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卡他莫拉菌中的 BRO β-内酰胺酶等位基因、抗生素耐药性及 BRO-1 选择性替代假说检验

BRO beta-lactamase alleles, antibiotic resistance and a test of the BRO-1 selective replacement hypothesis in Moraxella catarrhalis.

作者信息

Levy F, Walker E S

机构信息

Departments of Biological Sciences, Box 70703 and Internal Medicine, Box 70622, East Tennessee State University, Johnson City, TN 37614, USA.

出版信息

J Antimicrob Chemother. 2004 Feb;53(2):371-4. doi: 10.1093/jac/dkh063. Epub 2004 Jan 16.

Abstract

OBJECTIVES

The hypothesis that BRO-1 selectively replaced the BRO-2 isoform of the Moraxella catarrhalis BRO beta-lactamase was tested by examining the temporal distribution, antibiotic resistance and epidemiological characteristics of isolates from a long-term collection at a single locale.

METHODS

A rapid, one-step PCR assay conducted on 354 isolates spanning 1984-1994 distinguished bro alleles in over 97% of the beta-lactamase-producing isolates. Probes of dot blots were used to distinguish PCR failure from non-beta-lactamase-mediated penicillin resistance.

RESULTS

BRO-2 isolates comprised 0-10% of the population per year with no evidence of a decline over time. All beta-lactamase producers exceeded the clinical threshold for penicillin resistance. Bimodality of penicillin MICs for beta-lactamase producers was caused by variation within BRO-1 rather than differences between BRO-1 and BRO-2. Non-beta-lactamase factors also confer resistance to penicillin and may contribute to the BRO-1 bimodality. The 13 BRO-2 isolates were associated with diverse genotypes within which there was evidence of epidemiologically linked clusters. The exclusive association of BRO-2 with four unrelated genotypes suggested maintenance of BRO-2 by recurrent mutation or horizontal exchange.

CONCLUSIONS

The relative rarity of BRO-2 throughout the study, the absence of a declining temporal trend, and genetic diversity within BRO-2 all failed to support the hypothesis that BRO-2 was more common in the past and has been selectively replaced by BRO-1.

摘要

目的

通过检查来自单一地点长期收集的分离株的时间分布、抗生素耐药性和流行病学特征,对BRO-1选择性取代卡他莫拉菌BROβ-内酰胺酶的BRO-2亚型这一假说进行了检验。

方法

对1984年至1994年期间的354株分离株进行了快速一步PCR检测,在超过97%的产β-内酰胺酶分离株中鉴别出bro等位基因。斑点印迹探针用于区分PCR失败与非β-内酰胺酶介导的青霉素耐药性。

结果

BRO-2分离株每年占群体的0%-10%,没有随时间下降的证据。所有产β-内酰胺酶菌株均超过了青霉素耐药性的临床阈值。产β-内酰胺酶菌株青霉素MIC的双峰性是由BRO-1内的变异引起的,而不是BRO-1和BRO-2之间的差异。非β-内酰胺酶因素也赋予对青霉素的耐药性,并可能导致BRO-1双峰性。13株BRO-2分离株与不同的基因型相关,其中有流行病学相关簇的证据。BRO-2与四种不相关基因型之间唯一的关联表明,BRO-2是通过反复突变或水平交换得以维持的。

结论

在整个研究过程中BRO-2相对罕见,不存在随时间下降的趋势,以及BRO-2内存在遗传多样性,所有这些均未能支持BRO-2在过去更为常见且已被BRO-1选择性取代这一假说。

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