Abstract

A large number of potent broadly neutralizing antibodies (bnAbs) against HIV-1 have been reported in recent years, raising hope for the possibility of an effective vaccine based on epitopes recognized by these protective antibodies. However, many of these bnAbs contain the long heavy chain complementarity-determining region 3 (HCDR3), which is viewed as an obstacle to the development of an HIV-1 vaccine targeting the bnAb responses. This mini-review summarizes the current literature and discusses the different potential immunologic mechanisms for generating long HCDR3, including D–D fusion, VH replacement, long N region addition, and skewed D–J gene usage, among which potential VH replacement products appear to be significant contributors. VH replacement occurs through recombinase activated gene-mediated secondary recombination and contributes to the diversified naïve B cell repertoire. During VH replacement, a short stretch of nucleotides from previously rearranged VH genes remains within the newly formed HCDR3, thus elongating its length. Accumulating evidence suggests that long HCDR3s are present in significant numbers in the human mature naïve B cell repertoire and are primarily generated by recombination during B cell development. These new observations indicate that long HCDR3s, though low in frequency, are a normal feature of the human antibody naïve repertoire and they appear to be selected to target conserved epitopes located in deep, partially obscured regions of the HIV-1 envelope trimer. Therefore, the presence of long HCDR3 sequences should not necessarily be viewed as an obstacle to the development of an HIV-1 vaccine based upon bnAb responses.

Highlights

  • The development of a protective HIV-1 vaccine is believed to be the best hope in the battle against HIV-1/AIDS

  • We review the current literature on the immunologic mechanisms for the generation of antibodies with long heavy chain complementarity-determining region 3 (HCDR3), among which potential variable heavy chain region (VH) replacement products appear to make a significant contribution in the generation of HIV-1 Broadly neutralizing antibodies (bnAbs)

  • Long HCDR3s, while relatively low in frequency, are a normal part of the naïve B cell repertoire that can actively participate in humoral immune responses

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Summary

INTRODUCTION

The development of a protective HIV-1 vaccine is believed to be the best hope in the battle against HIV-1/AIDS. HIV-1 BROADLY NEUTRALIZING ANTIBODIES HAVE UNIQUE FEATURES Many potent bnAbs have been isolated and characterized from multiple subjects in the last 5 years [21,22,23,24,25,26,27,28,29,30,31,32,33], mainly due to the application of efficient methods for isolation of human monoclonal antibodies (mAbs) [27, 30, 34,35,36,37] These new HIV-1 bnAbs are much more potent and broader than previously described neutralizing Abs. With the elucidation of crystal structures of the HIV-1 Env trimer and gp120-antibody complexes [38,39,40,41], the vulnerable epitopes on the HIV-1 Env targeted by bnAbs are becoming clear.

Class Clone V gene
DISCUSSION

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