OXA-Type β-Lactamases

整合子 氯嘧啶 克拉维酸 亚胺培南 氨基酸 丝氨酸 生物 微生物学 化学 生物化学 抗生素 抗生素耐药性 阿莫西林 青霉素
作者
Thierry Naas,Patrice Nordmann
出处
期刊:Current Pharmaceutical Design [Bentham Science Publishers]
卷期号:5 (11): 865-879 被引量:143
标识
DOI:10.2174/1381612805666230112185101
摘要

The OXA-type (oxacillin-hydrolysing) enzymes are widespread and have been mostly described in Enterobacteriaceae and in P. aeruginosa. They usually confer resistance to amino- and ureidopenicillin and possess high-level hydrolytic activity against cloxacillin, oxacillin, and methicillin. Their activities are weakly inhibited by clavulanic acid but sodium chloride (NaCl) possesses a strong il'lhibition activity. Oxacillin-hydrolysing -lactamases belong to Ambler class D and thus possess an active serine site as classes A and C β-lactamases. Overall amino-acid identities between class D and class A or class C β-lactamases is about 16%. Until now, 24 Ambler class D enzymes, named OXA-1 to OXA-22, AmpS and LCR-1, have been characterised, either by sequence and/or by biochemical analyses, but for none of them a three dimensional structure is yet available. While some oxacillinases present a significant degree of amino-acid identity (for example, OXA-l and OXA-4; OXA-10 (PSE-2) derivatives; OXA-2 and OXA- 3), most of them are only weakly related (20% to 30% amino-acid identity). Oxacillinases usually display a restricted-spectrum phenotype. However extension of their spectrum towards oxyimino cephalosporins and/or imipenem has recently been observed mostly as a consequence of point mutations in OXA-2 or OXA-10 derivatives. Their frequent plasmid- and/or integron-location provide them a mean for a wide diffusion.

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