Given the cl'/> Carbamylmethyl Mercaptoacetate Thioether: A Novel Scaffold for the Development of L1 Metallo-β-lactamase Inhibitors
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Carbamylmethyl Mercaptoacetate Thioether: A Novel Scaffold for the Development of L1 Metallo-β-lactamase Inhibitors

机译:氨基甲基甲基巯基乙酸酯:一种新型支架,用于开发L1金属-β-内酰胺酶抑制剂

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摘要

Given the clinical importance of metallo-β-lactamases (MβLs), a new scaffold, N-substituted carbamylmethyl mercaptoacetate thioether, was constructed. The obtained molecules 1–16 inhibited MβLs from all three subclasses, but preferentially L1 from subclass B3. Compound 9 with a p-carboxyphenyl substituent exhibited the broadest spectrum with at least 70% inhibition of enzymes from all subclasses at 100 μM, while compound 5 with a p-methylphenyl substituent was the most potent inhibitor of any individual enzyme, with 97% inhibition at 100 μM and an IC50 value of 0.41 μM against L1. Isothermal titration calorimetry assays corroborate findings from UV–vis spectrophotometric assays that the inhibition of L1 by 5 is dose-dependent. Docking studies suggest that the carboxyl group, the sulfide atom, and the carbonyl group of the carbamyl coordinate Zn2 in a chelating fashion. Using E. coli cells expressing L1, 6 and 8 were able to decrease cefazolin minimum inhibitory concentration 8-fold.]]>
机译:<! [鉴于Metallo-β-内酰胺酶(Mβ-LS)的临床重要性,构建了一种新的支架,N取代的氨基甲基甲基巯基乙酸甲酯硫代乙酸甲酯硫代硫代乙酸硫代醚醚。所得分子 1 - 16抑制来自所有三个亚类的MβL,但优先于亚类B3优先L1。具有 P - 羧基取代基的化合物 9 表现出最广泛的光谱,其抑制来自100μm的所有亚类的酶至少70%,而化合物 5 使用 P - 甲基苯基取代基是任何单个酶的最有效的抑制剂,在100μm下抑制97%,IC 50 值为0.41μm。等温滴定量热法测定来自UV-Vis分光光度法测定的证实结果,即L1通过 5 / B>的抑制是依赖性的。对接研究表明羧基,硫化物原子和氨基甲酰坐标Zn2的羰基以螯合方式。使用 e。表达L1, 6 / B>和 8 /β的细胞能够降低CeFazolin最小抑制浓度8倍。]>

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  • 来源
    《ACS medicinal chemistry letters》 |2017年第5期|共6页
  • 作者

    Ya-Nan Chang; Yang Xiang; Yue-Juan Zhang; Wen-Ming Wang; Cheng Chen; Peter Oelschlaeger; Ke-Wu Yang;

  • 作者单位

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

    Department of Pharmaceutical Sciences College of Pharmacy Western University of Health Sciences 309 East Second Street Pomona California 91766 United States;

    Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education Chemical Biology Innovation Laboratory College of Chemistry and Materials Science Northwest University Xi’an 710127 P. R. China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;化学;
  • 关键词

    Antibiotic resistance; inhibitor; L1; mercaptoacetate thioether; metallo-β-lactamase;

    机译:抗生素抗性;抑制剂;L1;巯基乙酸酯硫醚;金属-β-内酰胺酶;
  • 入库时间 2022-08-20 00:55:27

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