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瘟病毒糖蛋白Erns通过一个两亲性螺旋以平面方式锚定在膜中。

The pestivirus glycoprotein Erns is anchored in plane in the membrane via an amphipathic helix.

作者信息

Tews Birke Andrea, Meyers Gregor

机构信息

Institut für Immunologie, Friedrich-Loeffler-Institut, Tübingen.

出版信息

J Biol Chem. 2007 Nov 9;282(45):32730-41. doi: 10.1074/jbc.M706803200. Epub 2007 Sep 11.

Abstract

E(rns) is a structural glycoprotein of pestiviruses found to be attached to the virion and to membranes within infected cells via its COOH terminus, although it lacks a hydrophobic anchor sequence. The COOH-terminal sequence was hypothesized to fold into an amphipathic alpha-helix. Alanine insertion scanning revealed that the ability of the E(rns) COOH terminus to bind membranes is considerably reduced by the insertion of a single amino acid at a wide variety of positions. Mutations decreasing the hydrophobicity of the apolar face of the putative helix led to reduction of membrane association. Proteinase K protection assays showed that E(rns) translated in vitro in the presence of microsomal membranes was protected, whereas a mutant with an artificial transmembrane region and a short cytosolic tag was shortened by the protease treatment. A tag fused to the COOH terminus of wild type E(rns) was not accessible for antibodies within digitonin-permeabilized cells, but the variant with the tag located downstream of the artificial transmembrane region was detected under the same conditions. These results are in accordance with the model that the COOH-terminal membrane anchor of E(rns) represents an amphipathic helix embedded in plane into the membrane. The integrity of the membrane anchor was found to be important for recovery of infectious virus.

摘要

E(rns)是瘟病毒的一种结构糖蛋白,尽管它缺乏疏水锚定序列,但通过其COOH末端与病毒粒子及感染细胞内的膜相连。推测COOH末端序列可折叠成两亲性α螺旋。丙氨酸插入扫描显示,在多种位置插入单个氨基酸会大大降低E(rns) COOH末端结合膜的能力。降低假定螺旋非极性面疏水性的突变会导致膜结合减少。蛋白酶K保护试验表明,在微粒体膜存在的情况下体外翻译的E(rns)受到保护,而具有人工跨膜区和短胞质标签的突变体则被蛋白酶处理缩短。与野生型E(rns) COOH末端融合的标签在洋地黄皂苷通透的细胞内无法被抗体识别,但在相同条件下可检测到标签位于人工跨膜区下游的变体。这些结果与E(rns)的COOH末端膜锚定代表嵌入膜平面的两亲性螺旋的模型一致。发现膜锚定的完整性对感染性病毒的恢复很重要。

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