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In vivo structure-function analysis of human Dicer reveals directional processing of precursor miRNAs

机译:人类Dicer的体内结构功能分析揭示了前体miRNA的定向加工

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摘要

Dicer is an RNase III family endoribonuclease and haploinsufficient tumor suppressor that processes mature miRNAs from the 5′ (5p) or 3′ (3p) arm of hairpin precursors. In murine Dicer knockout fibroblasts, we expressed human Dicer with point mutations in the RNase III, helicase, and PAZ domains and characterized miRNA expression by Northern blot and massively parallel sequencing of small RNAs. We report that inactivation of the RNase IIIA domain results in complete loss of 3p-derived mature miRNAs, but only partial reduction in 5p-derived mature miRNAs. Conversely, inactivation of the RNase IIIB domain by mutation of D1709, a residue mutated in a subset of nonepithelial ovarian cancers, results in complete loss of 5p-derived mature miRNAs, including the tumor-suppressive let-7 family, but only partial reduction in 3p-derived mature miRNAs. Mutation of the PAZ domain results in global reduction of miRNA processing, while mutation of theWalker A motif in the helicase domain of Dicer does not alter miRNA processing. These results provide insight into the biochemical activity of human Dicer in vivo and, furthermore, suggest that mutation of the clinically relevant residue D1709 within the RNase IIIB results in a uniquely miRNA-haploinsufficient state in which the let-7 family of tumor suppressor miRNAs is lost while a complement of 3p-derived miRNAs remains expressed.
机译:Dicer是一种RNase III家族核糖核酸内切酶和单倍体不足的肿瘤抑制因子,可处理发夹前体5'(5p)或3'(3p)臂上的成熟miRNA。在鼠Dicer敲除成纤维细胞中,我们表达了人类Dicer,其在RNase III,解旋酶和PAZ域中具有点突变,并通过Northern印迹和小RNA的大规模平行测序表征了miRNA的表达。我们报告说,RNase IIIA域的失活导致3p衍生的成熟miRNA的完全丧失,但5p衍生的成熟miRNA的仅部分减少。相反,通过突变D1709(一种在非上皮性卵巢癌的子集中突变的残基)使RNase IIIB结构域失活,会导致5p衍生的成熟miRNA完全丧失,包括抑制肿瘤的let-7家族,但仅部分降低了3p衍生的成熟miRNA。 PAZ结构域的突变导致miRNA加工的整体减少,而Dicer解旋酶结构域中的Walker A基序的突变不会改变miRNA的加工。这些结果提供了对人类Dicer体内生物化学活性的深入了解,此外,提示RNase IIIB中临床相关残基D1709的突变会导致独特的miRNA-单倍体不足状态,在该状态下,let-7家族的抑癌miRNA处于丢失,而仍然表达互补的3p的miRNA。

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