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首页> 外文期刊>The Journal of biological chemistry >Human Tribbles 3 Protects Nuclear DNA from Cytidine Deamination by APOBEC3A
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Human Tribbles 3 Protects Nuclear DNA from Cytidine Deamination by APOBEC3A

机译:人类的末端3通过apobec3a保护核DNA免受胞苷脱氨基

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The human polydeoxynucleotide cytidine deaminases APOBEC3A, APOBEC3C, and APOBEC3H are capable of mutating viral DNA in the nucleus, whereas APOBEC3A alone efficiently edits nuclear DNA. Deamination is rapidly followed by excision of uracil residues and can lead to double-stranded breaks. It is not known to which protein networks these DNA mutators belong. Using a yeast two-hybrid screen, we identified the human homolog of Drosophila Tribbles 3, TRIB3, as an interactor for APOBEC3A and APOBEC3C. The interaction was confirmed by co-affinity purification. Co-transfection of APOBEC3A with a TRIB3 expression vector reduced nuclear DNA editing whereas siRNA knockdown of TRIB3 increased the levels of nuclear DNA editing, indicating that TRIB3 functioned as a repressor of A3A. It also repressed A3A-associated γH2AX positive double-stranded breaks. The interaction results in degradation of A3A in a proteasome-independent manner. TRIB3 has been linked to cancer and via its own interactors and links the A3A DNA mutators to the Rb-BRCA1-ATM network. TRIB3 emerges as an important guardian of genome integrity.
机译:人聚佐寡核苷酸细胞苷脱胺酶apobec3a,apobec3c和apobec3h能够在细胞核中突变病毒性DNA,而单独的apobec3a有效地编辑核DNA。脱胺迅速接下来,切除尿嘧啶残留物,可以导致双链断裂。不知道这些DNA突变体属于哪些蛋白质网络。使用酵母双杂交筛网,我们鉴定了果蝇的人类同源物,Tribbers 3,Trib3,作为apobec3a和apobec3c的互动者。通过共亲和纯化证实相互作用。 APOBEC3A与TRED3表达载体的共转染核DNA编辑减少,而染色体3的siRNA敲低增加核DNA编辑水平,表明TRED3用作A3A阻遏物。它还抑制A3A相关的γH2AX正双链断裂。相互作用导致蛋白单级的方式降解A3A。 TRAD3已与癌症相关联,并通过其自身的交流剂与癌症联系起来并将A3A DNA突变体与RB-BRCA1-ATM网络联系起来。 TRIB3出现作为基因组完整性的重要监护人。

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