AI Article Synopsis

  • The HIV envelope glycoprotein (Env) is crucial for viral binding and immune responses but is difficult to target due to its complex structure and variability.
  • Flow virometry (FV) allows researchers to study HIV virions at the single-particle level using a range of monoclonal antibodies, demonstrating its effectiveness in characterizing Env.
  • The study highlights that both the production method of the virus and the addition of soluble CD4 can significantly influence the detection and conformation of Env on HIV virions.

Article Abstract

The HIV envelope glycoprotein (Env) is a trimeric protein that facilitates viral binding and fusion with target cells. As the sole viral protein on the HIV surface, Env is important both for immune responses to HIV and in vaccine designs. Targeting Env in clinical applications is challenging due to its heavy glycosylation, high genetic variability, conformational camouflage, and its low abundance on virions. Thus, there is a critical need to better understand this protein. Flow virometry (FV) is a useful methodology for phenotyping the virion surface in a high-throughput, single virion manner. To demonstrate the utility of FV to characterize Env, we stained HIV virions with a panel of 85 monoclonal antibodies targeting different regions of Env. A broad range of antibodies yielded robust staining of Env, with V3 antibodies showing the highest quantitative staining. A subset of antibodies tested in parallel on viruses produced in CD4 T cell lines, HEK293T cells, and primary cells showed that the cellular model of virus production can impact Env detection. Finally, in addition to being able to highlight Env heterogeneity on virions, we show FV can sensitively detect differences in Env conformation when soluble CD4 is added to virions before staining.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11209363PMC
http://dx.doi.org/10.3390/v16060935DOI Listing

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