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Seipin 是一种离散的同源寡聚体。

Seipin is a discrete homooligomer.

机构信息

Department of Pharmacology, The University of Texas Southwestern Medical Center, Dallas,Texas 75390, United States.

出版信息

Biochemistry. 2010 Dec 21;49(50):10747-55. doi: 10.1021/bi1013003. Epub 2010 Nov 18.

Abstract

Seipin is a transmembrane protein that resides in the endoplasmic reticulum and concentrates at junctions between the ER and cytosolic lipid droplets. Mutations in the human seipin gene, including the missense mutation A212P, lead to congenital generalized lipodystrophy (CGL), characterized by the lack of normal adipose tissue and accumulation of fat in liver and muscles. In both yeast and CGL patient fibroblasts, seipin is required for normal lipid droplet morphology; in its absence droplets appear to bud abnormally from the ER. Here we report the first purification and physical characterization of seipin. Yeast seipin is in a large discrete protein complex. Affinity purification demonstrated that seipin is the main if not exclusive protein in the complex. Detergent sucrose gradients in H(2)O, and D(2)O and gel filtration were used to determine the size of the seipin complex and account for detergent binding. Both seipin-myc13 (seipin fused to 13 tandem copies of the myc epitope) expressed from the endogenous promoter and overexpressed seipin-mCherry form ∼500 kDa proteins consisting of about 9 copies of seipin. The yeast orthologue of the human A212P allele forms only smaller complexes and is unstable; we hypothesize that this accounts for its null phenotype in humans. Seipin appears as a toroid by negative staining electron microscopy. We speculate that seipin plays at least a structural role in organizing droplets or in communication between droplets and ER.

摘要

Seipin 是一种跨膜蛋白,位于内质网中,集中在 ER 和细胞质脂滴之间的连接处。人类 seipin 基因的突变,包括错义突变 A212P,导致先天性全身性脂肪营养不良(CGL),其特征是缺乏正常的脂肪组织和肝脏和肌肉中脂肪的积累。在酵母和 CGL 患者成纤维细胞中,seipin 是正常脂滴形态所必需的;在其缺失的情况下,液滴似乎从 ER 异常出芽。在这里,我们报告了 seipin 的首次纯化和物理特性。酵母 seipin 存在于一个大的离散蛋白复合物中。亲和纯化表明 seipin 是复合物中的主要(如果不是唯一的)蛋白。在 H2O 和 D2O 中进行的去污剂蔗糖梯度和凝胶过滤用于确定 seipin 复合物的大小并解释去污剂结合。从内源性启动子表达的 seipin-myc13(与 13 个串联的 myc 表位融合的 seipin)和过表达的 seipin-mCherry 形成约 500 kDa 的蛋白,由约 9 个 seipin 组成。人类 A212P 等位基因的酵母同源物只形成较小的复合物且不稳定;我们假设这解释了其在人类中的无效表型。Seipin 通过负染电子显微镜呈现为环形。我们推测 seipin 至少在组织液滴或液滴与 ER 之间的通信中发挥结构作用。

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