Frontiers in Immunology (Feb 2024)

B cell repertoire sequencing of HIV-1 pediatric elite-neutralizers identifies multiple broadly neutralizing antibody clonotypes

  • Sanjeev Kumar,
  • Sanjeev Kumar,
  • Sanjeev Kumar,
  • Sanjeev Kumar,
  • Sanjeev Kumar,
  • Prashant Bajpai,
  • Collin Joyce,
  • Collin Joyce,
  • Collin Joyce,
  • Collin Joyce,
  • Sushil Kumar Kabra,
  • Rakesh Lodha,
  • Dennis R. Burton,
  • Dennis R. Burton,
  • Dennis R. Burton,
  • Dennis R. Burton,
  • Bryan Briney,
  • Bryan Briney,
  • Bryan Briney,
  • Bryan Briney,
  • Kalpana Luthra

DOI
https://doi.org/10.3389/fimmu.2024.1272493
Journal volume & issue
Vol. 15

Abstract

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IntroductionA limited subset of HIV-1 infected adult individuals typically after at least 2-3 years of chronic infection, develop broadly neutralizing antibodies (bnAbs), suggesting that highly conserved neutralizing epitopes on the HIV-1 envelope glycoprotein are difficult for B cell receptors to effectively target, during natural infection. Recent studies have shown the evolution of bnAbs in HIV-1 infected infants.MethodsWe used bulk BCR sequencing (BCR-seq) to profile the B cell receptors from longitudinal samples (3 time points) collected from a rare pair of antiretroviralnaïve, HIV-1 infected pediatric monozygotic twins (AIIMS_329 and AIIMS_330) who displayed elite plasma neutralizing activity against HIV-1.ResultsBCR-seq of both twins revealed convergent antibody characteristics including V-gene use, CDRH3 lengths and somatic hypermutation (SHM). Further, antibody clonotypes with genetic features similar to highly potent bnAbs isolated from adults showed ongoing development in donor AIIMS_330 but not in AIIMS_329, corroborating our earlier findings based on plasma bnAbs responses. An increase in SHM was observed in sequences of the IgA isotype from AIIMS_330.DiscussionThis study suggests that children living with chronic HIV-1 can develop clonotypes of HIV-1 bnAbs against multiple envelope epitopes similar to those isolated from adults, highlighting that such B cells could be steered to elicit bnAbs responses through vaccines aimed to induce bnAbs against HIV-1 in a broad range of people including children.

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