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

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

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

机译：新型酰胺连接的18β-甘草酸衍生物的设计，合成和生物学评价为新的ALK抑制剂

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A series of novel amide-linked 18 beta-glycyrrhetinic acid derivatives were developed by incorporating substituted piperazine amide fragments into the C30-COOH of 18 beta-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.

机译：通过将取代的哌嗪酰胺碎片掺入18β-甘草酸支架的C30-COOH中，开发了一系列新的酰胺连接的18β-甘油吡咯酸衍生物。通过MTT测定评估对karpas299，a549，hepg2，MCF-7和PC-3细胞系的抗癌活性的合成化合物。此外，一些具有苯基部分的吸电子基团的化合物表现出明显的抗增殖活性。还发现最有效的化合物4a对正常人肝细胞LO2细胞无毒。化合物4A对野生型ALK具有适度的抑制活性，IC50值为203.56nm，相对较弱的有效活性至C-Met（IC50> 1000nm）。进行分子对接研究以探讨化合物4a和x序列布之间的粘合图案中的多样化。

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《RSC Advances 》 |2020年第20期| 共13页
作者
Cai Dong; Zhang Zhi Hua; Chen Yu; Ruan Chao; Li Sheng Qiang; Chen Shi Qin; Chen Lian Shan;
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Jinzhou Med Univ Coll Publ Basic Sci Jinzhou 121001 Peoples R China;

Liaoning Univ Technol Sch Chem &

Environm Engn Jinzhou 121001 Peoples R China;

Shenyang Pharmaceut Univ Sch Life Sci &

Biopharmaceut Shenyang 110016 Peoples R China;

Jinzhou Med Univ Coll Pharm Jinzhou 121001 Peoples R China;

Jinzhou Med Univ Coll Pharm Jinzhou 121001 Peoples R China;

Jinzhou Med Univ Coll Pharm Jinzhou 121001 Peoples R China;

Jinzhou Med Univ Coll Pharm Jinzhou 121001 Peoples R China;

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正文语种 eng
中图分类化学 ;
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Design, synthesis and biological evaluation of novel amide-linked 18 beta-glycyrrhetinic acid derivatives as novel ALK inhibitors

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