Extensive Diversification of Human Immunodeficiency Virus Type 1 Subtype B Strains during Dual Infection of a Chimpanzee That Progressed to AIDS

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J Virol, April 1998, p. 3005-3017, Vol. 72, No. 4
0022-538X/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Extensive Diversification of Human Immunodeficiency Virus Type 1 Subtype B Strains during Dual Infection of a Chimpanzee That Progressed to AIDS

Qing Wei and Patricia N. Fultz^*

Department of Microbiology, University of Alabama School of Medicine, Birmingham, Alabama 35294

Received 22 August 1997/Accepted 24 December 1997

A chimpanzee (C-499) infected for more than 9 years with two subtype B isolates of human immunodeficiency virus type 1 (HIV-1),one (HIV-1_SF2) that replicates poorly and one (HIV-1_LAV-1b) thatreplicates efficiently in chimpanzees, died of AIDS 11 years afterinitial infection (F. J. Novembre et al., J. Virol. 71:4086-4091,1997). Nucleotide sequence and phylogenetic analyses of the C2to V5 region of env (C2-V5^env) in proviral DNA from peripheral blood lymphocytes obtained 22months before death revealed two distinct virus populations. Oneof these populations appeared to be a recombinant in env, havingthe V3 loop from HIV-1_SF2 and the V4-V5 region from HIV-1_LAV-1b;the other population had evolved from HIV-1_LAV-1b. In additionto C2-V5^env, the entire p17^gag and nef genes were sequenced; however, based on nucleotide sequencesand phlyogeny, whether the progenitor of the p17^gag and nef genes was SF2 or LAV-1b could not be determined. Comparedto the two original viruses, the divergence of all clones of C2-V5^env ranged from 9.37 to 20.2%, that of p17^gag ranged from 3.11 to 9.29%, and that of nef ranged from 4.02 to7.9%. In contrast, compared to the maximum variation of 20.2%in C2-V5^env for C-499, the maximum diversities in C2-V5^env in proviruses from two chimpanzees infected with HIV-1_LAV-1bfor 9 and 10 years were 9.65 and 2.48%, respectively. These resultsdemonstrate that (i) two distinct HIV-1 populations can coexistand undergo extensive diversification in chimpanzees with progressiveHIV-1-induced disease and (ii) recombination between two subtypeB strains occurred even though the second strain was inoculated15 months after the first one. Furthermore, evaluation of envgenes from three chimpanzees infected with the same strain suggeststhat the magnitude of HIV-1 diversification could be related tohigher viral burdens, manifestations of disease, and/or dual infection.

^* Corresponding author. Mailing address: Department of Microbiology, University of Alabama School of Medicine, 845 19th St.South, BBRB 511, Birmingham, AL 35294. Phone: (205) 934-0790.Fax: (205) 975-6788.

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