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囊性纤维化中的肺部感染:从微生物复杂性中获得临床见解。

Lung infections in cystic fibrosis: deriving clinical insight from microbial complexity.

机构信息

Molecular Microbiology Research Laboratory, Pharmaceutical Science Division, 150 Stamford Street, Franklin-Wilkins Building, King's College London, London, SE1 9NH, UK.

出版信息

Expert Rev Mol Diagn. 2010 Mar;10(2):187-96. doi: 10.1586/erm.09.81.

Abstract

Lower respiratory tract bacterial infections, such as those associated with cystic fibrosis lung disease, represent a major healthcare burden. Treatment strategies are currently informed by culture-based routine diagnostics whose limitations, including an inability to isolate all potentially clinically significant bacterial species present in a sample, are well documented. Some advances have resulted from the introduction of culture-independent molecular assays for the detection of specific pathogens. However, the application of bacterial community profiling techniques to the characterization of these infections has revealed much higher levels of microbial diversity than previously recognized. These findings are leading to a fundamental shift in the way such infections are considered. Increasingly, polymicrobial infections are being viewed as complex communities of interacting organisms, with dynamic processes key to their pathogenicity. Such a model requires an analytical strategy that provides insight into the interactions of all members of the infective community. The rapid advance in sequencing technology, along with protocols that limit analysis to viable bacterial cells, are for the first time providing an opportunity to gain such insight.

摘要

下呼吸道细菌感染,如与囊性纤维化肺病相关的感染,是一个主要的医疗保健负担。目前的治疗策略是基于培养的常规诊断,其局限性包括无法分离样本中存在的所有具有潜在临床意义的细菌。一些进展来自于检测特定病原体的非培养依赖性分子检测方法的引入。然而,将细菌群落分析技术应用于这些感染的特征描述,揭示了比以前认识到的更高水平的微生物多样性。这些发现正在导致人们对这些感染的看法发生根本性转变。越来越多的混合感染被视为相互作用的生物体的复杂群落,其动态过程是其致病性的关键。这种模型需要一种分析策略,能够深入了解感染性群落中所有成员的相互作用。测序技术的快速发展,以及将分析限制在存活细菌细胞的方案,首次为获得这种洞察力提供了机会。

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