Mitochondria targeted fluorogenic theranostic agents for cancer therapy

线粒体 化学 癌细胞 药效团 罗丹明123 癌症 细胞器 线粒体内膜 细胞凋亡 生物化学 生物 遗传学 多重耐药 抗生素
作者
H.B. Singh,Divya Sareen,Jiya Mary George,Vineet Bhardwaj,Saehee Rha,Suk Joong Lee,Sheetal Sharma,Amit Sharma,Jong Seung Kim
出处
期刊:Coordination Chemistry Reviews [Elsevier BV]
卷期号:452: 214283-214283 被引量:54
标识
DOI:10.1016/j.ccr.2021.214283
摘要

Mitochondria, an eukaryotic organelle, is regarded as the most critical target since it regulates several vital functions in cell physiology. It is the hub of metabolic activity and a source of fascination due to its role in a variety of diseases like cardiovascular, cancer and neurological disorders. Because of the structural and functional discrepancies between normal and cancerous mitochondria (respiratory rate, membrane potential, genetic mutations and energy-producing pathway), mitochondria have garnered substantial attention in cancer therapy. For delivering cytotoxins exclusively to mitochondria, several synthetic strategies are used for mitochondrial dysfunction and cell apoptosis/necrosis. Covalent binding of lipophilic cations (triphenylphosphonium ion, rhodamine, peptides etc) to the molecular-based pharmacophore is the most effective process. Significant mitochondrial accumulations (>1000 folds) can be accomplished by proper selection of cell types, their mitochondrial membrane potential and targeting unit. In this review article, we address various strategies for targeting small molecule-based theranostics to cancerous mitochondria for diagnostic and potential therapeutic purposes that have been published since 2015. Particularly, conventional chemotherapeutic drugs, photosensitizers for photodynamic and photothermal treatment, drug-free agents, intra-mitochondrial aggregation agents and their combination are among the molecular-based agents discussed.
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