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Phage-Derived Peptidoglycan Degrading Enzymes: Challenges and Future Prospects for In Vivo Therapy

机译:噬菌体衍生的肽聚糖降解酶:体内治疗的挑战和未来前景。

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摘要

Peptidoglycan degrading enzymes are of increasing interest as antibacterial agents, especially against multi-drug resistant pathogens. Herein we present a review about the biological features of virion-associated lysins and endolysins, phage-derived enzymes that have naturally evolved to compromise the bacterial peptidoglycan from without and from within, respectively. These natural features may determine the adaptability of the enzymes to kill bacteria in different environments. Endolysins are by far the most studied group of peptidoglycan-degrading enzymes, with several studies showing that they can exhibit potent antibacterial activity under specific conditions. However, the lytic activity of most endolysins seems to be significantly reduced when tested against actively growing bacteria, something that may be related to fact that these enzymes are naturally designed to degrade the peptidoglycan from within dead cells. This may negatively impact the efficacy of the endolysin in treating some infections in vivo. Here, we present a critical view of the methods commonly used to evaluate in vitro and in vivo the antibacterial performance of PG-degrading enzymes, focusing on the major hurdles concerning in vitro-to-in vivo translation.
机译:肽聚糖降解酶作为抗菌剂,尤其是针对多重耐药性病原体的抗菌剂越来越受到关注。在这里,我们提出有关病毒体相关的溶素和内溶素,从噬菌体衍生的酶的生物学特征的综述,所述噬菌体衍生的酶已经自然进化以分别损害来自和不来自内部的细菌肽聚糖。这些自然特征可能决定酶在不同环境中杀死细菌的适应性。迄今为止,内溶素是肽聚糖降解酶研究最多的一组,多项研究表明它们在特定条件下具有强大的抗菌活性。但是,当针对活跃的细菌进行测试时,大多数溶血素的溶解活性似乎显着降低,这可能与以下事实有关:这些酶是天然设计用于从死细胞中降解肽聚糖的。这可能会对内溶素在体内治疗某些感染的功效产生负面影响。在这里,我们提出了通常用于评估体外和体内PG降解酶的抗菌性能的方法的批判性观点,重点是有关体外到体内翻译的主要障碍。

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