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高相对分子质量 EBV 潜伏膜蛋白 1(LMP-1)复合物分析:对 LMP-1 同型寡聚化和脂筏结合的结构见解。

High molecular weight complex analysis of Epstein-Barr virus Latent Membrane Protein 1 (LMP-1): structural insights into LMP-1's homo-oligomerization and lipid raft association.

机构信息

Department of Molecular, Cellular and Developmental Biology, University of Colorado, Boulder, CO 80309, United States.

出版信息

Virus Res. 2013 Dec 26;178(2):314-27. doi: 10.1016/j.virusres.2013.09.025. Epub 2013 Sep 25.

Abstract

LMP-1 is a constitutively active Tumor Necrosis Factor Receptor analog encoded by Epstein-Barr virus. LMP-1 activation correlates with oligomerization and raft localization, but direct evidence of LMP-1 oligomers is limited. We report that LMP-1 forms multiple high molecular weight native LMP-1 complexes when analyzed by BN-PAGE, the largest of which are enriched in detergent resistant membranes. The largest of these high molecular weight complexes are not formed by purified LMP-1 or by loss of function LMP-1 mutants. Consistent with these results we find a dimeric form of LMP-1 that can be stabilized by disulfide crosslinking. We identify cysteine 238 in the C-terminus of LMP-1 as the crosslinked cysteine. Disulfide crosslinking occurs post-lysis but the dimer can be crosslinked in intact cells with membrane permeable crosslinkers. LMP-1/C238A retains wild type LMP-1 NF-κB activity. LMP-1's TRAF binding, raft association and oligomerization are associated with the dimeric form of LMP-1. Our results suggest the possibility that the observed dimeric species results from inter-oligomeric crosslinking of LMP-1 molecules in adjacent core LMP-1 oligomers.

摘要

LMP-1 是一种由 Epstein-Barr 病毒编码的组成性激活的肿瘤坏死因子受体类似物。LMP-1 的激活与寡聚化和筏定位相关,但 LMP-1 寡聚物的直接证据有限。我们报告说,当通过 BN-PAGE 分析时,LMP-1 形成多种高分子量天然 LMP-1 复合物,其中最大的复合物富含去污剂抗性膜。这些高分子量复合物中最大的复合物不是由纯化的 LMP-1 或丧失功能的 LMP-1 突变体形成的。与这些结果一致,我们发现 LMP-1 的二聚体形式可以通过二硫键交联稳定。我们确定 LMP-1 的 C 末端的半胱氨酸 238 是交联的半胱氨酸。二硫键交联发生在裂解后,但可以使用膜通透交联剂在完整细胞中交联二聚体。LMP-1/C238A 保留野生型 LMP-1 NF-κB 活性。LMP-1 的 TRAF 结合、筏关联和寡聚化与 LMP-1 的二聚体形式相关。我们的结果表明,观察到的二聚体物种可能是由于相邻核心 LMP-1 寡聚物中 LMP-1 分子的间寡聚交联所致。

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