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血栓素抑制剂对微血管及肿瘤光动力治疗反应的影响。

The effects of thromboxane inhibitors on the microvascular and tumor response to photodynamic therapy.

作者信息

Fingar V H, Siegel K A, Wieman T J, Doak K W

机构信息

Department of Surgery, University of Louisville, KY 40292.

出版信息

Photochem Photobiol. 1993 Sep;58(3):393-9. doi: 10.1111/j.1751-1097.1993.tb09580.x.

DOI:10.1111/j.1751-1097.1993.tb09580.x
PMID:8234474
Abstract

Vascular stasis and tissue ischemia are known to cause tumor cell death in several experimental models after photodynamic therapy (PDT); however, the mechanisms leading to this damage remain unclear. Because previous studies indicated that thromboxane release is implicated in vessel damage, we further examined the role of thromboxane in PDT. Rats bearing chondrosarcoma were injected with 25 mg/kg Photofrin (intravenously) 24 h before treatment. Light (135 J/cm2, 630 nm) was delivered to the tumor area after injection of one of the following inhibitors: (1) R68070: a thromboxane synthetase inhibitor; (2) SQ-29548: a thromboxane receptor antagonist; and (3) Flunarizine: an inhibitor of platelet shape change. Systemic thromboxane levels were determined. Vessel constriction and leakage were evaluated by intravital microscopy. Tumor response was assessed after treatment. Thromboxane levels were decreased more than 50% with SQ-29548 as compared to controls. Thromboxane levels in animals given R68070 and Flunarizine remained at baseline levels. SQ-29548 and R68070 reduced vessel constriction compared to controls, while Flunarizine totally prevented vessel constriction. R68070 and SQ-29548 inhibited vessel permeability compared to PDT controls; Flunarizine did not. Animals given these inhibitors showed markedly reduced tumor cure. These results indicate that the release of thromboxane is linked to the vascular response in PDT.

摘要

在光动力疗法(PDT)后的多个实验模型中,已知血管淤滞和组织缺血会导致肿瘤细胞死亡;然而,导致这种损伤的机制仍不清楚。由于先前的研究表明血栓素释放与血管损伤有关,我们进一步研究了血栓素在PDT中的作用。在治疗前24小时,给荷软骨肉瘤的大鼠静脉注射25mg/kg的卟吩姆钠。在注射以下抑制剂之一后,将光(135J/cm²,630nm)照射到肿瘤区域:(1)R68070:一种血栓素合成酶抑制剂;(2)SQ - 29548:一种血栓素受体拮抗剂;(3)氟桂利嗪:一种血小板形状改变抑制剂。测定全身血栓素水平。通过活体显微镜评估血管收缩和渗漏。治疗后评估肿瘤反应。与对照组相比,SQ - 29548使血栓素水平降低超过50%。给予R68070和氟桂利嗪的动物的血栓素水平保持在基线水平。与对照组相比,SQ - 29548和R68070减少了血管收缩,而氟桂利嗪完全阻止了血管收缩。与PDT对照组相比,R68070和SQ - 29548抑制了血管通透性;氟桂利嗪没有。给予这些抑制剂的动物显示肿瘤治愈率明显降低。这些结果表明,血栓素的释放与PDT中的血管反应有关。

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