Structural optimization of natural product nordihydroguaretic acid to discover novel analogues as AcrB inhibitors

Wang Yinhu; Alenzy Rawaf; Song Di; Liu Xingbang; Teng Yuetai; Mowla Rumana; Ma Yingang; Polyak Steven W.; Venter Henrietta; Ma Shutao

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Structural optimization of natural product nordihydroguaretic acid to discover novel analogues as AcrB inhibitors

机译：天然产物Nordihysrogoaretic酸的结构优化，发现新型类似物作为ACRB抑制剂

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Drug efflux pumps confer multidrug resistance to dangerous bacterial pathogens which makes these proteins promising drug targets. Herein, we present initial chemical optimization and structure-activity relationship (SAR) data around a previously described efflux pump inhibitor, nordihydroguaretic acid (NDGA). Four series of novel NDGA analogues that target Escherichia coli AcrB were designed, synthesized and evaluated for their ability to potentiate the activity of antibiotics, to inhibit AcrB-mediated substrate efflux and reduce off-target activity. Nine novel structures were identified that increased the efficacy of a panel of antibiotics, inhibited drug efflux and reduced permeabilization of the bacterial outer and inner membranes. Among them, WA7, WB11 and WD6 possessing broad-spectrum antimicrobial sensitization activity were identified as NDGA analogues with favorable properties as potential AcrB inhibitors, demonstrating moderate improvement in potency as compared to NDGA. In particular, WD6 was the most broadly active analogue improving the activity of all four classes of antibacterials tested. (C) 2019 Elsevier Masson SAS. All rights reserved.

机译：药物流出泵对危险的细菌病原体赋予多药耐药性，这使得这些蛋白质具有前景的药物靶标。在此，我们呈现出先前描述的外源泵抑制剂（NORDIHOROG毒酸（NDGA）周围的初始化学优化和结构 - 活性关系（SAR）数据。设计了四种新的NDGA类似物，其针对靶向大肠杆菌ACRB的组合，合成和评估它们能够提高抗生素活性的能力，以抑制ACRB介导的底物流出并减少脱靶活性。鉴定了九种新颖结构，提高了抗生素面板的功效，抑制药物流出并降低细菌外膜和内膜的渗透性。其中，具有广谱抗微生物敏化活性的WA7，WB11和WD6被鉴定为具有良好性质的NDGA类似物作为潜在的ACRB抑制剂，与NDGA相比，效力的中等改善。特别是，WD6是最宽的活性的模拟改善所测试的所有四种抗菌的活性。（c）2019年Elsevier Masson SAS。版权所有。

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《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2020年第2020期|共18页
作者
Wang Yinhu; Alenzy Rawaf; Song Di; Liu Xingbang; Teng Yuetai; Mowla Rumana; Ma Yingang; Polyak Steven W.; Venter Henrietta; Ma Shutao;
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作者单位

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

Univ South Australia Sch Pharm &

Med Sci Adelaide SA 5000 Australia;

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

Univ South Australia Sch Pharm &

Med Sci Adelaide SA 5000 Australia;

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

Univ South Australia Sch Pharm &

Med Sci Adelaide SA 5000 Australia;

Univ South Australia Sch Pharm &

Med Sci Adelaide SA 5000 Australia;

Shandong Univ Dept Med Chem Key Lab Chem Biol Minist Educ Sch Pharmaceut Sci 44 West Culture Rd;

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原文格式 PDF
正文语种 eng
中图分类药学;
关键词
Nordihydroguaretic acid; Multidrug resistance; Efflux pump; AcrB inhibitors; Structural optimization;

机译：Nordihydroguaretic acid;多药电阻;Efflux泵;ACRB抑制剂;结构优化;

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机译：天然产物Nordihysrogoaretic酸的结构优化，发现新型类似物作为ACRB抑制剂
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Structural optimization of natural product nordihydroguaretic acid to discover novel analogues as AcrB inhibitors

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