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细菌碳青霉烯类抗生素生产基因分析揭示了一条新的β-内酰胺生物合成途径。

Analysis of bacterial carbapenem antibiotic production genes reveals a novel beta-lactam biosynthesis pathway.

作者信息

McGowan S J, Sebaihia M, Porter L E, Stewart G S, Williams P, Bycroft B W, Salmond G P

机构信息

Department of Biochemistry, University of Cambridge, UK.

出版信息

Mol Microbiol. 1996 Nov;22(3):415-26.

PMID:8939426
Abstract

Carbapenems are beta-lactam antibiotics which have an increasing utility in chemotherapy, particularly for nosocomial, multidrug-resistant infections. Strain GS101 of the bacterial phytopathogen, Erwinia carotovora, makes the simple beta-lactam antibiotic, 1-carbapen-2-em-3-carboxylic acid. We have mapped and sequenced the Erwinia genes encoding carbapenem production and have cloned these genes into Escherichia coli where we have reconstituted, for the first time, functional expression of the beta-lactam in a heterologous host. The carbapenem synthesis gene products are unrelated to enzymes involved in the synthesis of the so-called sulphur-containing beta-lactams, namely penicillins, cephamycins and cephalosporins. However, two of the carbapenem biosynthesis genes, carA and carC, encode proteins which show significant homology with proteins encoded by the Streptomyces clavuligerus gene cluster responsible for the production of the beta-lactamase inhibitor, clavulanic acid. These homologies, and some similarities in genetic organization between the clusters, suggest an evolutionary relatedness between some of the genes encoding production of the antibiotic and the beta-lactamase inhibitor. Our observation are consistent with the evolution of a second major biosynthetic route to the production of beta-lactam-ring-containing antibiotics.

摘要

碳青霉烯类是β-内酰胺类抗生素,在化疗中应用日益广泛,尤其用于医院获得性多重耐药感染。细菌性植物病原体胡萝卜软腐欧文氏菌的GS101菌株能产生简单的β-内酰胺抗生素1-碳青霉烯-2-烯-3-羧酸。我们已对编码碳青霉烯产生的欧文氏菌基因进行了定位和测序,并将这些基因克隆到大肠杆菌中,首次在异源宿主中实现了β-内酰胺的功能性表达。碳青霉烯合成基因产物与参与合成所谓含硫β-内酰胺(即青霉素、头孢霉素和头孢菌素)的酶无关。然而,碳青霉烯生物合成基因中的两个基因carA和carC,编码的蛋白质与负责产生β-内酰胺酶抑制剂克拉维酸的链霉菌基因簇所编码的蛋白质具有显著同源性。这些同源性以及基因簇之间在遗传组织上的一些相似性,表明在一些编码抗生素和β-内酰胺酶抑制剂产生的基因之间存在进化相关性。我们的观察结果与含β-内酰胺环抗生素产生的第二条主要生物合成途径的进化一致。

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