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开发融合 Fc 的可卡因水解酶用于可卡因成瘾治疗:催化和药代动力学特性。

Development of Fc-Fused Cocaine Hydrolase for Cocaine Addiction Treatment: Catalytic and Pharmacokinetic Properties.

机构信息

Molecular Modeling and Biopharmaceutical Center (MMBC) and Department of Pharmaceutical Sciences, College of Pharmacy, University of Kentucky, 789 South Limestone Street, Lexington, KY, 40536, USA.

出版信息

AAPS J. 2018 Mar 19;20(3):53. doi: 10.1208/s12248-018-0214-9.

Abstract

Cocaine abuse is a worldwide public health and social problem without a US Food and Drug Administration (FDA)-approved medication. Accelerating cocaine metabolism that produces biologically inactive metabolites by administration of an efficient cocaine hydrolase (CocH) has been recognized as a promising strategy for cocaine abuse treatment. However, the therapeutic effects of CocH are limited by its short biological half-life (e.g., 8 h or shorter in rats). In this study, we designed and prepared a set of Fc-fusion proteins constructed by fusing Fc(M3) with CocH3 at the N-terminus of CocH3. A linker between the two protein domains was optimized to improve both the biological half-life and catalytic activity against cocaine. It has been concluded that Fc(M3)-GS-CocH3 not only has fully retained the catalytic efficiency of CocH3 against cocaine but also has the longest biological half-life (e.g., ∼ 136 h in rats) among all of the long-acting CocHs identified so far. A single dose (0.2 mg/kg, IV) of Fc(M3)-GS-CocH3 was able to significantly attenuate 15 mg/kg cocaine-induced hyperactivity for at least 11 days (268 h) after the Fc(M3)-GS-CocH3 administration.

摘要

可卡因滥用是一个全球性的公共卫生和社会问题,目前还没有获得美国食品和药物管理局 (FDA) 批准的药物。通过给予高效可卡因水解酶 (CocH) 来加速可卡因代谢,生成无生物活性的代谢物,已被认为是治疗可卡因滥用的一种有前途的策略。然而,CocH 的治疗效果受到其短的生物半衰期(例如,在大鼠中为 8 小时或更短)的限制。在本研究中,我们设计并制备了一组由 Fc(M3)与 CocH3 的 N 端融合而成的 Fc 融合蛋白。优化了两个蛋白结构域之间的连接子,以提高对可卡因的生物半衰期和催化活性。研究结果表明,Fc(M3)-GS-CocH3 不仅完全保留了 CocH3 对可卡因的催化效率,而且具有迄今为止鉴定的所有长效 CocHs 中最长的生物半衰期(例如,在大鼠中约为 136 小时)。单次给药(0.2 mg/kg,静脉注射)Fc(M3)-GS-CocH3 能够显著减轻 15 mg/kg 可卡因诱导的多动至少 11 天(268 小时)。

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