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首页> 外文期刊>Biophysical Chemistry: An International Journal Devoted to the Physical Chemistry of Biological Phenomena >Global architecture of human poly(A)-specific ribonuclease by atomic force microscopy in liquid and dynamic light scattering.
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Global architecture of human poly(A)-specific ribonuclease by atomic force microscopy in liquid and dynamic light scattering.

机译:人类poly(A)特异性核糖核酸酶在液体和动态光散射中的原子力显微镜的全局体系结构。

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摘要

Deadenylation is the initial and often rate-limiting step in the main pathways of eukaryotic mRNA decay. Poly(A)-specific ribonuclease (PARN) is a eukaryotic enzyme that efficiently degrades mRNA poly(A) tails. Structural and functional studies have shown that human PARN is composed of at least three functional domains, i.e. the catalytic nuclease domain and two RNA binding domains, the R3H and the RNA recognition motif (RRM), respectively. However, the complete structure of the full length protein is still unknown. We have investigated the global architecture of human PARN by atomic force microscopy (AFM) imaging in buffered milieu and report for the first time the dimensions of the full length protein at subnanometer resolution. The AFM images of single PARN molecules reveal compact ellipsoidal dimers (10.9x7.6x4.6nm). The dimeric form of PARN was confirmed by dynamic light scattering (DLS) measurements that rendered a molecular weight of 161kDa, in accordance with previous crystal structures of PARN fragments showing a dimeric composition. We discuss a putative internal arrangement of three functional domains within the full length PARN dimer.
机译:腺苷酸化是真核mRNA衰变主要途径中的初始且通常是限速步骤。聚(A)特异性核糖核酸酶(PARN)是一种真核酶,可有效降解mRNA聚(A)尾巴。结构和功能研究表明,人PARN至少由三个功能域组成,即催化核酸酶域和两个RNA结合域,分别为R3H和RNA识别基序(RRM)。但是,全长蛋白的完整结构仍是未知的。我们已经通过缓冲环境中的原子力显微镜(AFM)成像研究了人类PARN的全球架构,并首次报告了亚纳米分辨率下全长蛋白质的尺寸。单个PARN分子的AFM图像显示出紧凑的椭圆形二聚体(10.9x7.6x4.6nm)。根据显示二聚体组成的PARN片段的先前晶体结构,通过动态光散射(DLS)测量证实了PARN的二聚体形式,所述动态光散射(DLS)测量使得分子量为161kDa。我们讨论了全长PARN二聚体中三个功能域的推定内部排列。

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