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裂谷热病毒M片段:利用重组痘苗病毒研究白蛉病毒基因表达

Rift Valley fever virus M segment: use of recombinant vaccinia viruses to study Phlebovirus gene expression.

作者信息

Kakach L T, Wasmoen T L, Collett M S

机构信息

Molecular Genetics, Inc., Minnetonka, Minnesota 55343.

出版信息

J Virol. 1988 Mar;62(3):826-33. doi: 10.1128/JVI.62.3.826-833.1988.

Abstract

Recombinant vaccinia viruses were constructed and used in conjunction with site-specific antisera to study the coding capacity and detailed expression strategy of the M segment of the Phlebovirus Rift Valley fever virus (RVFV). The M segment could be completely and faithfully expressed in recombinant RVFV-vaccinia virus-infected cells, the gene products apparently being correctly processed and modified in the absence of the RVFV L and S genomic segments. The proteins encoded by the RVFV M segment included, in addition to the viral glycoproteins G2 and G1, two previously uncharacterized polypeptides of 78 and 14 kilodaltons (kDa). By manipulation of RVFV sequences present in the recombinant vaccinia viruses and use of specific antibody reagents, it was found that the 78-kDa protein initiated at the first initiation codon of the open reading frame and encompassed the entire preglycoprotein and glycoprotein G2 coding sequences. The 14-kDa protein appeared to begin from the second in-phase ATG and was composed of only the preglycoprotein sequences. Both viral glycoproteins G2 and G1 could be synthesized and correctly processed in the absence of the 78- and 14-kDa proteins, as well as a large portion of the preglycoprotein sequences. However, the hydrophobic amino acid sequence immediately preceding the mature glycoprotein coding sequences was required for authentic glycoprotein production. The M-segment expression strategy involving aspects of translational initiation and protein processing are discussed. The functional roles of the 78- and 14-kDa proteins remain unclear.

摘要

构建了重组痘苗病毒,并将其与位点特异性抗血清结合使用,以研究裂谷热病毒(RVFV)的M节段的编码能力和详细表达策略。M节段可以在重组RVFV-痘苗病毒感染的细胞中完全且忠实地表达,在没有RVFV L和S基因组节段的情况下,基因产物显然能够被正确加工和修饰。RVFV M节段编码的蛋白质除了病毒糖蛋白G2和G1外,还包括两种以前未被鉴定的分子量分别为78千道尔顿(kDa)和14 kDa的多肽。通过对重组痘苗病毒中存在的RVFV序列进行操作并使用特异性抗体试剂,发现78-kDa蛋白从开放阅读框的第一个起始密码子开始,包含整个前体糖蛋白和糖蛋白G2的编码序列。14-kDa蛋白似乎从第二个同相位的ATG开始,仅由前体糖蛋白序列组成。在没有78-kDa和14-kDa蛋白以及大部分前体糖蛋白序列的情况下,病毒糖蛋白G2和G1都可以合成并正确加工。然而,成熟糖蛋白编码序列之前紧邻的疏水氨基酸序列是产生真正糖蛋白所必需的。讨论了涉及翻译起始和蛋白质加工方面的M节段表达策略。78-kDa和14-kDa蛋白的功能作用仍不清楚。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/16ab/253638/1302979e4af5/jvirol00082-0175-a.jpg

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