Analysis of sequence diversity in hypervariable regions of the external glycoprotein of human immunodeficiency virus type 1.

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J Virol. 1990 December; 64(12): 5840-5850

Analysis of sequence diversity in hypervariable regions of the external glycoprotein of human immunodeficiency virus type 1.

P Simmonds, P Balfe, C A Ludlam, J O Bishop and A J Brown

Department of Genetics, University of Edinburgh, Scotland.

ABSTRACT

Nucleotide sequences in three hypervariable regions of the humanimmunodeficiency virus type 1 (HIV-1) env gene were obtainedby sequencing provirus present in peripheral blood mononuclearcells of HIV-infected individuals. Single molecules of targetsequences were isolated by limiting dilution and amplified intwo stages by the polymerase chain reaction, using nested primers.The product was directly sequenced to avoid errors introducedby Taq polymerase during the amplification process. There wasextensive variation between sequences from the same individualas well as between sequences from different individuals. Interpatientvariability was markedly less in individuals infected from acommon source. A high proportion of amino acid substitutionsin the hypervariable regions altered the number and positionsof potential N-linked glycosylation sites. Sequences in twohypervariable regions frequently contained short (3- to 15-bp)duplications or deletions, and by amplifying peripheral bloodmononuclear cell DNA containing 10(2) or 10(3) proviral moleculesand analyzing the product by high-resolution electrophoresis,the total number and abundance of distinct length variants withinan individual could be estimated, providing a more comprehensiveanalysis of the variants present than would be obtained by sequencingalone. Sequences from many individuals showed frequent aminoacid substitutions at certain key positions for neutralizing-antibodyand cytotoxic T-cell recognition in the immunodominant loop.The rates of synonymous and nonsynonymous nucleotide substitutionin the region of this and flanking regions indicate that strongpositive selection for amino acid change is operating in thegeneration of antigenic diversity.

J Virol. 1990 December; 64(12): 5840-5850

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