基于菲罗啉-四氮唑的钌 (II) 复合物可能是抗癌剂。

IF 0.6 Q3 COMMUNICATION Southern Communication Journal Pub Date : 2023-09-07 eCollection Date: 2023-01-01 DOI:10.5812/ijpr-136738
Saeid Abaspour, Behzad Soltani, Hamed Hamishehkar, Moayad Hossaini Sadr
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引用次数: 0

摘要

背景:由于铂基金属复合物的剧毒性和耐药性,其在肿瘤学中的发展受到了限制:这项工作旨在研究钌配合物在 B16F10 细胞系治疗中的细胞毒性活性和凋亡诱导作用:我们制备了一系列创新的 Ru(II) 复合物 [Ru(Tzphen)(bpy)(dcbpy)]+2 (S1)、[Ru(dcbpy)2(Tzphen)]+2 (S2)、[Ru(Phen)2(Tzphen)]+2 (S3)、[Ru(Tzphen)(bpy)2]+2 (S4)、[Ru(dmbpy)2(Tzphen)]+2 (S5) 基于 1、10-菲罗啉配体(含四唑),并通过体外细胞毒性、活性氧、用附件素 V/PI 染色法检测细胞凋亡、自噬和细胞摄取来研究它们的抗癌特性。研究结果S1、S2、S3、S4和S5复合物对B16F10模型的细胞毒性活性与顺铂相当。此外,由于复合物的存在,细胞内 ROS 含量增加。在所研究的复合物中,与对照组相比,用 S5 复合物处理的细胞凋亡率(Q3)最高,达 14.9%。复合物的细胞吸附性也表明,S4 和 S5 复合物具有更高的细胞吸附性、更好的内化性和更高的荧光强度:本研究为在癌症治疗中设计和使用 Ru 复合物提供了重要指导。
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Ruthenium (II) Complexes Based on Phenanthroline-Tetrazole as Possible Anticancer Agents.

Background: The development of platinum-based metal complexes in oncology is limited due to vigorous toxicity and drug resistance.

Objectives: This work aimed to study the cytotoxic activity and apoptosis induction of ruthenium complexes in a B16F10 cell line therapy.

Methods: We prepared a series of innovative Ru(II) complexes [Ru(Tzphen)(bpy)(dcbpy)]+2 (S1), [Ru(dcbpy)2(Tzphen)]+2 (S2), [Ru(Phen)2(Tzphen)]+2 (S3), [Ru(Tzphen)(bpy)2]+2 (S4), [Ru(dmbpy)2(Tzphen)]+2 (S5) based on 1,10-phenanthroline ligand containing tetrazole and their anticancer properties investigated by cytotoxicity in vitro, reactive oxygen species, apoptosis with annexin V/PI staining method, autophagy, and cell uptake.

Results: S1, S2, S3, S4, and S5 complexes showed comparable cytotoxicity activity relative to cisplatin against the B16F10 model. Moreover, intracellular ROS levels increased due to the presence of the complexes. Among the investigated complexes, the cells treated with the S5 complex indicated the highest apoptotic percentage (Q3) of 14.9% compared to the controls. The cell adsorption of the complexes also showed that the S4 and S5 complexes had higher cell adsorption, better internalization, and higher fluorescence light intensity.

Conclusions: The present work provides important guidance for designing and using Ru complexes in cancer therapy.

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