DNAH2 facilitates the homologous recombination repair of Fanconi anemia pathway through modulating FANCD2 ubiquitination.

IF 1.5 Q3 HEMATOLOGY
血液科学(英文) Pub Date : 2021-06-07 eCollection Date: 2021-07-01 DOI:10.1097/BS9.0000000000000076
Lixian Chang, Xingjie Gao, Yuxia Wang, Chunmin Huang, Min Gao, Xiaomin Wang, Chao Liu, Wenqi Wu, Wenbin An, Yang Wan, Aoli Zhang, Yingchi Zhang, Weiping Yuan, Xiaofan Zhu
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引用次数: 0

Abstract

Fanconi anemia (FA), an X-linked genetic or autosomal recessive disease, exhibits complicated pathogenesis. Previously, we detected the mutated Dynein Axonemal Heavy Chain 2 (DNAH2) gene in 2 FA cases. Herein, we further investigated the potential association between DNAH2 and the homologous recombination repair pathway of FA. The assays of homologous recombination repair, mitomycin C (MMC) sensitivity, immunofluorescence, and ubiquitination modification were performed in U2OS and DR-U2OS cell lines. In MMC-treated U2OS cells, the downregulation of the DNAH2 gene increased the sensitivity of cells to DNA inter-strand crosslinks. We also observed the reduced enrichment of FANCD2 protein to DNA damage sites. Furthermore, the ubiquitination modification level of FANCD2 was influenced by the deficiency of DNAH2. Thus, our results suggest that DNAH2 may modulate the cell homologous recombination repair partially by increasing the ubiquitination and the enrichment to DNA damage sites of FANCD2. DNAH2 may act as a novel co-pathogenic gene of FA patients.

DNAH2通过调控FANCD2泛素化促进Fanconi贫血通路的同源重组修复
摘要范科尼贫血(FA)是一种X连锁遗传或常染色体隐性遗传疾病,发病机制复杂。此前,我们在2例FA病例中检测到Dynein-Axonemal重链2(DNAH2)基因突变。在此,我们进一步研究了DNAH2与FA同源重组修复途径之间的潜在联系。在U2OS和DR-U2OS细胞系中进行了同源重组修复、丝裂霉素C(MMC)敏感性、免疫荧光和泛素化修饰的测定。在MMC处理的U2OS细胞中,DNAH2基因的下调增加了细胞对DNA链间交联的敏感性。我们还观察到FANCD2蛋白对DNA损伤位点的富集减少。此外,FANCD2的泛素化修饰水平受到DNAH2缺乏的影响。因此,我们的结果表明,DNAH2可能通过增加FANCD2的泛素化和对DNA损伤位点的富集来部分调节细胞同源重组修复。DNAH2可能是FA患者的一种新的共致病基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
1.70
自引率
0.00%
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审稿时长
10 weeks
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