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Vascular regrowth following photodynamic therapy in the chicken embryo chorioallantoic membrane

机译:鸡胚绒膜尿囊膜光动力治疗后的血管再生

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摘要

Photodynamic therapy (PDT) induces damage to the endothelium, which can lead to increased vascular permeability and, under intensive PDT conditions, even to platelet aggregation, vasoconstriction, and blood flow stasis. Eventually, ischemia, hypoxia, and inflammation can occur, resulting in angiogenesis. We studied the sequence of the vascular events after Visudyne®-PDT in the chicken chorioallantoic membrane (CAM) at day 11 of development. Using epi-fluorescence microscopy, we monitored the regrowth of capillaries in the PDT treated area. Immediately after irradiation, the treatment resulted in blood flow arrest. And 24 h post PDT, sprouting of new blood vessels was observed at the edge of the PDT zone. Neovessels looping out from the edge of the PDT zone gave rise to specialized endothelial tip structures guiding the vessels towards the center of the treated area. At 48 h almost all of the treated area was repopulated with functional but morphologically altered vasculature. These observations also showed reperfusion of some of the vessels that had been closed by the PDT treatment. CAM samples were immunohistochemically stained for Ki-67 showing proliferation of endothelial cells in the PDT area. Also, several markers of immature and angiogenic blood vessels, such as αVβ3-integrin, vimentin and galectin-1, were found to be enhanced in the PDT area, while the endothelial maturation marker intercellular adhesion molecule (ICAM)-1 was found to be suppressed. These results demonstrate that the new vascular bed is formed by both neo-angiogenesis and reperfusion of existing vessels. Both the quantitative real-time RT–PCR profile and the response to pharmacological treatment with Avastin®, an inhibitor of angiogenesis, suggest that angiogenesis occurs after PDT. The observed molecular profiling results and the kinetics of gene regulation may enable optimizing combination therapies involving PDT for treatment of cancer and other diseases.
机译:光动力疗法(PDT)会诱导内皮损伤,从而导致血管通透性增加,在强力PDT条件下,甚至会导致血小板聚集,血管收缩和血流淤滞。最终,可能发生局部缺血,缺氧和炎症,从而导致血管生成。在发育的第11天,我们研究了Visudyne ® -PDT在鸡绒膜尿囊膜(CAM)中的血管事件的顺序。使用落射荧光显微镜,我们监测了PDT治疗区域中毛细血管的再生。照射后,治疗立即导致血流停止。 PDT后24小时,在PDT区域的边缘观察到新血管的萌芽。新血管从PDT区边缘环出,形成专门的内皮尖端结构,将血管导向治疗区域的中心。在48小时时,几乎所有治疗区域都重新填充了功能正常但形态已改变的脉管系统。这些观察结果还显示了通过PDT处理已关闭的一些血管的再灌注。对CAM样品进行Ki-67免疫组织化学染色,显示PDT区内皮细胞增殖。此外,发现PDT区域增强了一些未成熟和血管生成的标记,例如αVβ3-整联蛋白,波形蛋白和半乳凝素-1,而发现内皮成熟标记的细胞间粘附分子(ICAM)-1压抑。这些结果表明,新血管床是由新血管生成和现有血管的再灌注形成的。实时定量RT-PCR谱以及血管生成抑制剂Avastin ®对药物治疗的反应均表明,PDT后发生血管生成。观察到的分子谱分析结果和基因调控动力学可以使涉及PDT的组合疗法优化用于癌症和其他疾病的治疗。

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