利用生物正交“纳米工厂”原位生产抗生素。

Microbiology insights Pub Date : 2021-02-24 eCollection Date: 2021-01-01 DOI:10.1177/1178636121997121
Cheng-Hsuan Li, Rui Huang, Jessa Marie Makabenta, Suzannah Schmidt-Malan, Robin Patel, Vincent M Rotello
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引用次数: 6

摘要

前药策略使用化学修饰来改善母体药物的药代动力学特性,从而提高治疗效果。传统的前药方法使用内源性酶进行激活。生物正交催化使用内源性酶无法进入的过程,为前药脱壳提供了一种补充策略。利用合成催化剂对前药进行位点选择性活化(解溶)是一种很有前途的药物局部活化策略。我们在这里讨论了最近的研究,将金属催化剂纳入聚合物和纳米颗粒支架中,以提供生物相容性的“类酶”催化剂,这种催化剂可以穿透细菌生物膜并原位激活前药抗生素,为治疗细菌生物膜感染提供了一种新的策略,并有可能减少脱靶效应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

<i>In situ</i> Generation of Antibiotics using Bioorthogonal "Nanofactories".

<i>In situ</i> Generation of Antibiotics using Bioorthogonal "Nanofactories".

In situ Generation of Antibiotics using Bioorthogonal "Nanofactories".

Prodrug strategies use chemical modifications to improve the pharmacokinetic properties and therefore therapeutic effects of parent drugs. Traditional prodrug approaches use endogenous enzymes for activation. Bioorthogonal catalysis uses processes that endogenous enzymes cannot access, providing a complementary strategy for prodrug uncaging. Site-selective activation of prodrugs to drugs (uncaging) using synthetic catalysts is a promising strategy for localized drug activation. We discuss here recent studies that incorporate metal catalysts into polymers and nanoparticle scaffolds to provide biocompatible "enzyme-like" catalysts that can penetrate bacterial biofilms and activate prodrug antibiotics in situ, affording a new strategy to treat bacterial biofilm infections with the potential for reduced off-target effects.

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