A novel humanized Chi3l1 blocking antibody attenuates acetaminophen-induced liver injury in mice.

Q2 Medicine
Leike Li, Yankai Wen, Daniel Wrapp, Jongmin Jeong, Peng Zhao, Wei Xiong, Constance Lynn Atkins, Zhao Shan, Deng Hui, Jason S McLellan, Ningyan Zhang, Cynthia Ju, Zhiqiang An
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Abstract

Acetaminophen (APAP) overdose is a leading cause of acute liver injury in the USA. The chitinase 3-like-1 (Chi3l1) protein contributes to APAP-induced liver injury (AILI) by promoting hepatic platelet recruitment. Here, we report the development of a Chi3l1-targeting antibody as a potential therapy for AILI. By immunizing a rabbit successively with the human and mouse Chi3l1 proteins, we isolated cross-reactive monoclonal antibodies (mAbs) from single memory B cells. One of the human and mouse Chi3l1 cross-reactive mAbs was humanized and characterized in both in vitro and in vivo biophysical and biological assays. X-ray crystallographic analysis of the lead antibody C59 in complex with the human Chi3l1 protein revealed that the kappa light contributes to majority of the antibody-antigen interaction; and that C59 binds to the 4α-5β loop and 4α-helix of Chi3l1, which is a functional epitope and hotspot for the development of Chi3l1 blocking antibodies. We humanized the C59 antibody by complementarity-determining region grafting and kappa chain framework region reverse mutations. The humanized C59 antibody exhibited similar efficacy as the parental rabbit antibody C59 in attenuating AILI in vivo. Our findings validate Chi3l1 as a potential drug target for AILI and provide proof of concept of developing Chi3l1 blocking antibody as a therapy for the treatment of AILI.

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一种新型人源化Chi3l1阻断抗体可减轻对乙酰氨基酚引起的小鼠肝损伤。
在美国,对乙酰氨基酚(APAP)过量是导致急性肝损伤的主要原因。几丁质酶3-like-1 (Chi3l1)蛋白通过促进肝血小板募集参与apap诱导的肝损伤(AILI)。在这里,我们报道了一种靶向chi31l1抗体的发展,作为治疗AILI的潜在方法。我们用人和小鼠Chi3l1蛋白先后免疫家兔,从单记忆B细胞中分离出交叉反应性单克隆抗体(mab)。其中一种人与小鼠Chi3l1交叉反应单克隆抗体被人源化,并在体外和体内进行了生物物理和生物学分析。与人Chi3l1蛋白复合物的先导抗体C59的x射线晶体分析显示,kappa光参与了大部分抗体-抗原相互作用;C59结合Chi3l1的4α-5β环和4α-螺旋,是Chi3l1阻断抗体的功能表位和发展热点。我们采用互补决定区嫁接和kappa链框架区反向突变的方法将C59抗体人源化。人源化C59抗体在体内的减毒效果与亲本兔抗体C59相似。我们的研究结果验证了Chi3l1作为AILI的潜在药物靶点,并为开发Chi3l1阻断抗体作为治疗AILI的概念提供了证据。
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来源期刊
Antibody Therapeutics
Antibody Therapeutics Medicine-Immunology and Allergy
CiteScore
8.70
自引率
0.00%
发文量
30
审稿时长
8 weeks
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