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系统的去泛素化酶定位研究发现 USP21 是中心体和微管相关功能的调节因子。

Systematic survey of deubiquitinase localization identifies USP21 as a regulator of centrosome- and microtubule-associated functions.

机构信息

Cellular and Molecular Physiology, Institute of Translational Medicine, University of Liverpool, Liverpool L69 3BX, United Kingdom.

出版信息

Mol Biol Cell. 2012 Mar;23(6):1095-103. doi: 10.1091/mbc.E11-08-0668. Epub 2012 Feb 1.

Abstract

Ubiquitination is a reversible modification that influences a broad range of physiological processes. There are approximately 90 deubiquitinases (DUBs) encoded in the human genome, of which 79 are predicted to have catalytic activity. We tagged 66 DUBs with green fluorescent protein and systematically surveyed their subcellular distribution, identifying enzymes specific to the nucleus, plasma membrane, and secretory and endocytic pathways. USP21 is unique in showing clear association with both centrosomes and microtubules. Using an in vitro assay, we show that microtubule binding is direct and identify a novel microtubule-binding motif encompassed within amino acids 59-75 of the N-terminus of USP21. Our functional studies indicate a key role for USP21 in the governance of microtubule- and centrosome-associated physiological processes: Depletion of USP21 in A549 cells compromises the reestablishment of a radial array of microtubules during recovery from cold-induced depolymerization and also reduces the probability of primary cilium formation, whereas USP21 knockdown in PC12 cells inhibits nerve growth factor-induced neurite outgrowth.

摘要

泛素化是一种可逆的修饰,影响广泛的生理过程。人类基因组中约有 90 种去泛素化酶(DUBs),其中 79 种被预测具有催化活性。我们用绿色荧光蛋白标记了 66 种 DUBs,并系统地研究了它们的亚细胞分布,鉴定出了特定于核、质膜以及分泌和内吞途径的酶。USP21 是唯一一种与中心体和微管都有明显关联的酶。通过体外实验,我们证明了微管结合是直接的,并确定了 USP21 的 N 端氨基酸 59-75 内包含的一个新的微管结合基序。我们的功能研究表明,USP21 在微管和中心体相关生理过程的调控中起着关键作用:在 A549 细胞中耗尽 USP21 会影响冷诱导解聚后微管重新形成放射状排列,也会降低初级纤毛形成的概率,而在 PC12 细胞中敲低 USP21 会抑制神经生长因子诱导的神经突生长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/36f6/3302736/651a6b49ca8d/1095fig1.jpg

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