Antibiotic-induced morphological changes enhance phage predation.

IF 4.9 1区 医学 Q1 MICROBIOLOGY
Julián Bulssico, Swapnesh Panigrahi, Mélanie Matveeva, Nicolas Ginet, Mireille Ansaldi
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Abstract

Due to the high public health risk posed by antibioresistance, phage therapy - the use of bacteriophages as antibacterial agents - is experiencing renewed interest. As the combined administration of antibiotics and phages is a common practice in compassionate treatments, our research focuses on the effects of antibiotics on phage predation, which may be of crucial importance for phage therapeutic applications. A distinctive manifestation of phage infection in solid media is the appearance of lysis plaques, corresponding to the circular thinning of a bacterial lawn. During plaque formation, successive cycles of phage replication take place from a single point of infection and spread radially in a lawn of immobilized bacterial hosts. Many factors affect plaque size, such as the composition and the reticulation of the propagation matrix, the characteristics of the phage, but also parameters related to the physiology of the bacterial host. It has also been known for decades that some antibiotics enable phages to spread more rapidly, resulting in better bacterial eradication. This phenomenon, called Phage-Antibiotic Synergy (PAS), is evidenced by larger lysis plaques on solid media. Our previous experimental work has focused on the phage characteristics and pointed to enhanced adsorption as a key factor leading to more efficient predation. However, since sublethal antibiotic concentrations can drastically affect bacterial physiology - for instance halting cell division in the case of ciprofloxacin or ceftazidime - and since plaque formation is strongly influenced by host growth dynamics, a comprehensive model integrating both the host growth and phage infection parameters is required to investigate PAS. We characterized the epidemics of two different phages (T5 and T7) during E. coli MG1655 infection on semi-solid media in the presence of sublethal antibiotic concentrations that affect (or not) cell morphology in different ways (cell filamentation or cell bloating). We observed that in these conditions lysis plaque enlargement is linked to the host's morphological changes. We conclude this work with a mathematical model that captures such observations and explains the increase in plaque size observed in the presence of antibiotics.

抗生素诱导的形态变化增强了噬菌体的捕食。
由于抗菌素耐药性对公众健康构成高度风险,噬菌体疗法——使用噬菌体作为抗菌剂——正重新引起人们的兴趣。由于抗生素和噬菌体联合使用是体恤治疗的常见做法,我们的研究重点是抗生素对噬菌体捕食的影响,这可能对噬菌体的治疗应用具有至关重要的意义。在固体培养基中噬菌体感染的一个独特表现是出现溶解斑块,对应于细菌草坪的圆形变薄。在斑块形成过程中,噬菌体复制的连续周期从一个感染点开始,并在固定的细菌宿主中呈放射状传播。影响斑块大小的因素有很多,如增殖基质的组成和网状结构、噬菌体的特性,以及与细菌宿主生理有关的参数。几十年来,人们也知道一些抗生素能使噬菌体传播得更快,从而更好地消灭细菌。这种现象被称为噬菌体-抗生素协同作用(PAS),固体介质上较大的溶解斑块就是证据。我们之前的实验工作主要集中在噬菌体的特性上,并指出增强吸附是导致更有效捕食的关键因素。然而,由于亚致死浓度的抗生素可以极大地影响细菌的生理机能——例如在环丙沙星或头孢他啶的情况下停止细胞分裂——并且由于菌斑的形成受到宿主生长动力学的强烈影响,因此需要一个综合宿主生长和噬菌体感染参数的综合模型来研究PAS。我们描述了在半固体培养基上感染大肠杆菌MG1655期间,两种不同噬菌体(T5和T7)在亚致死抗生素浓度的存在下以不同方式(细胞丝化或细胞膨胀)影响(或不影响)细胞形态的流行。我们观察到,在这些条件下,溶解斑块扩大与宿主的形态变化有关。我们用一个数学模型来总结这项工作,该模型捕获了这些观察结果,并解释了在抗生素存在下观察到的斑块大小的增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Pathogens
PLoS Pathogens MICROBIOLOGY-PARASITOLOGY
自引率
3.00%
发文量
598
期刊介绍: Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.
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