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In Vitro and In Silico Studies of Glycyrrhetinic Acid Derivatives as Anti- Filarial Agents

马来丝虫 体外 二乙基卡马嗪 生物信息学 淋巴丝虫病 药理学 药品 伊维菌素 化学 天然产物 巴汉吉丝虫 生物化学 生物 丝虫病 蠕虫 免疫学 基因 动物
作者
Rekha Tyagi,S. C. Verma,Shikha Mishra,Mrigank Srivastava,Sarfaraz Alam,Feroz Khan,Santosh K. Srivastava
出处
期刊:Current Topics in Medicinal Chemistry [Bentham Science]
卷期号:19 (14): 1191-1200 被引量:13
标识
DOI:10.2174/1568026619666190618141450
摘要

Lymphatic filariasis is one of the chronic diseases in many parts of the tropics and sub-tropics of the world despite the use of standard drugs diethylcarbamazine and ivermectin because they kill microfilaries and not the adult parasites. Therefore, new leads with activity on adult parasites are highly desirable.Anti-filarial lead optimization by semi-synthetic modification of glycyrrhetinic acid (GA).The GA was first converted into 3-O-acyl derivative, which was further converted into 12 amide derivatives. All these derivatives were assessed for their antifilarial potential by parasite motility assay. The binding affinity of active GA derivatives on trehalose-6-phosphate phosphatase (Bm-TPP) was assessed by molecular docking studies.Among 15 GA derivatives, GAD-2, GAD-3, and GAD-4 were found more potent than the GA and standard drug DEC. These derivatives reduced the motility of Brugia malayi adult worms by up to 74% while the GA and DEC reduced only up to 49%. Further, GA and most of its derivatives exhibited two times more reduction in MTT assay when compared to the standard drug DEC. These derivatives also showed 100% reduction of microfilariae and good interactions with Bm-TPP protein.The present study suggests that 3-O-acyl and linear chain amide derivatives of glycyrrhetinic acid may be potent leads against B. malayi microfilariae and adult worms. These results might be helpful in developing QSAR model for optimizing a new class of antifilarial lead from a very common, inexpensive, and non toxic natural product.

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