Elevated HIV Viral Load is Associated with Higher Recombination Rate In Vivo.

Mol Biol Evol

Department of Genome Sciences, University of Washington, Seattle, WA, USA.

Published: January 2024

AI Article Synopsis

  • HIV's high recombination rate leads to diversity within hosts, helping the virus evade the immune system and develop drug resistance.
  • The study aims to understand how recombination rates differ based on viral load and cellular coinfection during HIV infection.
  • Using a new method called RATS-LD, the researchers found that recombination rates are significantly higher in individuals with higher viral loads, suggesting that recombination is not a static process but varies greatly over time and among individuals.

Article Abstract

HIV's exceptionally high recombination rate drives its intrahost diversification, enabling immune escape and multidrug resistance within people living with HIV. While we know that HIV's recombination rate varies by genomic position, we have little understanding of how recombination varies throughout infection or between individuals as a function of the rate of cellular coinfection. We hypothesize that denser intrahost populations may have higher rates of coinfection and therefore recombination. To test this hypothesis, we develop a new approach (recombination analysis via time series linkage decay or RATS-LD) to quantify recombination using autocorrelation of linkage between mutations across time points. We validate RATS-LD on simulated data under short read sequencing conditions and then apply it to longitudinal, high-throughput intrahost viral sequencing data, stratifying populations by viral load (a proxy for density). Among sampled viral populations with the lowest viral loads (<26,800 copies/mL), we estimate a recombination rate of 1.5×10-5 events/bp/generation (95% CI: 7×10-6 to 2.9×10-5), similar to existing estimates. However, among samples with the highest viral loads (>82,000 copies/mL), our median estimate is approximately 6 times higher. In addition to co-varying across individuals, we also find that recombination rate and viral load are associated within single individuals across different time points. Our findings suggest that rather than acting as a constant, uniform force, recombination can vary dynamically and drastically across intrahost viral populations and within them over time. More broadly, we hypothesize that this phenomenon may affect other facultatively asexual populations where spatial co-localization varies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10777272PMC
http://dx.doi.org/10.1093/molbev/msad260DOI Listing

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