Naeve C W, Williams D
Department of Virology and Molecular Biology, St Jude Children's Research Hospital, Memphis, TN 38101.
EMBO J. 1990 Dec;9(12):3857-66. doi: 10.1002/j.1460-2075.1990.tb07604.x.
The covalent attachment of fatty acid moieties to proteins is a widespread post-translational modification of viral and cell proteins yet the functional consequences of acylation are not well understood. We have determined that the A/Japan/305/57 influenza virus hemagglutinin (HA) contains three potential acylation sites at cysteine residues 211, 218 and 221 in the cytoplasmic domain of the molecule. Site-directed mutagenesis of one or more of these sites has no effect on biosynthesis, transport or receptor binding activity of the molecule; however, modification of any single site is sufficient to abolish completely or inhibit severely membrane fusion activity, a function essential for virus infectivity. We present a molecular model of the transmembrane and cytoplasmic domains of the HA to illustrate the potential orientation of these fatty acids and to provide a conceptual framework for further experimentation.
脂肪酸部分与蛋白质的共价连接是病毒和细胞蛋白质广泛存在的一种翻译后修饰,但酰化作用的功能后果尚未得到充分理解。我们已经确定,A/日本/305/57流感病毒血凝素(HA)在该分子胞质结构域的半胱氨酸残基211、218和221处含有三个潜在的酰化位点。对这些位点中的一个或多个进行定点诱变对该分子的生物合成、转运或受体结合活性没有影响;然而,对任何单个位点的修饰都足以完全消除或严重抑制膜融合活性,而膜融合活性是病毒感染性所必需的功能。我们提出了HA跨膜和胞质结构域的分子模型,以说明这些脂肪酸的潜在取向,并为进一步的实验提供一个概念框架。
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