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Multiple V1/V2 env variants are frequently present during primary infection with human immunodeficiency virus type 1. | LitMetric

AI Article Synopsis

  • HIV-1 exists as a diverse population of viral variants, particularly noticeable in chronically infected individuals, but during acute HIV-1 infections, there can be multiple viral variants circulating despite the low probability of infection.
  • A study analyzing blood plasma samples from 26 individuals with acute HIV-1 infection found that half had multiple V1/V2 viral variants, contradicting the assumption that only a few variants are transmitted during initial infection.
  • The research also indicated that while various viral variants are present during acute infection, they show rapid penetration into different bodily compartments (like seminal plasma and cerebrospinal fluid), suggesting factors like transient hyperinfectiousness or the inefficiency of infecting cells might influence both the transmission probability and the variety

Article Abstract

Human immunodeficiency virus type 1 (HIV-1) exists as a complex population of multiple genotypic variants in persons with chronic infection. However, acute HIV-1 infection via sexual transmission is a low-probability event in which there is thought to be low genetic complexity in the initial inoculum. In order to assess the viral complexity present during primary HIV-1 infection, the V1/V2 and V3 variable regions of the env gene were examined by using a heteroduplex tracking assay (HTA) capable of resolving these genotypic variants. Blood plasma samples from 26 primary HIV-1-infected subjects were analyzed for their level of diversity. Half of the subjects had more than one V1/V2 viral variant during primary infection, indicating the frequent transmission of multiple variants. This observation is inconsistent with the idea of infrequent transmission based on a small transmitting inoculum of cell-free virus. In chronically infected subjects, the complexity of the viral populations was even greater in both the V1/V2 and the V3 regions than in acutely infected subjects, indicating that in spite of the presence of multiple variants in acute infection, the virus does pass through a genetic bottleneck during transmission. We also examined how well the infecting virus penetrated different anatomical compartments by using the HTA. Viral variants detected in blood plasma were compared to those detected in seminal plasma and/or cerebral spinal fluid of six individuals. The virus in each of these compartments was to a large extent identical to virus in blood plasma, a finding consistent with rapid penetration of the infecting variant(s). The low-probability transmission of multiple variants could be the result of transient periods of hyperinfectiousness or hypersusceptibility. Alternatively, the inefficient transfer of a multiply infected cell could account for both the low probability of transmission and the transfer of multiple variants.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC521858PMC
http://dx.doi.org/10.1128/JVI.78.20.11208-11218.2004DOI Listing

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