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通过靶向缀合到支架抗体来开发新型长效抗糖尿病 FGF21 模拟物。

Development of a novel long-acting antidiabetic FGF21 mimetic by targeted conjugation to a scaffold antibody.

机构信息

CovX Research, Pfizer Worldwide Research and Development, San Diego, California, USA.

出版信息

J Pharmacol Exp Ther. 2013 Aug;346(2):270-80. doi: 10.1124/jpet.113.204420. Epub 2013 May 29.

DOI:10.1124/jpet.113.204420
PMID:23720456
Abstract

Fibroblast growth factor (FGF)21 improves insulin sensitivity, reduces body weight, and reverses hepatic steatosis in preclinical species. We generated long-acting FGF21 mimetics by site-specific conjugation of the protein to a scaffold antibody. Linking FGF21 through the C terminus decreased bioactivity, whereas bioactivity was maintained by linkage to selected internal positions. In mice, these CovX-Bodies retain efficacy while increasing half-life up to 70-fold compared with wild-type FGF21. A preferred midlinked CovX-Body, CVX-343, demonstrated enhanced in vivo stability in preclinical species, and a single injection improved glucose tolerance for 6 days in ob/ob mice. In diet-induced obese mice, weekly doses of CVX-343 reduced body weight, blood glucose, and lipids levels. In db/db mice, CVX-343 increased glucose tolerance, pancreatic β-cell mass, and proliferation. CVX-343, created by linkage of the CovX scaffold antibody to the engineered residue A129C of FGF21 protein, demonstrated superior preclinical pharmacodynamics by extending serum half-life of FGF21 while preserving full therapeutic functionality.

摘要

成纤维细胞生长因子 21 (FGF21) 可改善胰岛素敏感性、降低体重并逆转临床前物种的肝脂肪变性。我们通过将蛋白质特异性连接到支架抗体上来产生长效 FGF21 模拟物。通过 C 末端连接 FGF21 会降低其生物活性,而通过与选定的内部位置连接则可以保持其生物活性。在小鼠中,与野生型 FGF21 相比,这些 CovX 抗体保留了功效,同时半衰期延长了 70 倍。一种优选的中链 CovX 抗体 CVX-343 在临床前物种中表现出增强的体内稳定性,单次注射可使 ob/ob 小鼠的葡萄糖耐量提高 6 天。在饮食诱导的肥胖小鼠中,每周给予 CVX-343 可降低体重、血糖和血脂水平。在 db/db 小鼠中,CVX-343 可提高葡萄糖耐量、增加胰岛 β 细胞质量和增殖。CVX-343 通过将 CovX 支架抗体与 FGF21 蛋白的工程残基 A129C 连接而产生,通过延长 FGF21 的血清半衰期同时保留其全部治疗功能,显示出优越的临床前药效学。

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