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对单克隆抗体中和作用具有抗性的人呼吸道合胞病毒G糖蛋白中的提前终止密码子。

Premature stop codons in the G glycoprotein of human respiratory syncytial viruses resistant to neutralization by monoclonal antibodies.

作者信息

Rueda P, Delgado T, Portela A, Melero J A, García-Barreno B

机构信息

Servicio de Biología Molecular, Centro Nacional de Microbiología, Madrid, Spain.

出版信息

J Virol. 1991 Jun;65(6):3374-8. doi: 10.1128/JVI.65.6.3374-3378.1991.

Abstract

Mutants of human respiratory syncytial (RS) virus which escaped neutralization by monoclonal antibodies directed against the G glycoprotein were selected from the Long strain. Most mutants showed drastic antigenic changes, reflected in the lack of reactivity with several anti-G antibodies, including the one used for selection. Sequence analysis revealed the presence of in-frame premature stop codons in the mutated G genes which shortened the G polypeptide by between 11 and 42 amino acids. In contrast, two mutants selected with monoclonal antibody 25G contained two amino acid substitutions (Phe-265----Leu and Leu-274----Pro) and had lost only the capacity to bind the antibody used in their selection. These results demonstrate that the carboxy-terminal end of the G molecule is dispensable for infectivity in tissue culture and indicate the importance of this part of the G protein in determining its antigenicity.

摘要

从长株中筛选出逃避针对G糖蛋白的单克隆抗体中和作用的人呼吸道合胞(RS)病毒突变体。大多数突变体表现出剧烈的抗原变化,这体现在与几种抗G抗体(包括用于筛选的抗体)缺乏反应性上。序列分析显示,突变的G基因中存在框内过早终止密码子,使G多肽缩短了11至42个氨基酸。相比之下,用单克隆抗体25G筛选出的两个突变体含有两个氨基酸取代(Phe-265→Leu和Leu-274→Pro),并且仅丧失了结合用于筛选的抗体的能力。这些结果表明,G分子的羧基末端对于组织培养中的感染性是可有可无的,并表明G蛋白的这一部分在决定其抗原性方面的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1662/241000/18714c0b343a/jvirol00049-0626-a.jpg

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