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核纤层蛋白A/C依赖的Nesprin-2定位,Nesprin-2是位于核膜的一种巨大支架蛋白。

Lamin A/C-dependent localization of Nesprin-2, a giant scaffolder at the nuclear envelope.

作者信息

Libotte Thorsten, Zaim Hafida, Abraham Sabu, Padmakumar V C, Schneider Maria, Lu Wenshu, Munck Martina, Hutchison Christopher, Wehnert Manfred, Fahrenkrog Birthe, Sauder Ursula, Aebi Ueli, Noegel Angelika A, Karakesisoglou Iakowos

机构信息

Center for Biochemistry, Medical Faculty, University of Cologne, 50931 Cologne, Germany.

出版信息

Mol Biol Cell. 2005 Jul;16(7):3411-24. doi: 10.1091/mbc.e04-11-1009. Epub 2005 Apr 20.

Abstract

The vertebrate proteins Nesprin-1 and Nesprin-2 (also referred to as Enaptin and NUANCE) together with ANC-1 of Caenorhabditis elegans and MSP-300 of Drosophila melanogaster belong to a novel family of alpha-actinin type actin-binding proteins residing at the nuclear membrane. Using biochemical techniques, we demonstrate that Nesprin-2 binds directly to emerin and the C-terminal common region of lamin A/C. Selective disruption of the lamin A/C network in COS7 cells, using a dominant negative lamin B mutant, resulted in the redistribution of Nesprin-2. Furthermore, using lamin A/C knockout fibroblasts we show that lamin A/C is necessary for the nuclear envelope localization of Nesprin-2. In normal skin where lamin A/C is differentially expressed, strong Nesprin-2 expression was found in all epidermal layers, including the basal layer where only lamin C is present. This indicates that lamin C is sufficient for proper Nesprin-2 localization at the nuclear envelope. Expression of dominant negative Nesprin-2 constructs and knockdown studies in COS7 cells revealed that the presence of Nesprin-2 at the nuclear envelope is necessary for the proper localization of emerin. Our data imply a scaffolding function of Nesprin-2 at the nuclear membrane and suggest a potential involvement of this multi-isomeric protein in human disease.

摘要

脊椎动物蛋白Nesprin-1和Nesprin-2(也称为Enaptin和NUANCE),连同秀丽隐杆线虫的ANC-1和黑腹果蝇的MSP-300,属于一类新的位于核膜的α-辅肌动蛋白型肌动蛋白结合蛋白家族。运用生化技术,我们证明Nesprin-2直接与emerin以及核纤层蛋白A/C的C端共同区域结合。使用显性负性核纤层蛋白B突变体选择性破坏COS7细胞中的核纤层蛋白A/C网络,导致Nesprin-2重新分布。此外,利用核纤层蛋白A/C基因敲除的成纤维细胞,我们发现核纤层蛋白A/C对于Nesprin-2在核膜的定位是必需的。在核纤层蛋白A/C差异表达的正常皮肤中,在所有表皮层均发现Nesprin-2强表达,包括仅存在核纤层蛋白C的基底层。这表明核纤层蛋白C足以使Nesprin-2在核膜正确定位。在COS7细胞中表达显性负性Nesprin-2构建体并进行敲低研究表明,Nesprin-2在核膜的存在对于emerin的正确定位是必需的。我们的数据表明Nesprin-2在核膜具有支架功能,并提示这种多异构体蛋白可能与人类疾病有关。

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