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条件性抗菌肽治疗学。

Conditional Antimicrobial Peptide Therapeutics.

机构信息

Howard Hughes Medical Institute, Cambridge, Massachusetts 02139, United States.

Department of Medicine, Brigham and Women's Hospital and Harvard Medical School, Boston Massachusetts 02115, United States.

出版信息

ACS Nano. 2022 Oct 25;16(10):15779-15791. doi: 10.1021/acsnano.2c04162. Epub 2022 Aug 18.

Abstract

Antimicrobial peptides (AMPs) constitute a promising class of alternatives to antibiotics to curb antimicrobial resistance. Nonetheless, their utility as a systemic agent is hampered by short circulation time and toxicity. Infection sites, analogous to tumors, harbor an aberrant microenvironment that has the potential to be exploited to develop conditionally activated therapeutics with an improved therapeutic index. In particular, we identified strategies to prolong systemic circulation of small, cationic AMPs in a mouse model of bacterial pneumonia. Specifically, we report an albumin-binding domain (ABD)-AMP conjugate as a long-circulating conditional AMP therapeutic with a masked activity that can be liberated by proteases in the infected tissue microenvironment. Our systemically administered conjugate enhanced the pulmonary delivery of active AMP while also reducing AMP exposure to other off-target organs. Importantly, this reduction in off-target exposure improved the safety profile of the AMP. The framework we present can be generalized to quantify and optimize the performance of this emerging class of conditional therapeutics.

摘要

抗菌肽 (AMPs) 是一类很有前途的抗生素替代品,可以抑制抗菌药物耐药性。然而,由于其循环时间短和毒性,它们作为全身性药物的应用受到了限制。感染部位类似于肿瘤,拥有一种可能被利用的异常微环境,以开发具有改善治疗指数的条件激活治疗药物。特别是,我们确定了在细菌性肺炎的小鼠模型中延长小分子阳离子 AMP 系统循环的策略。具体来说,我们报告了一种白蛋白结合域 (ABD)-AMP 缀合物,作为一种具有潜伏活性的长循环条件 AMP 治疗药物,其活性可被感染组织微环境中的蛋白酶释放。我们系统给予的缀合物增强了 AMP 在肺部的递送,同时减少了 AMP 暴露于其他非靶标器官。重要的是,这种减少非靶标暴露提高了 AMP 的安全性。我们提出的框架可以推广来量化和优化这一新兴的条件治疗药物类别的性能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1532/9619929/a27af0fc2a1e/nn2c04162_0001.jpg

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