Tandem bispecific neutralizing antibody eliminates HIV-1 infection in humanized mice
Xilin Wu, … , Paul Zhou, Zhiwei Chen
Xilin Wu, … , Paul Zhou, Zhiwei Chen
Published February 20, 2018
Citation Information: J Clin Invest. 2018;128(6):2239-2251. https://doi.org/10.1172/JCI96764.
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Research Article AIDS/HIV Virology

Tandem bispecific neutralizing antibody eliminates HIV-1 infection in humanized mice

Abstract

The discovery of an HIV-1 cure remains a medical challenge because the virus rebounds quickly after the cessation of combination antiretroviral therapy (cART). Here, we investigate the potential of an engineered tandem bispecific broadly neutralizing antibody (bs-bnAb) as an innovative product for HIV-1 prophylactic and therapeutic interventions. We discovered that by preserving 2 single-chain variable fragment (scFv) binding domains of each parental bnAb, a single gene–encoded tandem bs-bnAb, BiIA-SG, displayed substantially improved breadth and potency. BiIA-SG neutralized all 124 HIV-1–pseudotyped viruses tested, including global subtypes/recombinant forms, transmitted/founder viruses, variants not susceptible to parental bnAbs and to many other bnAbs with an average IC50 value of 0.073 μg/ml (range < 0.001–1.03 μg/ml). In humanized mice, an injection of BiIA-SG conferred sterile protection when administered prior to challenges with diverse live HIV-1 stains. Moreover, whereas BiIA-SG delayed viral rebound in a short-term therapeutic setting when combined with cART, a single injection of adeno-associated virus–transferred (AAV-transferred) BiIA-SG gene resulted dose-dependently in prolonged in vivo expression of BiIA-SG, which was associated with complete viremia control and subsequent elimination of infected cells in humanized mice. These results warrant the clinical development of BiIA-SG as a promising bs-bnAb–based biomedical intervention for the prevention and treatment of HIV-1 infection.

Authors

Xilin Wu, Jia Guo, Mengyue Niu, Minghui An, Li Liu, Hui Wang, Xia Jin, Qi Zhang, Ka Shing Lam, Tongjin Wu, Hua Wang, Qian Wang, Yanhua Du, Jingjing Li, Lin Cheng, Hang Ying Tang, Hong Shang, Linqi Zhang, Paul Zhou, Zhiwei Chen

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Figure 3

Neutralizing activity of BiIA-DG and BiIA-SG.

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Neutralizing activity of BiIA-DG and BiIA-SG. (A) The graph shows the br...
(A) The graph shows the breadth and the IC50 and IC90 values of BiIA-DG and BiIA-SG compared with parental IAs and the bnAb VRC01-IgG against the HKU panel of 40 pseudoviruses of various subtypes. Since the molecular weights of IAs are smaller than those of BiIAs and regular antibodies, equimolar concentration (nM) is used for comparison. Error bars indicate mean with 95% CI; 2-tailed, unpaired, Student’s t tests were performed. ***P < 0.001; **P < 0.01. (B) The graph shows the IC90 values of BiIA-SG compared with parental IA-PGT128 (left) and IA-Hu5A8 (middle) against monoresistant viruses, and the IC50 values of BiIA-SG against dual-resistant viruses (right). Each pseudovirus was tested in duplicate in our experiments. (C) Two live R5-tropic HIV-1 strains, HIV-1JR-FL (subtype B) and HIV-1BJZS7 (subtype CRF01_AE), were tested for neutralization by BiIA-SG compared with 2 parental IAs and their combination. HIV-1BJZS7 is a T/F strain. Data represent duplicate mean ± SD. All experiments were repeated twice.