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光动力疗法对内吞过程的抑制作用。

Inhibition of endocytic processes by photodynamic therapy.

作者信息

Kessel David

机构信息

Department of Pharmacology, Wayne State University School of Medicine, Detroit, Michigan 48201, USA.

出版信息

Lasers Surg Med. 2011 Sep;43(7):542-7. doi: 10.1002/lsm.21067.

DOI:10.1002/lsm.21067
PMID:22057481
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3211108/
Abstract

BACKGROUND AND OBJECTIVES

Recent studies have demonstrated an effect of photodamage on the endocytic pathway involved in recycling of membrane components. Using a series of agents with known sub-cellular targets, we explored the determinants of photodynamic inhibition of endocytic processes in three cell lines: A murine leukemia, a murine hepatoma, and a non-malignant epithelial cell line of human origin.

STUDY DESIGN/MATERIALS AND METHODS: The PI-3 kinase antagonist wortmannin blocks endosomal processing pathway dependent on this enzyme, providing an indication of the "flux" of endocytosis. Microscopic observations were used to assess the effect of photodamage on this pathway. Photosensitizing agents specific for mitochondrial, endoplasmic reticulum (ER), lysosomal, and endosomal photodamage were employed.

RESULTS

Sub-lethal photodamage directed against endosomes or lysosomes interrupted early steps in this endocytic process in the hepatoma cell line. A mechanism for these effects is proposed. Mitochondrial photodamage could interrupt endocytosis, but at levels that also induced apoptosis. ER photodamage did not affect endocytosis even at lethal levels. Somewhat similar results were obtained with other cell lines, but there were sufficient differences to indicate that the cell phenotype is, in part, a determinant of the endocytic response to PDT.

CONCLUSIONS

PDT is therefore seen to have an effect on endocytic processes. Further work will be needed to delineate the role of these endocytic effects in the array of responses to photodynamic therapy.

摘要

背景与目的

近期研究已证实光损伤对参与膜成分循环利用的内吞途径有影响。我们使用一系列具有已知亚细胞靶点的试剂,在三种细胞系中探究了光动力抑制内吞过程的决定因素,这三种细胞系分别为:一种小鼠白血病细胞系、一种小鼠肝癌细胞系以及一种人源非恶性上皮细胞系。

研究设计/材料与方法:PI-3激酶拮抗剂渥曼青霉素可阻断依赖该酶的内体加工途径,从而指示内吞作用的“通量”。通过显微镜观察来评估光损伤对该途径的影响。使用了对线粒体、内质网(ER)、溶酶体和内体具有光损伤特异性的光敏剂。

结果

针对内体或溶酶体的亚致死性光损伤会中断肝癌细胞系中该内吞过程的早期步骤。本文提出了这些效应的一种机制。线粒体光损伤可中断内吞作用,但程度上也会诱导细胞凋亡。即使在致死水平,内质网光损伤也不影响内吞作用。在其他细胞系中也获得了 somewhat similar 结果,但存在足够差异表明细胞表型部分决定了对光动力疗法的内吞反应。

结论

因此可见光动力疗法对内吞过程有影响。需要进一步开展工作来阐明这些内吞效应在光动力疗法一系列反应中的作用。