An Efficiently Cleaved HIV-1 Clade C Env Selectively Binds to Neutralizing Antibodies |
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| Authors: | Saikat Boliar Supratik Das Manish Bansal Brihaspati N Shukla Shilpa Patil Tripti Shrivastava Sweety Samal Sandeep Goswami C Richter King Jayanta Bhattacharya Bimal K Chakrabarti |
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| Institution: | 1. THSTI-IAVI HIV Vaccine Design Program, Translational Health Science and Technology Institute, 496 Udyog Vihar, Phase-III, Gurgaon-122 016, Haryana, India.; 2. IAVI Vaccine Design, New York, NY, United States of America.; CIP, NCI-Frederick, NIH, UNITED STATES, |
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| Abstract: | An ideal HIV-1 Env immunogen is expected to mimic the native trimeric conformation for inducing broadly neutralizing antibody responses. The native conformation is dependent on efficient cleavage of HIV-1 Env. The clade B isolate, JRFL Env is efficiently cleaved when expressed on the cell surface. Here, for the first time, we report the identification of a native clade C Env, 4-2.J41 that is naturally and efficiently cleaved on the cell surface as confirmed by its biochemical and antigenic characteristics. In addition to binding to several conformation-dependent neutralizing antibodies, 4-2.J41 Env binds efficiently to the cleavage-dependent antibody PGT151; thus validating its native cleaved conformation. In contrast, 4-2.J41 Env occludes non-neutralizing epitopes. The cytoplasmic-tail of 4-2.J41 Env plays an important role in maintaining its conformation. Furthermore, codon optimization of 4-2.J41 Env sequence significantly increases its expression while retaining its native conformation. Since clade C of HIV-1 is the prevalent subtype, identification and characterization of this efficiently cleaved Env would provide a platform for rational immunogen design. |
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