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巯基苯乙酸的一系列硫酯衍生物对金属β-内酰胺酶的抑制作用。

Inhibition of metallo-beta-lactamases by a series of thiol ester derivatives of mercaptophenylacetic acid.

作者信息

Payne D J, Bateson J H, Gasson B C, Khushi T, Proctor D, Pearson S C, Reid R

机构信息

SmithKline Beecham Pharmaceuticals, Collegeville, PA 19426-0989, USA. David_J

出版信息

FEMS Microbiol Lett. 1997 Dec 1;157(1):171-5. doi: 10.1111/j.1574-6968.1997.tb12769.x.

Abstract

A series of mercaptophenylacetic acid thiol esters bearing a phenyl substituent adjacent to the carboxylic acid function has been shown to be inhibitors of metallo-beta-lactamases. The inhibition of the Bacteroides fragilis CfiA and Bacillus cereus II metallo-beta-lactamases was Zn2- dependent, greater inhibition being observed at 1 microM ZnSO4 than at 100 microM ZnSO4. Despite this Zn2+ dependency, isothermal titration calorimetry studies illustrated that representative compounds had no detectable affinity for Zn2+ (K > 1 mM). This indicates that their mode of inhibition was not by chelation of the active site Zn2+. Greatest potency was observed against the Stenotrophomonas maltophilia L1 metallo-beta-lactamase with I50 values of between < 1.95 microM and 6 microM and SB-217843 exhibited a similar level of inhibition of this enzyme at 1 and 100 microM Zn2+ (I50 values 5 and 6 microM, respectively). Inhibition of B. cereus II metallo-beta-lactamase by SB-218018 and SB-217782 was competitive with Ki values of 185 microM and 1500 microM, respectively. Therefore, these compounds are specific inhibitors of metallo-beta-lactamases and provide further probes of the active sites of these enzymes.

摘要

一系列在羧酸官能团相邻位置带有苯基取代基的巯基苯乙酸硫醇酯已被证明是金属β-内酰胺酶的抑制剂。脆弱拟杆菌CfiA和蜡样芽孢杆菌II金属β-内酰胺酶的抑制作用依赖于Zn2+,在1 microM硫酸锌时观察到的抑制作用比在100 microM硫酸锌时更强。尽管存在这种对Zn2+的依赖性,但等温滴定量热法研究表明,代表性化合物对Zn2+没有可检测到的亲和力(K>1 mM)。这表明它们的抑制模式不是通过螯合活性位点的Zn2+。对嗜麦芽窄食单胞菌L1金属β-内酰胺酶观察到最大的效力,I50值在<1.95 microM和6 microM之间,并且SB-217843在1 microM和100 microM Zn2+时对该酶表现出相似水平的抑制作用(I50值分别为5 microM和6 microM)。SB-218018和SB-217782对蜡样芽孢杆菌II金属β-内酰胺酶的抑制作用具有竞争性,Ki值分别为185 microM和1500 microM。因此,这些化合物是金属β-内酰胺酶的特异性抑制剂,并为这些酶的活性位点提供了进一步的探针。

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