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二氢吩嗪铱(III)配合物作为一种光毒性的癌症干细胞选择性、线粒体靶向试剂。

Dipyridophenazine iridium(III) complex as a phototoxic cancer stem cell selective, mitochondria targeting agent.

机构信息

Czech Academy of Sciences, Institute of Biophysics, Brno, CZ-61265, Czech Republic.

Departamento de Quimica Inorganica, Universidad de Murcia and Institute for Bio- Health Research of Murcia (IMIB-Arrixaca), E-30071, Murcia, Spain.

出版信息

Chem Biol Interact. 2022 Jun 1;360:109955. doi: 10.1016/j.cbi.2022.109955. Epub 2022 Apr 18.

DOI:10.1016/j.cbi.2022.109955
PMID:35447138
Abstract

In this work, the mechanism underlying the anticancer activity of a photoactivatable Ir(III) compound of the type [Ir(C^N)(dppz)][PF] where C^N = 1-methyl-2-(2'-thienyl)benzimidazole (complex 1) was investigated. Complex 1 photoactivated by visible light shows potent activity against highly aggressive and poorly treatable Rhabdomyosarcoma (RD) cells, the most frequent soft tissue sarcomas of children. This remarkable activity of 1 was observed not only in RD cells cultured in 2D monolayers but, more importantly, also in 3D spheroids, which resemble in many aspects solid tumors and serve as a promising model to mimic the in vivo situation. Importantly, photoactivated 1 kills not only differentiated RD cells but also even more effectively cancer stem cells (CSCs) of RD. One of the factors responsible for the activity of irradiated 1 in RD CSCs is its ability to produce ROS in these cells more effectively than in differentiated RD cells. Moreover, photoactivated 1 caused in RD differentiated cells and CSCs a significant decrease of mitochondrial membrane potential and promotes opening mitochondrial permeability transition pores in these cells, a mechanism that has never been demonstrated for any other metal-based anticancer complex. The results of this work give evidence that 1 has a potential for further evaluation using in vivo models as a promising chemotherapeutic agent for photodynamic therapy of hardly treatable human Rhabdomyosarcoma, particularly for its activity in both stem and differentiated cancer cells.

摘要

在这项工作中,研究了一种光活化型 Ir(III)配合物[Ir(C^N)(dppz)][PF](其中 C^N = 1-甲基-2-(2'-噻吩基)苯并咪唑(配合物 1))的抗癌活性的作用机制。可见光激活的配合物 1 对高度侵袭性和治疗效果差的横纹肌肉瘤 (RD) 细胞表现出很强的活性,RD 是儿童最常见的软组织肉瘤。这种令人瞩目的 1 的活性不仅在二维单层培养的 RD 细胞中观察到,而且更重要的是在 3D 球体中也观察到,3D 球体在许多方面类似于实体肿瘤,并作为模拟体内情况的有前途的模型。重要的是,光活化的 1 不仅可以杀死分化的 RD 细胞,而且还可以更有效地杀死 RD 的癌症干细胞 (CSC)。辐照 1 在 RD CSCs 中具有活性的一个因素是其在这些细胞中比在分化的 RD 细胞中更有效地产生 ROS 的能力。此外,光活化的 1 导致 RD 分化细胞和 CSCs 中线粒体膜电位显著下降,并促进这些细胞中线粒体通透性转换孔的开放,这是任何其他基于金属的抗癌配合物都从未证明过的机制。这项工作的结果表明,1 具有进一步在体内模型中进行评估的潜力,作为一种很有前途的光动力疗法药物,用于治疗难以治疗的人类横纹肌肉瘤,特别是其在干细胞和分化癌细胞中的活性。

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