Centrosome Duplication via the ATR/BRCA1 Pathway

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