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探究乏氧激活型铱(III)配合物敏化剂在 3D 肿瘤球体中的光毒性。

Exploring the Phototoxicity of Hypoxic Active Iridium(III)-Based Sensitizers in 3D Tumor Spheroids.

机构信息

Institut de la Matière Condensée et des Nanosciences, Molecular Chemistry, Materials and Catalysis , UCLouvain , Place Louis Pasteur 1 Box L4.01.02, B-1348 Louvain-la-Neuve , Belgium.

Institut de Recherche Expérimentale et Clinique, Pole of Pharmacology and Therapeutics , UCLouvain , Avenue Hippocrate 57 Box B1.57.04, B-1200 Woluwé-Saint-Lambert , Belgium.

出版信息

J Am Chem Soc. 2019 Nov 20;141(46):18486-18491. doi: 10.1021/jacs.9b07723. Epub 2019 Nov 6.

Abstract

Among all molecules developed for anticancer therapies, photodynamic therapeutic agents have a unique profile. Their maximal activity is specifically triggered in tumors by light, and toxicity of even systemically delivered drug is prevented in nonilluminated parts of the body. Photosensitizers exert their therapeutic effect by producing reactive oxygen species via a light-activated reaction with molecular oxygen. Consequently, the lowering of O deep in solid tumors limits their treatment and makes essential the design of oxygen-independent sensitizers. In this perspective, we have recently developed Ir(III)-based molecules able to oxidize biomolecules by type I processes under oxygen-free conditions. We examine here their phototoxicity in relevant biological models. We show that drugs, which are mitochondria-accumulated, induce upon light irradiation a dramatic decrease of the cell viability, even under low oxygen conditions. Finally, assays on 3D tumor spheroids highlight the importance of the light-activation step and the oxygen consumption rate on the drug activity.

摘要

在所有开发用于癌症治疗的分子中,光动力治疗剂具有独特的特性。它们的最大活性是在肿瘤中通过光特异性触发的,并且即使在身体未被照亮的部分,全身性给予药物也不会产生毒性。通过与分子氧的光激活反应产生活性氧,光敏剂发挥其治疗作用。因此,在实体瘤深处的氧降低限制了它们的治疗,这使得设计不依赖氧的敏化剂变得至关重要。在这方面,我们最近开发了基于 Ir(III)的分子,它们能够在无氧条件下通过 I 型过程氧化生物分子。我们在这里检查了它们在相关生物模型中的光毒性。我们表明,在光照下,积聚在线粒体中的药物即使在低氧条件下也会导致细胞活力急剧下降。最后,对 3D 肿瘤球体的测定突出了光激活步骤和耗氧率对药物活性的重要性。

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