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SHV-2β-内酰胺酶的核苷酸序列与系统发育

Nucleotide sequence and phylogeny of SHV-2 beta-lactamase.

作者信息

Huletsky A, Couture F, Levesque R C

机构信息

Département de Microbiologie, Faculté de Médecine, Université Laval, Quebec, Canada.

出版信息

Antimicrob Agents Chemother. 1990 Sep;34(9):1725-32. doi: 10.1128/AAC.34.9.1725.

Abstract

We determined the nucleotide sequence of the blaSHV-2(pBP60-1) gene from Klebsiella ozaenae which confers resistance to broad-spectrum cephalosporins. The structural gene encodes a polypeptide product of 286 amino acids, and the estimated molecular weight of the mature protein is 28,900. Amino acid sequence comparison of the SHV-2pBP60-1 enzyme with all known class A beta-lactamases and homology studies showed that the residues were highly conserved. Furthermore, SHV-2pBP60-1 was clearly related to SHV-1, LEN-1, and OHIO-1. The SHV-2pBP60-1 enzyme differed from SHV-1 isolated from Klebsiella pneumoniae by seven amino acid substitutions. One of these substitutions, the Gly----Ser substitution at position 234, is probably a key region for the novel activity of cefotaxime hydrolysis. A phylogenetic tree was constructed by using all class A beta-lactamases of known sequences by a progressive alignment method. The data suggested that the beta-lactamases of gram-positive Streptomyces, Staphylococcus, and Bacillus species appeared early in evolution, followed by the PSE and CARB enzymes of Pseudomonas species and, more recently, by the SHV-type and TEM-type enzymes found in enteric bacteria. Larger evolutionary distances separated clusters of the gram-positive beta-lactamases than separated clusters of the gram-negative enzymes. Results of this phylogenetic study suggested that extended-spectrum enzymes are recent derivatives that are selected by the use of new cephalosporins.

摘要

我们测定了来自鼻硬结克雷伯菌的blaSHV - 2(pBP60 - 1)基因的核苷酸序列,该基因赋予对广谱头孢菌素的抗性。结构基因编码一个由286个氨基酸组成的多肽产物,成熟蛋白的估计分子量为28,900。将SHV - 2pBP60 - 1酶与所有已知的A类β - 内酰胺酶进行氨基酸序列比较及同源性研究表明,这些残基高度保守。此外,SHV - 2pBP60 - 1与SHV - 1、LEN - 1和OHIO - 1明显相关。SHV - 2pBP60 - 1酶与从肺炎克雷伯菌分离出的SHV - 1在7个氨基酸替换上有所不同。其中一个替换,即第234位的甘氨酸替换为丝氨酸,可能是头孢噻肟水解新活性的关键区域。通过逐步比对法,利用所有已知序列的A类β - 内酰胺酶构建了系统发育树。数据表明,革兰氏阳性链霉菌、葡萄球菌和芽孢杆菌属的β - 内酰胺酶在进化早期出现,随后是假单胞菌属的PSE和CARB酶,最近是在肠道细菌中发现的SHV型和TEM型酶。革兰氏阳性β - 内酰胺酶簇之间的进化距离比革兰氏阴性酶簇之间的进化距离更大。这项系统发育研究的结果表明,超广谱酶是通过使用新型头孢菌素选择出来的近期衍生物。

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Nucleotide sequence and phylogeny of SHV-2 beta-lactamase.SHV-2β-内酰胺酶的核苷酸序列与系统发育
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