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FANCJ/BRIP1在DNA损伤反应中对FANCD2的招募与调控

FANCJ/BRIP1 recruitment and regulation of FANCD2 in DNA damage responses.

作者信息

Zhang Fan, Fan Qiang, Ren Keqin, Auerbach Arleen D, Andreassen Paul R

机构信息

Division of Experimental Hematology and Cancer Biology, Cincinnati Children's Research Foundation, 3333 Burnet Ave. ML S7.203, Cincinnati, OH 45229, USA.

出版信息

Chromosoma. 2010 Dec;119(6):637-49. doi: 10.1007/s00412-010-0285-6. Epub 2010 Jul 31.

DOI:10.1007/s00412-010-0285-6
PMID:20676667
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4928586/
Abstract

FANCJ/BRIP1 encodes a helicase that has been implicated in the maintenance of genomic stability. Here, to better understand FANCJ function in DNA damage responses, we have examined the regulation of its cellular localization. FANCJ nuclear foci assemble spontaneously during S phase and are induced by various stresses. FANCJ foci colocalize with the replication fork following treatment with hydroxyurea, but not spontaneously. Using FANCJ mutants, we find that FANCJ helicase activity and the capacity to bind BRCA1 are both involved in FANCJ recruitment. Given similarities to the recruitment of another Fanconi anemia protein, FANCD2, we tested for colocalization of FANCJ and FANCD2. Importantly, these proteins show substantial colocalization, and FANCJ promotes the assembly of FANCD2 nuclear foci. This process is linked to the proper localization of FANCJ itself since both FANCJ and FANCD2 nuclear foci are compromised by FANCJ mutants that abrogate its helicase activity or interaction with BRCA1. Our results suggest that FANCJ is recruited in response to replication stress and that FANCJ/BRIP1 may serve to link FANCD2 to BRCA1.

摘要

FANCJ/BRIP1编码一种解旋酶,该酶与基因组稳定性的维持有关。在此,为了更好地理解FANCJ在DNA损伤反应中的功能,我们研究了其细胞定位的调控。FANCJ核灶在S期自发组装,并由各种应激诱导产生。用羟基脲处理后,FANCJ灶与复制叉共定位,但并非自发共定位。使用FANCJ突变体,我们发现FANCJ解旋酶活性和结合BRCA1的能力都参与了FANCJ的募集。鉴于与另一种范可尼贫血蛋白FANCD2的募集存在相似性,我们测试了FANCJ和FANCD2的共定位情况。重要的是,这些蛋白显示出大量共定位,并且FANCJ促进FANCD2核灶的组装。由于FANCJ和FANCD2核灶都因消除其解旋酶活性或与BRCA1相互作用的FANCJ突变体而受损,所以这个过程与FANCJ自身的正确定位有关。我们的结果表明,FANCJ是在复制应激反应中被募集的,并且FANCJ/BRIP1可能起到将FANCD2与BRCA1联系起来的作用。

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