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溶酶体信号增强 A431 癌细胞中线粒体介导的光动力疗法:铁的作用。

Lysosomal signaling enhances mitochondria-mediated photodynamic therapy in A431 cancer cells: role of iron.

机构信息

Department of Pharmaceutical and Biomedical Sciences, Center for Cell Death, Injury and Regeneration, Medical University of South Carolina, Charleston, SC, USA.

出版信息

Photochem Photobiol. 2012 Mar-Apr;88(2):461-8. doi: 10.1111/j.1751-1097.2012.01081.x. Epub 2012 Jan 25.

Abstract

In photodynamic therapy (PDT), light activates a photosensitizer added to a tissue, resulting in singlet oxygen formation and cell death. The photosensitizer phthalocyanine 4 (Pc 4) localizes primarily to mitochondrial membranes in cancer cells, resulting in mitochondria-mediated cell death. The aim of this study was to determine how lysosomes contribute to PDT-induced cell killing by mitochondria-targeted photosensitizers such as Pc 4. We monitored cell killing of A431 cells after Pc 4-PDT in the presence and absence of bafilomycin, an inhibitor of the vacuolar proton pump of lysosomes and endosomes. Bafilomycin was not toxic by itself, but greatly enhanced Pc 4-PDT-induced cell killing. To investigate whether iron loading of lysosomes affects bafilomycin-induced killing, cells were incubated with ammonium ferric citrate (30 μM) for 30 h prior to PDT. Ammonium ferric citrate enhanced Pc 4 plus bafilomycin-induced cell killing without having toxicity by itself. Iron chelators (desferrioxamine and starch-desferrioxamine) and the inhibitor of the mitochondrial calcium (and ferrous iron) uniporter, Ru360, protected against Pc 4 plus bafilomycin toxicity. These results support the conclusion that chelatable iron stored in the lysosomes enhances the efficacy of bafilomycin-mediated PDT and that lysosomal disruption augments PDT with Pc 4.

摘要

在光动力疗法(PDT)中,光会激活添加到组织中的光敏剂,导致单线态氧的形成和细胞死亡。光敏剂酞菁 4(Pc 4)主要定位于癌细胞的线粒体膜,导致线粒体介导的细胞死亡。本研究旨在确定溶酶体如何通过靶向线粒体的光敏剂如 Pc 4 促进 PDT 诱导的细胞杀伤。我们在存在和不存在巴弗洛霉素的情况下监测 A431 细胞在用 Pc 4-PDT 处理后的细胞杀伤情况,巴弗洛霉素是溶酶体和内体的液泡质子泵的抑制剂。巴弗洛霉素本身没有毒性,但大大增强了 Pc 4-PDT 诱导的细胞杀伤。为了研究溶酶体中铁的负载是否影响巴弗洛霉素诱导的杀伤,在用 Pc 4 进行 PDT 之前,将细胞用柠檬酸铁铵(30 μM)孵育 30 h。柠檬酸铁铵增强了 Pc 4 加巴弗洛霉素诱导的细胞杀伤,而本身没有毒性。铁螯合剂(去铁胺和淀粉去铁胺)和线粒体钙(和亚铁)单向转运体抑制剂 Ru360 可防止 Pc 4 加巴弗洛霉素的毒性。这些结果支持这样的结论,即溶酶体中储存的可螯合铁增强了巴弗洛霉素介导的 PDT 的功效,并且溶酶体破坏增强了用 Pc 4 进行的 PDT。

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