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单细胞视角下的非生长但代谢活跃(NGMA)细菌。

A single-cell perspective on non-growing but metabolically active (NGMA) bacteria.

机构信息

School of Life Sciences, Swiss Federal Institute of Technology in Lausanne (EPFL), 1015, Lausanne, Switzerland,

出版信息

Curr Top Microbiol Immunol. 2013;374:135-61. doi: 10.1007/82_2013_333.

Abstract

A long-standing and fundamental problem in microbiology is the non-trivial discrimination between live and dead cells. The existence of physically intact and possibly viable bacterial cells that fail to replicate during a more or less protracted period of observation, despite environmental conditions that are ostensibly propitious for growth, has been extensively documented in many different organisms. In clinical settings, non-culturable cells may contribute to non-apparent infections capable of reactivating after months or years of clinical latency, a phenomenon that has been well documented in the specific case of Mycobacterium tuberculosis. The prevalence of these silent but potentially problematic bacterial reservoirs has been highlighted by classical approaches such as limiting culture dilution till extinction of growing cells, followed by resuscitation of apparently "viable but non-culturable" (VBNC) subpopulations. Although these assays are useful to demonstrate the presence of VBNC cells in a population, they are effectively retrospective and are not well suited to the analysis of non-replicating cells per se. Here, we argue that research on a closely related problem, which we shall refer to as the "non-growing but metabolically active" state, is poised to advance rapidly thanks to the recent development of novel technologies and methods for real-time single-cell analysis. In particular, the combination of fluorescent reporter dyes and strains, microfluidic and microelectromechanical systems, and time-lapse fluorescence microscopy offers tremendous and largely untapped potential for future exploration of the physiology of non-replicating cells.

摘要

长期以来,微生物学的一个基本问题是难以区分活细胞和死细胞。在许多不同的生物体中,广泛记录了这样一种现象:尽管环境条件表面上有利于生长,但仍存在物理上完整且可能具有活力的细菌细胞,它们在或多或少长时间的观察期间无法复制。在临床环境中,无法培养的细胞可能导致非明显感染,这些感染在数月或数年后的临床潜伏期后重新活跃,这种现象在结核分枝杆菌的具体情况下得到了很好的记录。这些沉默但潜在有问题的细菌储库的普遍性已通过经典方法得到强调,例如将培养稀释到生长细胞灭绝,然后复苏明显的“存活但不可培养”(VBNC)亚群。尽管这些检测对于证明群体中存在 VBNC 细胞很有用,但它们实际上是回顾性的,并且不适合分析本身不复制的细胞。在这里,我们认为,由于用于实时单细胞分析的新技术和方法的最新发展,我们将其称为“非生长但代谢活跃”状态的相关问题的研究有望迅速取得进展。特别是,荧光报告染料和菌株、微流控和微机电系统以及延时荧光显微镜的组合为未来探索非复制细胞的生理学提供了巨大且尚未充分开发的潜力。

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