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摩根氏摩根菌AmpCβ-内酰胺酶三种新变体的生化与分子特征

Biochemical and molecular characterization of three new variants of AmpC beta-lactamases from Morganella morganii.

作者信息

Power Pablo, Galleni Moreno, Ayala Juan A, Gutkind Gabriel

机构信息

Cátedra de Microbiología, Facultad de Farmacia y Bioquímica, Universidad de Buenos Aires, Junín 954, Buenos Aires 1113, Argentina.

出版信息

Antimicrob Agents Chemother. 2006 Mar;50(3):962-7. doi: 10.1128/AAC.50.3.962-967.2006.

Abstract

Morganella morganii produces an inducible, chromosomally encoded AmpC beta-lactamase. We describe in this study three new variants of AmpC within this species with apparent pIs of 6.6 (M19 from M. morganii strain PP19), 7.4 (M29 from M. morganii strain PP29), and 7.8 (M37 from M. morganii strain PP37). After gene sequencing, deduced amino acid sequences displayed one to six substitutions when compared to the available Morganella AmpC sequences. An AmpR-encoding gene was also found upstream of ampC, including the LysR regulators' helix-turn-helix DNA-binding domain and the putative T-N11-A-protected region in the ampR-ampC intercistronic sequence. All three AmpC variants were purified from in vitro-generated derepressed mutants and showed overall similar kinetic parameters. None of the observed amino acid changes, occurring at the surface of the protein, appear to have a major influence in their catalytic properties. Morganella AmpCs exhibit the highest catalytic efficiencies (k(cat)/K(m)) on classical penicillins, cefoxitin, narrow-spectrum cephalosporins, and cefotaxime. Cefotaxime was more effectively hydrolyzed than other oxyimino-cephalosporins, whereas cefepime was 3 log-fold less efficiently hydrolyzed than other cephalosporins such as cephalothin. Several differences with other AmpC beta-lactamases were found. Ampicillin was more efficiently hydrolyzed than benzylpenicillin. High k(cat)/K(m) values were observed for oxacillin and piperacillin, which are usually poor substrates for AmpC. A fairly efficient hydrolysis of imipenem was detected as well. Aztreonam, carbenicillin, and tazobactam were effective transient inactivators of these variants.

摘要

摩根氏摩根菌产生一种可诱导的、染色体编码的AmpCβ-内酰胺酶。我们在本研究中描述了该菌种内三种新的AmpC变体,其表观pI分别为6.6(来自摩根氏摩根菌PP19菌株的M19)、7.4(来自摩根氏摩根菌PP29菌株的M29)和7.8(来自摩根氏摩根菌PP37菌株的M37)。基因测序后,与现有的摩根氏菌AmpC序列相比,推导的氨基酸序列显示有1至6个取代。在ampC上游还发现了一个编码AmpR的基因,包括LysR调节因子的螺旋-转角-螺旋DNA结合结构域以及ampR-ampC基因间序列中假定的T-N11-A保护区域。所有三种AmpC变体均从体外产生的去阻遏突变体中纯化得到,并且显示出总体相似的动力学参数。在蛋白质表面发生的所有观察到的氨基酸变化似乎对其催化特性没有重大影响。摩根氏菌AmpC对经典青霉素、头孢西丁、窄谱头孢菌素和头孢噻肟表现出最高的催化效率(k(cat)/K(m))。头孢噻肟比其他氧亚氨基头孢菌素更有效地被水解,而头孢吡肟比其他头孢菌素如头孢噻吩的水解效率低3个对数级。发现了与其他AmpCβ-内酰胺酶的几个差异。氨苄西林比苄青霉素更有效地被水解。观察到奥沙西林和哌拉西林具有较高的k(cat)/K(m)值,而它们通常是AmpC的不良底物。还检测到亚胺培南有相当有效的水解。氨曲南、羧苄青霉素和他唑巴坦是这些变体的有效瞬时失活剂。

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