GB12-09, a bispecific antibody targeting IL4Rα and IL31Rα for atopic dermatitis therapy

Author:

Deng Feiyan12,Qiu Yuxin12,Zhang Xiangling12,Guo Nining12,Hu Junhong12,Yang Wenjie12,Shang Wei12,Liu Bicheng34,Qin Suofu12

Affiliation:

1. Drug Discovery , Center for Research and Development, , Shenzhen 518057 , China

2. Kexing BioPharma Co., Ltd , Center for Research and Development, , Shenzhen 518057 , China

3. Institute of Nephrology , Zhong Da Hospital, , Nanjing 999077 , China

4. Southeast University School of Medicine , Zhong Da Hospital, , Nanjing 999077 , China

Abstract

Abstract Atopic dermatitis (AD) is a chronic inflammatory skin condition characterized by dysregulated immune responses. The key mediators of AD pathogenesis are T helper 2 (TH2) cells and TH2 cytokines. Targeting interleukin 4 (IL4), IL13 or IL31 has become a pivotal focus in both research and clinical treatments for AD. However, the need remains pressing for the development of a more effective and safer therapy, as the current approaches often yield low response rates and adverse effects. In response to this challenge, we have engineered a immunoglobulin G—single-chain fragment variable (scFv) format bispecific antibody (Ab) designed to concurrently target IL4R and IL31R. Our innovative design involved sequence optimization of VL-VH and the introduction of disulfide bond (VH44-VL100) within the IL31Rα Ab scFv region to stabilize the scFv structure. Our bispecific Ab efficiently inhibited the IL4/IL13/IL31 signaling pathways in vitro and reduced serum immunoglobulin E and IL31 levels in vivo. Consequently, this intervention led to improved inflammation profiles and notable amelioration of AD symptoms. This research highlighted a novel approach to AD therapy by employing bispecific Ab targeting IL4Rα and IL31Rα with potent efficacy.

Funder

Shenzhen Government, China

Shenzhen Kexing BioPharma Co., Ltd

Publisher

Oxford University Press (OUP)

Subject

Immunology,Immunology and Allergy

Reference41 articles.

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