Characterization of V3 Sequence Heterogeneity in Subtype C Human Immunodeficiency Virus Type 1 Isolates from Malawi: Underrepresentation of X4 Variants

Li-Hua Ping , Julie A. Nelson , Irving Hoffman , Li-Hua Ping , Julie A. Nelson , Irving Hoffman , Jody Schock , Suzanna L. Lamers , Melissa Goodman , Pietro Vernazza , Peter N. Kazembe , Martin Maida , Dick Zimba , Maureen M. Goodenow , Joseph J. Eron , Susan A. Fiscus , Myron S. Cohen , Ronald Swanstrom
1999 Journal of Virology 195 citations

Abstract

ABSTRACT We have examined the nature of V3 sequence variability among subtype C human immunodeficiency virus type 1 (HIV-1) sequences from plasma-derived viral RNA present in infected men from Malawi. Sequence variability was assessed by direct sequence analysis of the V3 reverse transcription-PCR products, examination of virus populations by a subtype C V3-specific heteroduplex tracking assay (V3-HTA), and selected sequence analysis of molecular clones derived from the PCR products. Sequence variability in V3 among the subtype C viruses was not associated with the presence of basic amino acid substitutions. This observation is in contrast to that for subtype B HIV-1, where sequence variability is associated with such substitutions, and these substitutions are determinants of altered coreceptor usage. Evolutionary variants in subtype C V3 sequences, as defined by the V3-HTA, were not correlated with the CD4 level in the infected person, while such a correlation was found with subtype B V3 sequences. Viruses were isolated from a subset of the subjects; all isolates used CCR5 and not CXCR4 as a coreceptor, and none was able to grow in MT-2 cells, a hallmark of the syncytium-inducing phenotype that is correlated with CXCR4 usage. The overall sequence variability of the subtype C V3 region was no greater than that of the conserved regions of gp120. This limited sequence variability was also a feature of subtype B V3 sequences that do not carry the basic amino acid substitutions associated with altered coreceptor usage. Our results indicate that altered coreceptor usage is rare in subtype C HIV-1 isolates in sub-Saharan Africa and that sequence variability is not a feature of the V3 region of env in the absence of altered coreceptor usage.

Keywords

BiologyPeptide sequenceV3 loopGeneticsSequence analysisVirologyHeteroduplexSequence (biology)Consensus sequenceReverse transcriptaseSequence alignmentVirusPhenotypeRNAGene

MeSH Terms

Base SequenceDNAViralEvolutionMolecularGenetic HeterogeneityGenetic VariationHIV Envelope Protein gp120HIV SeropositivityHIV-1HumansMalawiMolecular Sequence DataNucleic Acid HeteroduplexesPeptide FragmentsRNAViralReceptorsCCR5ReceptorsCXCR4

Affiliated Institutions

Related Publications

Publication Info

Year
1999
Type
article
Volume
73
Issue
8
Pages
6271-6281
Citations
195
Access
Closed

External Links

Download PDF (Free) View on DOI.org PubMed Semantic Scholar

Social Impact

Altmetric
PlumX Metrics

Social media, news, blog, policy document mentions

Citation Metrics

195
OpenAlex
9
Influential

Cite This

Li-Hua Ping, Julie A. Nelson, Irving Hoffman et al. (1999). Characterization of V3 Sequence Heterogeneity in Subtype C Human Immunodeficiency Virus Type 1 Isolates from Malawi: Underrepresentation of X4 Variants. Journal of Virology , 73 (8) , 6271-6281. https://doi.org/10.1128/jvi.73.8.6271-6281.1999

Identifiers

DOI
10.1128/jvi.73.8.6271-6281.1999
PMID
10400718
PMCID
PMC112705

Data Quality

Data completeness: 86%