革兰氏阴性杆状细胞β -内酰胺酶诱导及稳定抑制的临床意义。

D M Livermore
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引用次数: 119

摘要

大多数肠杆菌和铜绿假单胞菌菌株产生染色体决定的I类β -内酰胺酶。当这些酶大量合成时,除了亚胺培南,有时还有卡比西林和替诺西林外,几乎对所有β -内酰胺类产生耐药性。当铜绿假单胞菌和肠杆菌、柠檬酸杆菌、摩根菌、吲哚阳性变形杆菌和沙雷氏菌暴露于β -内酰胺时,通过诱导,β -内酰胺酶的产生会短暂升高。永久高水平的酶生产是通过突变产生的,在这些物种的稳定抑制突变体中。这些突变体以高频率(10(-5)-10(-8)自发产生。大多数早期青霉素和第一代头孢菌素在亚抑制浓度下是I类酶的强诱导剂,头孢西丁和亚胺培南也是如此。因此,它们的mic反映了这些抗生素对诱导表达β -内酰胺酶的稳定性。除了亚胺培南,这种不稳定性通常是如此之大,以至于诱导酶引起临床耐药性。虽然大多数其他较新的头孢菌素和脲霉素对I类酶不稳定,但它们在MIC以下诱导较差,除非存在次级诱导剂(如头孢西丁或亚胺培南),否则它们的不稳定不会反映在耐药性中。虽然这些药物的弱诱导剂活性有助于维持其对诱导细胞的活性,但它使药物对先前存在的稳定抑制突变体具有高度选择性。据报道,在许多病例中,在接受β -内酰胺酶不稳定的弱诱导剂(如脲霉素和第三代头孢菌素)治疗的患者中,稳定抑制的突变体超过了可诱导的细菌种群。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical significance of beta-lactamase induction and stable derepression in gram-negative rods.

Most strains of enterobacteria and Pseudomonas aeruginosa produce chromosomally-determined Class I beta-lactamases. When synthesized copiously these enzymes cause resistance to almost all beta-lactams, except imipenem and, sometimes, carbenicillin and tenocillin. Elevated beta-lactamase production arises transiently, via induction, in Pseudomonas aeruginosa and Enterobacter, Citrobacter, Morganella, indole-positive Proteus and Serratia spp. when these organisms are exposed to beta-lactams. Permanent high-level enzyme production arises via mutation, in the stably-derepressed mutants of these species. These mutants arise spontaneously at high frequency (10(-5) -10(-8). Most early penicillins and first-generation cephalosporins are strong inducers of Class I enzymes at sub-inhibitory concentrations, as are cefoxitin and imipenem. Consequently their MICs reflect what lability these antibiotics have to inducibly-expressed beta-lactamase. Except with imipenem this lability usually is so great that the inducible enzyme causes clinical resistance. Although most other newer cephalosporins and ureidopenicillins are labile to the Class I enzymes they induce poorly below the MIC, and their lability is not reflected in resistance unless secondary inducers (e.g. cefoxitin or imipenem) are present. Although the weak inducer activity of these agents helps to maintain their activity against the inducible cells it renders the drugs highly selective for the pre-existing stably-derepressed mutants. Many cases have been reported where stably-derepressed mutants have overrun inducible populations of bacteria in patients undergoing therapy with beta-lactamase-labile weak inducers such as ureidopenicillin and third-generation cephalosporins.

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