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含外围钯(II)-联吡啶配合物的四价阳离子卟啉的光照射及其对纯化的DNA分子、成纤维细胞和黑色素瘤细胞系的诱导效应。

Light exposure of tetra-cationic porphyrins containing peripheral Pd(II)-bipyridyl complexes and the induced effects on purified DNA molecule, fibroblast and melanoma cell lines.

作者信息

Trentin Luana B, Viana Altevir R, Iwersen Sophia, Iglesias Bernardo A, Chaves Otávio A, Schuch André P

机构信息

Laboratory of Photobiology, Department of Biochemistry and Molecular Biology, Federal University of Santa Maria - UFSM, Santa Maria, RS, Brazil.

Laboratory of Bioinorganic and Porphyrinoid Materials, Department of Chemistry, Federal University of Santa Maria - UFSM, Santa Maria, RS, Brazil.

出版信息

Photochem Photobiol. 2025 May-Jun;101(3):565-579. doi: 10.1111/php.14017. Epub 2024 Aug 27.

DOI:10.1111/php.14017
PMID:39189637
Abstract

Photodynamic therapy (PDT) combines a light source, oxygen, and a photosensitizer (PS) to generate reactive oxygen species (ROS) for treating diseases. In this study, we evaluated two meso-tetra-pyridyl porphyrins with [Pd(bpy)Cl], namely 3-PdTPyP and 4-PdTPyP, as PS for PDT application. DNA interaction was assessed by spectroscopic measurements (UV-Vis and fluorescence emission), viscosity analysis, and molecular docking simulations. The results indicate that Pd(II)-porphyrins do not intercalate into DNA, suggesting that the minor groove is the primary interaction site, mainly through van der Waals forces. These metalloporphyrins effectively induced nitrogenous bases oxidation, particularly in purines, after white light irradiation. The induced DNA lesions were able to inactivate plasmid DNA metabolism (DNA replication and transcription) in a bacterial model. 3-PdTPyP and 4-PdTPyP significantly decreased the viability of treated melanoma cell lines (A375 and B16-F10), demonstrating that melanoma cell lines were more sensitive to these Pd(II)-porphyrins than the fibroblast cell line (L929). Moreover, 3-PdTPyP was more photototoxic to A375 cells (IC50 = 0.43 μM), whereas 4-PdTPyP was more photototoxic to B16-F10 cells (IC50 = 0.51 μM). These findings suggest that these porphyrins are promising PS for future PDT research focused on skin cancer.

摘要

光动力疗法(PDT)结合光源、氧气和光敏剂(PS)以产生活性氧(ROS)来治疗疾病。在本研究中,我们评估了两种带有[Pd(bpy)Cl]的中位四吡啶基卟啉,即3-PdTPyP和4-PdTPyP,作为用于PDT应用的PS。通过光谱测量(紫外-可见光谱和荧光发射)、粘度分析和分子对接模拟来评估DNA相互作用。结果表明,Pd(II)-卟啉不会插入DNA,这表明小沟是主要的相互作用位点,主要通过范德华力。这些金属卟啉在白光照射后能有效诱导含氮碱基氧化,尤其是嘌呤。诱导的DNA损伤能够在细菌模型中使质粒DNA代谢(DNA复制和转录)失活。3-PdTPyP和4-PdTPyP显著降低了处理过的黑色素瘤细胞系(A375和B16-F10)的活力,表明黑色素瘤细胞对比成纤维细胞系(L929)对这些Pd(II)-卟啉更敏感。此外,3-PdTPyP对A375细胞的光毒性更强(IC50 = 0.43 μM),而4-PdTPyP对B16-F10细胞的光毒性更强(IC50 = 0.51 μM)。这些发现表明,这些卟啉是未来针对皮肤癌的PDT研究中有前景的PS。

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