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药物-光照间隔对光卟啉光动力疗法在小鼠肿瘤模型中作用模式的影响。

Effect of drug-light interval on the mode of action of Photofrin photodynamic therapy in a mouse tumor model.

作者信息

Li Li-Bo, Luo Rong-Cheng

机构信息

Department of Oncology, Nanfang Hospital, Southern Medical University, Guangzhou, PR China.

出版信息

Lasers Med Sci. 2009 Jul;24(4):597-603. doi: 10.1007/s10103-008-0620-9. Epub 2008 Oct 21.

Abstract

Our objective was to examine the effect of time intervals between Photofrin injection and laser irradiation [i.e., drug-light interval (DLI)] on the mode of action of Photofrin photodynamic therapy (PDT). Kunming mice transplanted with sarcoma-180 cells were used as an animal model. The tumor-bearing mice in the control group were given neither photosensitizer nor laser irradiation. PDT groups were given intravenous (i.v.) injection of Photofrin (7.5 mg/kg) prior to being irradiated with a 630 nm laser at 120 J/cm(2) at different DLIs (1 min-48 h). Tumors and overlying skin were visually examined daily. Histopathological and electron microscopic examinations were carried out 48 h after PDT. Survival rates were recorded. The mice in the groups that had experienced short DLIs (<60 min) showed stronger skin reactions than the groups subjected to long DLIs (>6 h). Histological examination showed that antitumor effects were achieved mainly by the destruction of tumor blood vessels and the formation of thrombosis at short DLIs, whereas, at long DLIs, the tumor cells were killed directly by PDT-mediated cytotoxicity. Electron microscopy revealed various degrees of mitochondrial swelling. The survival rate of the mice subjected to long DLIs was slightly higher than that of the mice subjected to short DLIs. Both vascular (e.g., tumor vessel destruction) and cellular (e.g., cytotoxicity) effects contributed to Photofrin PDT-induced tumor ablation.

摘要

我们的目的是研究卟啉钠注射与激光照射之间的时间间隔[即药物 - 光间隔(DLI)]对卟啉钠光动力疗法(PDT)作用模式的影响。将移植有肉瘤 - 180细胞的昆明小鼠用作动物模型。对照组的荷瘤小鼠既未给予光敏剂也未给予激光照射。PDT组在以不同的DLI(1分钟至48小时)接受120 J/cm²的630 nm激光照射之前,静脉内(i.v.)注射卟啉钠(7.5 mg/kg)。每天对肿瘤及覆盖的皮肤进行肉眼检查。在PDT后48小时进行组织病理学和电子显微镜检查。记录生存率。经历短DLI(<60分钟)的组中的小鼠比经历长DLI(>6小时)的组表现出更强的皮肤反应。组织学检查表明,在短DLI时,抗肿瘤作用主要通过肿瘤血管的破坏和血栓形成来实现,而在长DLI时,肿瘤细胞通过PDT介导的细胞毒性被直接杀死。电子显微镜显示线粒体有不同程度的肿胀。经历长DLI的小鼠的生存率略高于经历短DLI的小鼠。血管(例如肿瘤血管破坏)和细胞(例如细胞毒性)效应均有助于卟啉钠PDT诱导的肿瘤消融。

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