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Literature DB >> 25965315

A broad range of mutations in HIV-1 neutralizing human monoclonal antibodies specific for V2, V3, and the CD4 binding site.

Liuzhe Li¹, Xiao-Hong Wang², Constance Williams¹, Barbara Volsky¹, Olivia Steczko¹, Michael S Seaman³, Kalpana Luthra⁴, Phillipe Nyambi¹, Arthur Nadas⁵, Véronique Giudicelli⁶, Marie-Paule Lefranc⁶, Susan Zolla-Pazner⁷, Miroslaw K Gorny⁸.

Abstract

The HIV vaccine-induced neutralizing antibodies (Abs) display low rates of mutation in their variable regions. To determine the range of neutralization mediated by similar human monoclonal Abs (mAbs) but derived from unselected chronically HIV-1 infected subjects, we tested a panel of 66 mAbs specific to V3, CD4 binding site (CD4bs) and V2 regions. The mAbs were tested against 41 pseudoviruses, including 15 tier 1 and 26 tier 2, 3 viruses, showing that the neutralization potency and breadth of anti-V3 mAbs were significantly higher than those of the anti-CD4bs and anti-V2 mAbs, and only anti-V3 mAbs were able to neutralize some tier 2, 3 viruses. The percentage of mutations in the variable regions of the heavy (VH) and light (VL) chains varied broadly in a range from 2% to 18% and correlated moderately with the neutralization breadth of tier 2, 3 viruses. There was no correlation with neutralization of tier 1 viruses as some mAbs with low and high percentages of mutations neutralized the same number of viruses. The electrostatic interactions between anti-V3 mAbs and the charged V3 region may contribute to their neutralization because the isoelectric points of the VH CDR3 of 48 anti-V3 mAbs were inversely correlated with the neutralization breadth of tier 2, 3 viruses. The results demonstrate that infection-induced antibodies to CD4bs, V3 and V2 regions can mediate cross-clade neutralization despite low levels of mutations which can be achieved by HIV-1 vaccine-induced antibodies.

Entities: CellLine Chemical Disease Gene Species

Keywords: CD4 binding site; HIV neutralizing antibodies; HIV-1; Human monoclonal antibodies; Somatic mutation; V2 region; V3 region

Mesh：

Substances：

Year: 2015 PMID： 25965315 PMCID： PMC4461508 DOI： 10.1016/j.molimm.2015.04.011

Source DB: PubMed Journal: Mol Immunol ISSN： 0161-5890 Impact factor: 4.407

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