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基因型到表型的困境:实验室应如何处理不一致的易感性结果?

The Genotype-to-Phenotype Dilemma: How Should Laboratories Approach Discordant Susceptibility Results?

机构信息

Department of Pathology and Laboratory Medicine, Children's Hospital Los Angeles, Los Angeles, California, USA.

Keck School of Medicine, University of Southern California, Los Angeles, California, USA.

出版信息

J Clin Microbiol. 2021 May 19;59(6). doi: 10.1128/JCM.00138-20.

Abstract

Traditional culture-based methods for identification and antimicrobial susceptibility testing (AST) of bacteria take 2 to 3 days on average. Syndromic molecular diagnostic panels have revolutionized clinical microbiology laboratories as they can simultaneously identify an organism and detect some of the most significant antimicrobial resistance (AMR) genes directly from positive blood culture broth or from various specimen types (e.g., whole blood, cerebrospinal fluid, and respiratory specimens). The presence or absence of an AMR marker associated with a particular organism can be used to predict the phenotypic AST results to more rapidly guide therapy. Numerous studies have shown that genotypic susceptibility predictions by syndromic panels can improve patient outcomes. However, an important limitation of AMR marker detection to predict phenotype is the potential discrepancies that may arise upon performing phenotypic AST of the recovered organism in culture. The focus of this minireview is to address how clinical laboratories should interpret rapid molecular results from commercial platforms in relation to phenotypic AST. Stepwise approaches and solutions are provided to resolve discordant results between genotypic and phenotypic susceptibility results.

摘要

基于传统文化的细菌鉴定和抗菌药物敏感性测试(AST)方法平均需要 2 到 3 天。综合征分子诊断试剂盒已彻底改变了临床微生物学实验室,因为它们可以直接从阳性血培养肉汤或各种标本类型(例如全血、脑脊液和呼吸道标本)中同时鉴定生物体并检测一些最重要的抗菌药物耐药性(AMR)基因。与特定生物体相关的 AMR 标志物的存在与否可用于预测表型 AST 结果,从而更快速地指导治疗。许多研究表明,综合征检测试剂盒的基因型药敏预测可以改善患者的预后。然而,通过综合征检测试剂盒进行 AMR 标志物检测来预测表型存在一个重要的局限性,即可能会在对培养物中回收的生物体进行表型 AST 时出现差异。本篇综述的重点是解决临床实验室应如何根据表型 AST 解释商业平台上的快速分子结果。提供了逐步的方法和解决方案来解决基因型和表型药敏结果之间的不相符。

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