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一株大肠杆菌在多次菌血症发作期间超广谱β-内酰胺耐药性(SHV-8)的演变

Evolution of extended-spectrum beta-lactam resistance (SHV-8) in a strain of Escherichia coli during multiple episodes of bacteremia.

作者信息

Rasheed J K, Jay C, Metchock B, Berkowitz F, Weigel L, Crellin J, Steward C, Hill B, Medeiros A A, Tenover F C

机构信息

Nosocomial Pathogens Laboratory Branch, Centers for Disease Control and Prevention, Atlanta, Georgia 30333, USA.

出版信息

Antimicrob Agents Chemother. 1997 Mar;41(3):647-53. doi: 10.1128/AAC.41.3.647.

Abstract

Nine isolates of Escherichia coli were recovered from seven blood cultures over a period of 3 months from a 19-month-old female with aplastic anemia. Initial isolates were susceptible to extended-spectrum cephalosporins, including ceftazidime (MIC, < or = 0.25 microgram/ml), but gradually became resistant to this drug (MICs, > or = 128 micrograms/ml) and other cephalosporins and the monobactam aztreonam. Molecular typing methods, including plasmid profile analysis, pulsed-field gel electrophoresis, and arbitrarily primed PCR, indicated that the nine isolates were derived from a common ancestor. Dot blot hybridization and PCR analysis of total bacterial DNA using blaSHV- and blaTEM-specific DNA probes and primers identified the presence of a blaTEM beta-lactamase gene in all of the isolates and a blaSHV gene in the isolates with elevated ceftazidime MICs. Isoelectric focusing analysis of crude lysates showed that all nine isolates contained an enzyme with a pI of 5.4 corresponding to the TEM-1 beta-lactamase, and those isolates containing an SHV-type beta-lactamase demonstrated an additional band with a pI of 7.6. The first of the ceftazidime-resistant isolates appeared to hyperproduce the SHV enzyme compared to the other resistant isolates. DNA sequencing revealed a blaSHV-1 gene in the first ceftazidime-resistant isolate and a novel blaSHV gene, blaSHV-8, with an Asp-to-Asn substitution at amino acid position 179 in the remaining four isolates. Three of the ceftazidime-resistant isolates also showed a change in porin profile. The patient had received multiple courses of antimicrobial agents during her illness, including multiple courses of ceftazidime. This collection of blood isolates from the same patient appears to represent the in vivo evolution of resistance under selective pressure of treatment with various cephalosporins.

摘要

在3个月的时间里,从一名19个月大的再生障碍性贫血女性患者的7次血培养中分离出9株大肠杆菌。最初分离出的菌株对包括头孢他啶(MIC,≤0.25微克/毫升)在内的广谱头孢菌素敏感,但逐渐对该药物(MIC,≥128微克/毫升)以及其他头孢菌素和单环β-内酰胺类氨曲南产生耐药性。分子分型方法,包括质粒图谱分析、脉冲场凝胶电泳和随机引物PCR,表明这9株分离菌来源于一个共同祖先。使用blaSHV和blaTEM特异性DNA探针及引物对细菌总DNA进行斑点杂交和PCR分析,发现在所有分离菌中均存在blaTEMβ-内酰胺酶基因,而在头孢他啶MIC升高的分离菌中存在blaSHV基因。对粗裂解物进行等电聚焦分析表明,所有9株分离菌均含有一种pI为5.4的酶,对应于TEM-1β-内酰胺酶,而那些含有SHV型β-内酰胺酶的分离菌显示出一条pI为7.6的额外条带。与其他耐药分离菌相比,第一株对头孢他啶耐药的分离菌似乎超量产生SHV酶。DNA测序显示,第一株对头孢他啶耐药的分离菌中存在blaSHV-1基因,而其余4株分离菌中存在一个新的blaSHV基因blaSHV-8,在氨基酸位置179处有天冬氨酸到天冬酰胺的替换。3株对头孢他啶耐药的分离菌的孔蛋白图谱也发生了变化。该患者在患病期间接受了多疗程的抗菌药物治疗,包括多疗程的头孢他啶。从同一患者采集的这些血液分离菌似乎代表了在各种头孢菌素治疗的选择压力下耐药性的体内演变。

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