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一种靶向线粒体的对硝基还原酶敏感的自裂解间隔基,作为不带电荷的胺基分子的有效载体。

A mitochondria targeted nitroreductase-sensitive self-immolative spacer as an efficient shuttle for uncharged amine-based molecules.

作者信息

Michel Laurane, Steinmetz Vincent, Godel-Pastre Sophia, Durand Philippe, Chevalier Arnaud

机构信息

Université Paris-Saclay, CNRS, Institut de Chimie des Substances Naturelles, UPR 2301 Gif-sur-Yvette 91198 France

出版信息

Chem Sci. 2025 Jul 16. doi: 10.1039/d5sc03665h.

Abstract

Mitochondria have emerged as critical therapeutic targets in a wide range of diseases. The detailed examination of this organelle, as well as the search for methods to efficiently address it, therefore, represent significant challenges. In this article, we present a simple and robust method for the functionalization of uncharged amine-based molecules to enable their intracellular transport and selective accumulation in mitochondria. To this end, we have synthesized a self-immolative spacer that is both sensitive to mitochondrial nitroreductase and incorporates a triphenylphosphonium vectorising moiety. To demonstrate the efficacy of this mitochondrial shuttling technology, we have designed, synthesized, and employed a fluorogenic probe that unambiguously validates the concept. An initial extension of this technology for therapeutic purposes is proposed through the intramitochondrial delivery of native doxorubicin, showing promising potential for overcoming drug resistance mechanisms.

摘要

线粒体已成为多种疾病的关键治疗靶点。因此,对这种细胞器进行详细检查以及寻找有效应对方法面临重大挑战。在本文中,我们提出了一种简单且可靠的方法,用于使不带电荷的胺基分子功能化,以实现其细胞内运输并选择性积聚于线粒体中。为此,我们合成了一种对线粒体硝基还原酶敏感且含有三苯基膦靶向部分的自裂解间隔物。为证明这种线粒体穿梭技术的功效,我们设计、合成并应用了一种荧光探针,明确验证了这一概念。通过线粒体内递送天然阿霉素,提出了该技术用于治疗目的的初步扩展,显示出克服耐药机制的潜在前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c4f/12422130/3d56cdf5e68e/d5sc03665h-f1.jpg

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