Effect of amino acid replacements, additions and deletions on the antiviral activity of a peptide derived from the HIV-1 GP41 sequence.

Peptide research Pub Date : 1995-11-01
S Jiang, K Lin
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引用次数: 0

Abstract

We demonstrated that a synthetic peptide (EWDREINNYTSLIHSLIEESQNQQEKNEQEGGC), designated SJ-2176, corresponding to the HIV-1 IIIB gp41 sequence (637-666), inhibited HIV-1 replication, virus-induced cell-cell fusion and cytopathic effects in both CD4+ T and monocytic cell lines. In this study, we show that lengthening the peptide at either the N- or C-terminus enhanced its activity, while shortening the peptide from either end decreased the antiviral activity. Substitution of conserved residues in SJ-2176 by alanines resulted in a decrease or elimination of antiviral activity. Replacement of arginine and lysine in the peptide by glutamines did not diminish antiviral activity and rendered the peptide resistant to trypsin.

氨基酸替换、添加和删除对HIV-1 GP41序列衍生肽抗病毒活性的影响
我们证明了一个合成肽(EWDREINNYTSLIHSLIEESQNQQEKNEQEGGC),编号SJ-2176,对应于HIV-1 IIIB gp41序列(637-666),在CD4+ T和单核细胞系中抑制HIV-1复制、病毒诱导的细胞-细胞融合和细胞病变效应。在这项研究中,我们发现在N端或c端延长肽增强了其活性,而在任何一端缩短肽则降低了抗病毒活性。SJ-2176的保守残基被丙氨酸取代导致抗病毒活性降低或消除。用谷氨酰胺替代肽中的精氨酸和赖氨酸不会降低抗病毒活性,并使肽对胰蛋白酶具有抗性。
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