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内质网降解增强蛋白 2(EDEM2)在蓖麻毒素从内质网到细胞质运输中的作用与内质网降解增强蛋白 1(EDEM1)相比。

The role of EDEM2 compared with EDEM1 in ricin transport from the endoplasmic reticulum to the cytosol.

机构信息

*Department of Molecular Biology, University of Gdańsk, 80-308 Gdańsk, Poland.

出版信息

Biochem J. 2014 Feb 1;457(3):485-96. doi: 10.1042/BJ20130155.

Abstract

EDEM1 [ER (endoplasmic reticulum)-degradation-enhancing α-mannosidase I-like protein 1] and EDEM2 are crucial regulators of ERAD (ER-associated degradation) that extracts non-native glycoproteins from the calnexin chaperone system. Ricin is a potent plant cytotoxin composed of an A-chain (RTA) connected by a disulfide bond to a cell-binding lectin B-chain (RTB). After endocytic uptake, the toxin is transported retrogradely to the ER, where the enzymatically active RTA is translocated to the cytosol in a similar manner as misfolded ER proteins. This transport is promoted by EDEM1. In the present study we report that EDEM2 is also involved in ricin retrotranslocation out of the ER. However, the role of EDEM1 and EDEM2 in ricin transport to the cytosol seems to differ. EDEM2 promotes ricin retrotranslocation irrespectively of ER translocon accessibility; moreover, co-immunoprecipitation and pull-down studies revealed that more ricin can interact with EDEM2 in comparison with EDEM1. On the other hand, interactions of both lectins with RTA are dependent on the structure of the RTA. Thus our data display a newly discovered role for EDEM2. Moreover, analysis of the involvement of EDEM1 and EDEM2 in ricin retrotranslocation to the cytosol may provide crucial information about general mechanisms of the recognition of ERAD substrates in the ER.

摘要

EDEM1(内质网降解增强的α-甘露糖苷酶 I 样蛋白 1)和 EDEM2 是内质网相关降解(ERAD)的关键调节因子,可从钙连蛋白伴侣系统中提取非天然糖蛋白。蓖麻毒素是一种由 A 链(RTA)通过二硫键连接到细胞结合凝集素 B 链(RTB)组成的有效植物细胞毒素。在细胞内摄取后,毒素被逆行转运到内质网,其中酶活性的 RTA 以类似于错误折叠的 ER 蛋白的方式易位到细胞质中。这种转运由 EDEM1 促进。在本研究中,我们报告 EDEM2 也参与了蓖麻毒素从内质网的逆行易位。然而,EDEM1 和 EDEM2 在蓖麻毒素向细胞质转运中的作用似乎不同。EDEM2 促进蓖麻毒素逆行易位,而与内质网易位体的可及性无关;此外,免疫共沉淀和下拉研究表明,与 EDEM1 相比,更多的蓖麻毒素可以与 EDEM2 相互作用。另一方面,两种凝集素与 RTA 的相互作用都依赖于 RTA 的结构。因此,我们的数据显示了 EDEM2 的一个新发现的作用。此外,分析 EDEM1 和 EDEM2 在内质网中蓖麻毒素逆行易位到细胞质中的参与可能为 ERAD 底物在 ER 中的识别的一般机制提供关键信息。

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