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hDbr1 is a nucleocytoplasmic shuttling protein with a protein phosphatase-like motif essential for debranching activity.

机译:hDbr1是一种具有胞质穿梭蛋白,具有对脱支活性至关重要的蛋白磷酸酶样基序。

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摘要

In higher eukaryotes most genes contain multiple introns. Introns are excised from pre-mRNAs by splicing and eventually degraded in the nucleus. It is likely that rapid intron turnover in the nucleus is important in higher eukaryotes, but this pathway is poorly understood. In order to gain insights into this pathway, we analyzed the human lariat RNA debranching enzyme1 (hDbr1) protein that catalyzes debranching of lariat-intron RNAs. Transfection experiments demonstrate that hDbr1 is localized in a nucleoplasm of HeLa cells through a bipartite type nuclear localization signal near carboxyl-terminus. The conserved GNHE motif, originally identified in protein phosphatase protein family, is critical for hDbr1 to dissolve lariat structure in vitro. Furthermore, heterokaryon experiments show that hDbr1 is a nucleocytoplasmic shuttling protein, suggesting novel role(s) of hDbr1 in the cytoplasm.
机译:在高级真核生物中,大多数基因包含多个内含子。内含子通过剪接从前mRNA中切除,并最终在细胞核中降解。在高等真核生物中,核内快速内含子更新很重要,但对此途径了解甚少。为了获得对该途径的见解,我们分析了人类套索RNA脱支酶1(hDbr1)蛋白,该蛋白催化套索内含子RNA的脱支。转染实验表明,hDbr1通过靠近羧基末端的二分型核定位信号定位在HeLa细胞的核质中。最初在蛋白磷酸酶蛋白家族中鉴定的保守GNHE基序对于hDbr1在体外溶解套索结构至关重要。此外,异核体实验显示hDbr1是一种核质穿梭蛋白,提示hDbr1在细胞质中具有新的作用。

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