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英国和丹麦淀粉样肽通过分泌囊泡的轴突运输。

Axonal transport of British and Danish amyloid peptides via secretory vesicles.

作者信息

Choi Seung-Il, Vidal Ruben, Frangione Blas, Levy Efrat

机构信息

Department of Pathology, New York University School of Medicine, New York, New York, USA.

出版信息

FASEB J. 2004 Feb;18(2):373-5. doi: 10.1096/fj.03-0730fje. Epub 2003 Dec 4.

Abstract

The ABri and ADan amyloid peptides deposited in familial British and Danish neurodegenerative disorders are generated by processing mutant forms of the precursor protein BRI2. Although the pathogenic process that leads to deposition of amyloid in the brains of patients has been studied extensively, the cellular processes and normal function of the precursor protein did not receive much attention. We observed in a variety of transfected cell lines the presence of two independent proteolytic processing events. In addition to the previously described cleavage, which results in the production of carboxyl-terminal approximately 3 kDa wild-type peptide or approximately 4 kDa ABri or ADan peptides, we describe a novel amino-terminal cleavage site within BRI2. Both cleavages occur within the cis- or medial-Golgi. Following cleavage, the BRI2-derived carboxyl-terminal peptides are transported via a regulated secretory pathway into secretory vesicles in neuronal cells. Worth noting is that expression of wild-type British or Danish mutants of BRI2, in mouse neuroblastoma N2a cells that do not express endogenous BRI2, induces elongation of neurites, which suggests a role for this protein in differentiation of neuronal cells.

摘要

在家族性英国和丹麦神经退行性疾病中沉积的ABri和ADan淀粉样肽是由前体蛋白BRI2的突变形式加工产生的。尽管导致患者大脑中淀粉样蛋白沉积的致病过程已得到广泛研究,但前体蛋白的细胞过程和正常功能却未受到太多关注。我们在多种转染细胞系中观察到存在两种独立的蛋白水解加工事件。除了先前描述的切割,该切割导致产生羧基末端约3 kDa的野生型肽或约4 kDa的ABri或ADan肽外,我们还描述了BRI2内一个新的氨基末端切割位点。两种切割均发生在内质网或高尔基体中间。切割后,BRI2衍生的羧基末端肽通过调节性分泌途径转运到神经元细胞的分泌小泡中。值得注意的是,在不表达内源性BRI2的小鼠神经母细胞瘤N2a细胞中,BRI2的野生型英国或丹麦突变体的表达会诱导神经突伸长,这表明该蛋白在神经元细胞分化中起作用。

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