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Human endonuclease V is a ribonuclease specific for inosine-containing RNA

机译:人核酸内切酶V是一种特定于含肌苷RNA的核糖核酸酶

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Deamination of DNA bases can create missense mutations predisposing humans to cancer and also interfere with other basic molecular genetic processes; this deamination generates deoxyinosine from deoxyadenosine. In Escherichia coli, the highly conserved endonuclease V is involved in alternative excision repair that removes deoxyinosine from DNA. However, its exact activities and roles in humans are unknown. Here we characterize the FLJ35220 protein, the human homologue of E. coli endonuclease V, hEndoV as a ribonuclease specific for inosine-containing RNA. hEndoV preferentially binds to RNA and efficiently hydrolyses the second phosphodiester bond located 30' to the inosine in unpaired inosine-containing ssRNA regions in dsRNA. It localizes to the cytoplasm in cells. The ribonuclease activity is promoted by Tudor staphylococcal nuclease and detected on inosine-containing dsRNA created by the action of adenosine deaminases acting on RNA. These results demonstrate that hEndoV controls the fate of inosine-containing RNA in humans.
机译:DNA碱基的脱氨基会产生错义突变,使人类易患癌症,并且还会干扰其他基本分子遗传过程。该脱氨基从脱氧腺苷产生脱氧肌苷。在大肠杆菌中,高度保守的内切核酸酶V参与了从DNA中去除脱氧肌苷的替代切除修复。但是,其在人类中的确切活动和作用尚不清楚。在这里,我们将FLJ35220蛋白(人类大肠杆菌内切酶V,hEndoV的人类同源物)表征为对含肌苷的RNA特异的核糖核酸酶。 hEndoV优先结合RNA,并有效水解位于dsRNA中未配对的含肌苷的ssRNA区域中距肌苷30'的第二个磷酸二酯键。它定位于细胞中的细胞质。核糖核酸酶活性由Tudor葡萄球菌核酸酶促进,并在腺苷脱氨酶作用于RNA产生的含肌苷的dsRNA上检测到。这些结果证明,hEndoV控制着人体内含肌苷的RNA的命运。

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