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α-1干扰素的抗病毒和抗增殖活性:半胱氨酸残基的作用

Antiviral and antiproliferative activities of interferon-alpha 1: the role of cysteine residues.

作者信息

Beilharz M W, Nisbet I T, Tymms M J, Hertzog P J, Linnane A W

出版信息

J Interferon Res. 1986 Dec;6(6):677-85. doi: 10.1089/jir.1986.6.677.

Abstract

Site-specific in vitro mutagenesis was used to direct serine for cysteine substitutions within the sequence of human interferon-alpha 1 (IFN-alpha 1). Antiviral specific activities and antiproliferative activities of IFN-alpha 1 analogs, expressed in M13 as fusion proteins, were assessed following purification by monoclonal antibody affinity chromatography. Based on analysis of IFN-alpha 2, IFN-alpha 1 contains two disulfide bridges between cysteine residues 29 and 139 and cysteine residues 1 and 99. IFN-alpha 1 also contains a fifth cysteine residue at position 86. The series of serine for cysteine substitutions performed indicated that IFN-alpha 1 molecules unable to form the residue 29 to residue 139 disulfide bridge have substantially reduced antiviral and antiproliferative activities, IFN-alpha 1 molecules unable to form the residue 1 to residue 99 disulfide bridge have only marginally altered antiviral and antiproliferative activities, the low antiviral activity of IFN-alpha 1 compared with other human IFN-alpha subtypes is not due to the formation of nonnative disulfide bridges involving the fifth cysteine residue at position 86, which the other subtypes lack, and (iv) the reduced biological activities of certain analogs may be due to the formation of nonnative disulfide bridges.

摘要

位点特异性体外诱变被用于在人α-1干扰素(IFN-α1)序列中指导丝氨酸向半胱氨酸的替换。通过单克隆抗体亲和层析纯化后,评估了以M13融合蛋白形式表达的IFN-α1类似物的抗病毒特异性活性和抗增殖活性。基于对IFN-α2的分析,IFN-α1在半胱氨酸残基29和139以及半胱氨酸残基1和99之间含有两个二硫键。IFN-α1在第86位还含有第五个半胱氨酸残基。进行的一系列丝氨酸向半胱氨酸的替换表明,无法形成29位至139位残基二硫键的IFN-α1分子的抗病毒和抗增殖活性大幅降低,无法形成1位至99位残基二硫键的IFN-α1分子的抗病毒和抗增殖活性仅有轻微改变,与其他人IFN-α亚型相比,IFN-α1的低抗病毒活性并非由于涉及第86位第五个半胱氨酸残基(其他亚型缺乏该残基)形成非天然二硫键,并且(iv)某些类似物的生物活性降低可能是由于形成了非天然二硫键。

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