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人冠状病毒 NL63 的开放阅读框 3 编码一个病毒粒子整合的 N-糖基化膜蛋白。

Human coronavirus NL63 open reading frame 3 encodes a virion-incorporated N-glycosylated membrane protein.

机构信息

University of Bonn Medical Centre, Bonn, Germany.

出版信息

Virol J. 2010 Jan 15;7:6. doi: 10.1186/1743-422X-7-6.

Abstract

BACKGROUND

Human pathogenic coronavirus NL63 (hCoV-NL63) is a group 1 (alpha) coronavirus commonly associated with respiratory tract infections. In addition to known non-structural and structural proteins all coronaviruses have one or more accessory proteins whose functions are mostly unknown. Our study focuses on hCoV-NL63 open reading frame 3 (ORF 3) which is a highly conserved accessory protein among coronaviruses.

RESULTS

In-silico analysis of the 225 amino acid sequence of hCoV-NL63 ORF 3 predicted a triple membrane-spanning protein. Expression in infected CaCo-2 and LLC-MK2 cells was confirmed by immunofluorescence and Western blot analysis. The protein was detected within the endoplasmatic reticulum/Golgi intermediate compartment (ERGIC) where coronavirus assembly and budding takes place. Subcellular localization studies using recombinant ORF 3 protein transfected in Huh-7 cells revealed occurrence in ERGIC, Golgi- and lysosomal compartments. By fluorescence microscopy of differently tagged envelope (E), membrane (M) and nucleocapsid (N) proteins it was shown that ORF 3 protein colocalizes extensively with E and M within the ERGIC. Using N-terminally FLAG-tagged ORF 3 protein and an antiserum specific to the C-terminus we verified the proposed topology of an extracellular N-terminus and a cytosolic C-terminus. By in-vitro translation analysis and subsequent endoglycosidase H digestion we showed that ORF 3 protein is N-glycosylated at the N-terminus. Analysis of purified viral particles revealed that ORF 3 protein is incorporated into virions and is therefore an additional structural protein.

CONCLUSIONS

This study is the first extensive expression analysis of a group 1 hCoV-ORF 3 protein. We give evidence that ORF 3 protein is a structural N-glycosylated and virion-incorporated protein.

摘要

背景

人致病性冠状病毒 NL63(hCoV-NL63)是一种常见的呼吸道感染相关的组 1(α)冠状病毒。除了已知的非结构和结构蛋白外,所有冠状病毒都有一个或多个辅助蛋白,其功能大多未知。我们的研究集中在 hCoV-NL63 开放阅读框 3(ORF3)上,这是冠状病毒中高度保守的辅助蛋白。

结果

hCoV-NL63 ORF3 的 225 个氨基酸序列的计算机分析预测了一种三跨膜蛋白。通过感染 CaCo-2 和 LLC-MK2 细胞的免疫荧光和 Western blot 分析证实了表达。该蛋白在冠状病毒组装和出芽发生的内质网/高尔基体中间区室(ERGIC)中被检测到。在 Huh-7 细胞中转染重组 ORF3 蛋白的亚细胞定位研究表明,该蛋白存在于 ERGIC、高尔基体和溶酶体区室中。通过不同标记的包膜(E)、膜(M)和核衣壳(N)蛋白的荧光显微镜观察,显示 ORF3 蛋白与 ERGIC 中的 E 和 M 广泛共定位。使用 N 端 FLAG 标记的 ORF3 蛋白和针对 C 端的抗血清,我们验证了细胞外 N 端和细胞质 C 端的提议拓扑结构。通过体外翻译分析和随后的内切糖苷酶 H 消化,我们表明 ORF3 蛋白在 N 端发生 N 糖基化。对纯化的病毒颗粒的分析表明,ORF3 蛋白被整合到病毒粒子中,因此是一种额外的结构蛋白。

结论

本研究是对组 1 hCoV-ORF3 蛋白的首次广泛表达分析。我们证明了 ORF3 蛋白是一种结构上的 N-糖基化和病毒粒子整合蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfab/2819038/8ac9e03794c3/1743-422X-7-6-1.jpg

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