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用于通过荧光监测实现高效药物释放的可见光和近红外光光可激活羟基肉桂酸酯系统。

Visible and NIR light photoactivatable -hydroxycinnamate system for efficient drug release with fluorescence monitoring.

作者信息

Gupta Ajay, Singh Neelu, Gautam Aryan, Dhakar Neetesh, Kumar Sunil, Sasmal Pijus K

机构信息

School of Physical Sciences, Jawaharlal Nehru University New Delhi 110067 India

Department of Physics, Indian Institute of Technology Delhi New Delhi 110016 India.

出版信息

RSC Med Chem. 2023 Mar 1;14(6):1088-1100. doi: 10.1039/d2md00438k. eCollection 2023 Jun 22.

Abstract

Photoactivatable protecting groups (PPGs) have become powerful materials for controlling the activity of biologically important molecules in the biomedical field. However, designing PPGs that can be efficiently activated by biologically benign visible and NIR light with fluorescence monitoring is still a great challenge. Herein, we report -hydroxycinnamate-based PPGs that can be activated by both visible (one-photon) and NIR (two-photon) light for controlled drug release with real-time monitoring. Thus, a photoremovable 7-diethylamino -hydroxycinnamate group is covalently attached to an anticancer drug, gemcitabine, to establish a photoactivatable prodrug system. Upon excitation by visible (400-700 nm) or NIR (800 nm) light, the prodrug efficiently releases drug which is quantified by monitoring the formation of a strongly fluorescent coumarin reporter. The prodrug is taken up by the cancer cells and interestingly accumulates within mitochondria as determined by FACS and fluorescence microscopy imaging. Further, the prodrug demonstrates photo-triggered, dose-dependent, and temporally controlled cell death upon irradiation with both visible and NIR light. This photoactivatable system could be useful and adapted in the future for the development of advanced therapies in biomedicine.

摘要

光可激活保护基团(PPGs)已成为生物医学领域中控制生物重要分子活性的有力材料。然而,设计能够通过生物良性可见光和近红外光有效激活并进行荧光监测的PPGs仍然是一个巨大的挑战。在此,我们报道了基于对羟基肉桂酸酯的PPGs,其可通过可见光(单光子)和近红外光(双光子)激活,用于可控药物释放并进行实时监测。因此,一个可光去除的7 - 二乙氨基对羟基肉桂酸酯基团共价连接到抗癌药物吉西他滨上,以建立一个光可激活前药系统。在可见光(400 - 700 nm)或近红外光(800 nm)激发下,前药有效释放药物,通过监测强荧光香豆素报告基团的形成来对药物进行定量。前药被癌细胞摄取,有趣的是,通过流式细胞术和荧光显微镜成像确定其在线粒体内积累。此外,前药在用可见光和近红外光照射时均表现出光触发、剂量依赖性和时间可控的细胞死亡。这种光可激活系统未来可能对生物医学中先进疗法的开发有用且适用。

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