Design, synthesis and biological evaluation of novel amide-linked 18β-glycyrrhetinic acid derivatives as novel ALK inhibitors

Dong Cai; Zhi Hua Zhang; Yu Chen; Chao Ruan; Sheng Qiang Li; Shi Qin Chen; Lian Shan Chen

doi:10.1039/d0ra00681e

Design, synthesis and biological evaluation of novel amide-linked 18β-glycyrrhetinic acid derivatives as novel ALK inhibitors

RSC Adv. 2020 Mar 23;10(20):11694-11706. doi: 10.1039/d0ra00681e. eCollection 2020 Mar 19.

Authors

Dong Cai¹, Zhi Hua Zhang², Yu Chen³, Chao Ruan⁴, Sheng Qiang Li⁴, Shi Qin Chen⁴, Lian Shan Chen⁴

Affiliations

¹ College of Public Basic Sciences, Jinzhou Medical University Jinzhou 121001 China.
² School of Chemical and Environmental Engineering, Liaoning University of Technology Jinzhou 121001 China.
³ School of Life Science and Biopharmaceutics, Shenyang Pharmaceutical University Shenyang 110016 China.
⁴ College of Pharmacy, Jinzhou Medical University Jinzhou 121001 China 509205162@QQ.com.

Abstract

A series of novel amide-linked 18β-glycyrrhetinic acid derivatives were developed by incorporating substituted piperazine amide fragments into the C30-COOH of 18β-glycyrrhetinic acid scaffold. The synthesized compounds were evaluated for their anticancer activity against Karpas299, A549, HepG2, MCF-7, and PC-3 cell lines by MTT assay. Besides, some compounds with electron-withdrawing groups on phenyl moieties exhibited noticeable antiproliferative activity. The most potent compound 4a was also found to be non-toxic to normal human hepatocytes LO2 cells. The compound 4a exhibited moderate inhibitory activity against wild-type ALK with an IC₅₀ value of 203.56 nM and relatively weak potent activity to c-Met (IC₅₀ > 1000 nM). Molecular docking studies were performed to explore the diversification in bonding patterns between the compound 4a and Crizotinib.