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改变辅助配体的 5-(2-吡嗪基)四唑基双钌(II)配合物的光化学性质用于癌症光疗。

Photochemical property of two Ru(II) compounds based on 5-(2-pyrazinyl)tetrazole for cancer phototherapy by changing auxiliary ligand.

机构信息

Jiangsu Laboratory of Advanced Functional Material, Department of Chemistry and Material Engineering, Changshu Institute of Technology, Changshu 215500, Jiangsu, PR China.

School of Pharmacy, Guilin Medical University, Guilin 541004, Guangxi, PR China.

出版信息

J Inorg Biochem. 2019 Apr;193:124-129. doi: 10.1016/j.jinorgbio.2019.01.015. Epub 2019 Jan 28.

DOI:10.1016/j.jinorgbio.2019.01.015
PMID:30711558
Abstract

Ru(II) compounds are potential candidates for photodynamic therapy (PDT) and auxiliary ligands may have an impact on the property of the resulting coordination compounds. In the present study, two Ru(II) compounds based on 5-(2-pyrazinyl)tetrazole (Hpztz) and two classic auxiliary ligands, 2,2'-bipyridine (bipy) or 1,10-phenanthroline (phen) have been prepared and characterized, namely [Ru(pztz)(bipy)][PF] (1) and [Ru(pztz)(phen)][PF] (2). The nanoparticles (NPs) of the two compounds have been prepared by self-assembly in aqueous solution. In vitro MTT assay on HeLa cells show that [Ru(pztz)(phen)][PF] with a lower IC (half-maximal inhibitory concentration) of only 7.4 μg/mL is superior to that of [Ru(pztz)(bipy)][PF] (17.8 μg/mL) under irradiation. Meanwhile, negligible dark toxicity have been also observed for the two compounds. In addition, in vivo fluorescence imaging suggests that [Ru(pztz)(phen)][PF] NPs are able to target to the tumor by enhanced permeability and retention effect (EPR). Furthermore, in vivo phototherapy on nude mice demonstrate that such NPs can effectively inhibit the growth of the tumor. After treatment for 10 cycles, an obvious decrease in the tumor volume can be observed while the normal tissues, including heart, liver, spleen, lung and kidney, suffer from no damage, indicating the high phototoxicity, low dark toxicity and excellent biocompatibility of [Ru(pztz)(phen)][PF] NPs.

摘要

钌(II)化合物是光动力疗法(PDT)的潜在候选物,辅助配体可能会对所得配合物的性质产生影响。在本研究中,制备并表征了基于 5-(2-吡嗪基)四唑(Hpztz)和两个经典辅助配体,即 2,2'-联吡啶(bipy)或 1,10-菲啰啉(phen)的两种 Ru(II)化合物,即 [Ru(pztz)(bipy)][PF](1)和 [Ru(pztz)(phen)][PF](2)。通过在水溶液中自组装制备了两种化合物的纳米颗粒(NPs)。在 HeLa 细胞中的体外 MTT 测定表明,在光照下,具有低 IC(半最大抑制浓度)仅为 7.4μg/mL 的 [Ru(pztz)(phen)][PF] 优于 [Ru(pztz)(bipy)][PF](17.8μg/mL)。同时,两种化合物也观察到几乎没有暗毒性。此外,体内荧光成像表明,[Ru(pztz)(phen)][PF] NPs 能够通过增强的通透性和保留效应(EPR)靶向肿瘤。此外,裸鼠体内光疗表明,这些 NPs 能够有效抑制肿瘤的生长。经过 10 个周期的治疗后,可以观察到肿瘤体积明显减小,而包括心脏、肝脏、脾脏、肺和肾脏在内的正常组织没有受到损伤,表明 [Ru(pztz)(phen)][PF] NPs 具有高光毒性、低暗毒性和良好的生物相容性。

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