4.7 Article

Broadly neutralizing antibodies with few somatic mutations and hepatitis C virus clearance

Journal

JCI INSIGHT
Volume 2, Issue 9, Pages -

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/jci.insight.92872

Keywords

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Funding

  1. US NIH [K08 AI102761, U19 AI088791, 1P30AI094189, HHSN272200900055C, HHSN272201400058C]
  2. National Center for Research Resources [UL1 RR024975]
  3. National Center for Advancing Translational Sciences [2 UL1 TR000445]
  4. NIH [P30 CA68485, DK058404, P01 AI45008]
  5. University of Pennsylvania Center

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Here, we report the isolation of broadly neutralizing mAbs (bNAbs) from persons with broadly neutralizing serum who spontaneously cleared hepatitis C virus (HCV) infection. We found that bNAbs from two donors bound the same epitope and were encoded by the same germline heavy chain variable gene segment. Remarkably, these bNAbs were encoded by antibody variable genes with sparse somatic mutations. For one of the most potent bNAbs, these somatic mutations were critical for antibody neutralizing breadth and for binding to autologous envelope variants circulating late in infection. However, somatic mutations were not necessary for binding of the bNAb unmutated ancestor to envelope proteins of early autologous transmitted/ founder viruses. This study identifies a public B cell clonotype favoring early recognition of a conserved HCV epitope, proving that anti-HCV bNAbs can achieve substantial neutralizing breadth with relatively few somatic mutations, and identifies HCV envelope variants that favored selection and maturation of an anti-HCV bNAb in vivo. These data provide insight into the molecular mechanisms of immune-mediated clearance of HCV infection and present a roadmap to guide development of a vaccine capable of stimulating anti-HCV bNAbs with a physiologic number of somatic mutations characteristic of vaccine responses.

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