An anti-CTLA-4 heavy chain–only antibody with enhanced T reg depletion shows excellent preclinical efficacy and safety profile

Author:

Gan Xin1,Shan Qianqian1,Li He1,Janssens Rick12,Shen Yuqiang1,He Yun1,Chen Fei1,van Haperen Rien12,Drabek Dubravka12ORCID,Li Jin1,Zhang Yang1ORCID,Zhao Jiuqiao1,Qin Beibei1ORCID,Jheng Ming-Jin1,Chen Victor1,Wang Jingsong1,Rong Yiping1,Grosveld Frank12

Affiliation:

1. Harbour BioMed, Shanghai 201203, China

2. Department of Cell Biology, Erasmus Medical Center, 3000 CA Rotterdam, The Netherlands

Abstract

The value of anti-CTLA-4 antibodies in cancer therapy is well established. However, the broad application of currently available anti-CTLA-4 therapeutic antibodies is hampered by their narrow therapeutic index. It is therefore challenging and attractive to develop the next generation of anti-CTLA-4 therapeutics with improved safety and efficacy. To this end, we generated fully human heavy chain–only antibodies (HCAbs) against CTLA-4. The hIgG1 Fc domain of the top candidate, HCAb 4003-1, was further engineered to enhance its regulatory T (T reg ) cell depletion effect and to decrease its half-life, resulting in HCAb 4003-2. We tested these HCAbs in in vitro and in vivo experiments in comparison with ipilimumab and other anti-CTLA4 antibodies. The results show that human HCAb 4003-2 binds human CTLA-4 with high affinity and potently blocks the binding of B7-1 (CD80) and B7-2 (CD86) to CTLA-4. The results also show efficient tumor penetration. HCAb 4003-2 exhibits enhanced antibody-dependent cellular cytotoxicity function, lower serum exposure, and more potent anti-tumor activity than ipilimumab in murine tumor models, which is partly driven by a substantial depletion of intratumoral T reg s. Importantly, the enhanced efficacy combined with the shorter serum half-life and less systemic drug exposure in vivo potentially provides an improved therapeutic window in cynomolgus monkeys and preliminary clinical applications. With its augmented efficacy via T reg depletion and improved safety profile, HCAb 4003-2 is a promising candidate for the development of next generation anti-CTLA-4 therapy.

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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