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来自艰难梭状芽孢杆菌的一种β-内酰胺酶的特性分析。

Characterization of a beta-lactamase from Clostridium clostridioforme.

作者信息

Appelbaum P C, Spangler S K, Pankuch G A, Philippon A, Jacobs M R, Shiman R, Goldstein E J, Citron D M

机构信息

Hershey Medical Center, PA 17033.

出版信息

J Antimicrob Chemother. 1994 Jan;33(1):33-40. doi: 10.1093/jac/33.1.33.

DOI:10.1093/jac/33.1.33
PMID:8157571
Abstract

A beta-lactamase-producing strain of Clostridium clostridioforme isolated from human peritoneal fluid was examined by MIC testing and enzyme characterization. MICs of penicillins (64-512 mg/L) were higher than those of cephalosporins (8-128 mg/L); the strain was susceptible to cefoxitin (8 mg/L) and imipenem (1 mg/L). No enhancement of cephalosporin activity occurred when clavulanate was also added, but a limited degree of enhancement of penicillin activity (resulting in beta-lactam MICs higher than available NCCLS breakpoints) occurred when clavulanate, sulbactam or tazobactam was added simultaneously. By contrast, addition of BRL 42715 with amoxycillin, ticarcillin or piperacillin led to a drop in beta-lactam MICs from 512 to < or = 1 mg/L, with a drop from 64 to 1 mg/L when BRL 42715 was added with cefotaxime. All inhibitors were added at fixed concentrations of 2 mg/L. As determined spectrophotometrically, the enzyme hydrolysed penicillin G, cloxacillin and piperacillin (Vmax values (%) 372, 1816, 1001, respectively relative to cephaloridine) more efficiently than cephalosporins (69-191, with cephaloridine as 100%). Km values (microM) varied between 30-308 microM (penicillins) and 2-20 microM (cephalosporins). Relative enzyme efficiency (relative Vmax/Km with cephaloridine as 100) varied from 21-100 (cephalosporins) and 8-77 (penicillins). IC50 values (microM) with nitrocefin, piperacillin and penicillin G substrates (concentrations 20, 100 and 20 microM, respectively) were > 1000, 7, 3.5 (clavulanate); > 1000, 300, 59 (sulbactam), > 1000, 29, 7.7 (tazobactam); 0.0004, 0.001, 0.0018 (BRL 42715). The enzyme was not inhibited by EDTA, cefoxitin, cloxacillin or aztreonam, but was inhibited by pCMB.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

从人腹腔液中分离出的一株产β-内酰胺酶的艰难梭状芽胞杆菌,通过最小抑菌浓度(MIC)测试和酶特性分析进行了研究。青霉素的MIC值(64 - 512mg/L)高于头孢菌素(8 - 128mg/L);该菌株对头孢西丁(8mg/L)和亚胺培南(1mg/L)敏感。加入克拉维酸时头孢菌素活性未增强,但同时加入克拉维酸、舒巴坦或他唑巴坦时,青霉素活性有一定程度增强(导致β-内酰胺MIC值高于现有的美国国家临床实验室标准化委员会(NCCLS)断点)。相比之下,将BRL 42715与阿莫西林、替卡西林或哌拉西林联合使用时,β-内酰胺MIC值从512降至≤1mg/L,与头孢噻肟联合使用时从64降至1mg/L。所有抑制剂均以2mg/L的固定浓度添加。通过分光光度法测定,该酶水解青霉素G、氯唑西林和哌拉西林(相对于头孢菌素的Vmax值(%)分别为372、1816、1001)比水解头孢菌素(69 - 191,以头孢菌素为100%)更有效。Km值(μM)在30 - 308μM(青霉素)和2 - 20μM(头孢菌素)之间变化。相对酶效率(以头孢菌素为100的相对Vmax/Km)在21 - 100(头孢菌素)和8 - 77(青霉素)之间变化。对硝基头孢菌素、哌拉西林和青霉素G底物(浓度分别为20、100和20μM)的IC50值(μM)分别为:>1000、7、3.5(克拉维酸);>1000、300、59(舒巴坦);>1000、29、7.7(他唑巴坦);0.0004、0.001、0.0018(BRL 42715)。该酶不受EDTA、头孢西丁、氯唑西林或氨曲南抑制,但受对氯汞苯甲酸抑制。(摘要截短于250字)

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