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使用富含组氨酸的肽作为载体将硫醇化货物选择性细胞内递送至肿瘤和新生血管细胞。

Selective Intracellular Delivery of Thiolated Cargo to Tumor and Neovasculature Cells Using Histidine-Rich Peptides as Vectors.

作者信息

Eksteen J Johannes, Ausbacher Dominik, Vasskog Terje, Rekdal Øystein, Svendsen John S M

机构信息

NORCE Norwegian Research Centre AS, Siva Innovasjonssenter, Sykehusvegen 21, NO 9294 Tromsø, Norway.

Department of Pharmacy, UiT Arctic University of Norway, NO 9037 Tromsø, Norway.

出版信息

ACS Omega. 2020 Mar 6;5(10):4937-4942. doi: 10.1021/acsomega.9b00700. eCollection 2020 Mar 17.

Abstract

Short histidine-rich peptides could serve as novel activatable vectors for delivering cytotoxic payloads to tumor and neovasculature cells. This explorative study reports preliminary results showing that zinc ions, which are found in elevated levels at neovasculature sites, can trigger the intracellular delivery of a short antimicrobial peptide when conjugated to a histidine-rich peptide through a disulfide bond. The importance of exofacial thiols in the mode of action of these disulfide-linked conjugates is also shown.

摘要

富含组氨酸的短肽可作为新型可激活载体,用于将细胞毒性载荷递送至肿瘤细胞和新生血管细胞。这项探索性研究报告了初步结果,表明在新生血管部位含量升高的锌离子,当通过二硫键与富含组氨酸的肽缀合时,可触发一种短抗菌肽的细胞内递送。还展示了细胞外硫醇在这些二硫键连接的缀合物作用模式中的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eded/7081261/5829951873f6/ao9b00700_0001.jpg

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