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噬菌体介导的细菌生物防治动力学

Kinetics of phage-mediated biocontrol of bacteria.

作者信息

Abedon Stephen T

机构信息

Department of Microbiology, The Ohio State University, Mansfield, Ohio 44906, USA.

出版信息

Foodborne Pathog Dis. 2009 Sep;6(7):807-15. doi: 10.1089/fpd.2008.0242.

Abstract

Bacteriophages (phages) are the viruses of bacteria. One subset of phages, those that can be described as obligately lytic, can effect an active phage therapy because their population growth occurs at the expense of bacterial survival. That is, phages can be employed to reduce bacterial loads--such as in animals preslaughter, in foods postharvest, or in humans postinfection--and in the process can actually increase what in pharmacological terms would be their antibacterial dose. This self-amplification may provide advantages if either antibacterial dosing or penetration to target bacteria is otherwise constrained. One situation in which these kinetic aspects of drug delivery may be constrained is in preslaughter treatment of food animals toward control of zoonotic pathogens (e.g., Escherichia coli O157:H7 in cattle). In such treatment, the self-amplifying nature of phages may be harnessed, though potentially under time constraints. In this discursive I cover three areas. The first is semantic, where I contrast the terms phage therapy and phage-mediated biocontrol of bacteria, both of which are employed to describe similar but perhaps not identical procedures. Second, I consider the importance of time in therapy or biocontrol procedures while contrasting passive versus active therapies. Third, I discuss conceptually how to go about modifying phage characteristics to increase rates of phage population growth and do so explicitly by casting phage infection in terms of Michaelis-Menten saturation kinetics. I conclude suggesting that phage therapy ultimately may be rationally guided by theoretical considerations of the impact of phage properties on rates of phage population growth.

摘要

噬菌体是细菌的病毒。噬菌体的一个子集,即那些可被描述为专性裂解的噬菌体,可实现积极的噬菌体疗法,因为它们的种群增长是以细菌的存活为代价的。也就是说,噬菌体可用于减少细菌数量——例如在屠宰前的动物、收获后的食品或感染后的人类体内——并且在此过程中实际上可以增加从药理学角度来说的抗菌剂量。如果抗菌给药或对靶细菌的渗透在其他方面受到限制,这种自我扩增可能会带来优势。药物递送的这些动力学方面可能受到限制的一种情况是在对食用动物进行屠宰前处理以控制人畜共患病原体(例如牛体内的大肠杆菌O157:H7)时。在这种处理中,虽然可能受到时间限制,但可以利用噬菌体的自我扩增特性。在这篇论述中,我涵盖三个领域。第一个是语义方面,我对比了噬菌体疗法和噬菌体介导的细菌生物防治这两个术语,这两个术语都用于描述相似但可能不完全相同的程序。其次,我在对比被动疗法和主动疗法的同时,考虑时间在治疗或生物防治程序中的重要性。第三,我从概念上讨论如何着手改变噬菌体特性以提高噬菌体种群增长率,并通过根据米氏饱和动力学来描述噬菌体感染明确做到这一点。我得出结论,认为噬菌体疗法最终可能会由关于噬菌体特性对噬菌体种群增长率影响的理论考虑进行合理指导。

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