Inhibition of Survival Mechanisms and Cell Death Induction in Melanoma Following Photodynamic Therapy Mediated by Meso-5,10,15,20-tetrakis-(4-hydroxyphenyl)-porphyrin

被引:2
作者
Baldea, Ioana [1 ]
Danescu, Sorina [2 ]
Tabaran, Flaviu [3 ]
Filip, Adriana Gabriela [1 ]
Ion, Rodica Mariana [4 ]
Olteanu, Diana Elena [1 ]
Sevastre-Berghian, Alexandra Cristina [1 ]
Decea, Roxana Maria [1 ]
Iacovita, Cristian [5 ]
Hanganu, Daniela [6 ]
Cenariu, Mihai [7 ]
机构
[1] Iuliu Hatieganu Univ Med & Pharm, Dept Physiol, Clinicilor 1 3, Cluj Napoca 400012, Romania
[2] Iuliu Hatieganu Univ Med & Pharm, Dept Dermatol, Clinicilor 1 3, Cluj Napoca 400012, Romania
[3] Univ Agr Studies & Vet Med, Dept Morphopathol, Calea Manastur 3 5, Cluj Napoca 400658, Romania
[4] Natl Inst Res & Dev Chem & Petrochem ICECHIM, Nanomed Res Grp, 202 Splaiul Independentei, Bucharest 060024, Romania
[5] Iuliu Hatieganu Univ Med & Pharm, Fac Pharm, Dept Pharmaceut Phys Biophys, 6 Pasteur St, Cluj Napoca 400349, Romania
[6] Univ Med & Pharm Iuliu Hatieganu, Dept Pharmacognosy, 6 Pasteur St, Cluj Napoca 400349, Romania
[7] Univ Agr Sci & Vet Med, Dept Biochem, Calea Manastur 3 5, Cluj Napoca 400658, Romania
关键词
melanoma-endothelial cells co-culture; photodynamic therapy; mitochondrial apoptosis; angiogenesis; oxidative stress damage; inflammatory markers; DOWN-REGULATION; QUANTUM YIELDS; PHOTOSENSITIZERS; PIGMENTATION; ANGIOGENESIS; PORPHYRINS; ACTIVATION; APOPTOSIS; AUTOPHAGY;
D O I
10.3390/pr11030917
中图分类号
TQ [化学工业];
学科分类号
0817 ;
摘要
(1) Background: Photodynamic therapy (PDT) involves the selective killing of tumor cells by the generation of reactive oxygen species using a photosensitizer (PS) activated by irradiation. In melanoma, PDT efficiency is altered by several mechanisms, such as the presence of melanin and melanosomes and pro-survival pathways mediated by transcription factors such as: AP-1 (activator protein), MITF (microphthalmia inducible transcription factor), HIF1 alpha (hypoxia inducible factor), and NF-kB (nuclear factor kappa B). The study aimed to investigate the anti-melanoma effects of PDT mediated by meso-5,10,15,20-tetrakis-(4-hydroxyphenyl)-porphyrin (THPP) as a photosensitizer. (2) Methods: Cocultures of melanoma, two human, WM35 and M1-15, and murine B16-F10, with endothelial cells, were used. Cytotoxicity, oxidative damage, angiogenesis markers, and melanogenesis were assessed using colorimetry, flowcytometry, confocal microscopy, spectrophotometry, ELISA, and Western blotting. (3) Results: The maximal killing efficiency of PDT was reached in WM35, followed by M1-15, and then B16-F10, and it occurred through both apoptosis and necrosis. Although constitutive pigmentation diminished the PDT efficiency, de novo melanogenesis exhibited no protection. PDT increased TNF alpha, and inhibited NFkB, MITF, HIF1 alpha, and AP1, leading to inflammation and angiogenesis markers' inhibition. (4) Conclusions: THPP-mediated PDT efficiently induced cell death through apoptosis, necrosis, and the inhibition of pro-survival pathways mediated by NFkB, AP1, HIF1 alpha, and MITF in the melanoma coculture models.
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页数:23
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