人血小板摄取抗血管内皮生长因子(VEGF)药物。
Human Platelets Take up Anti-VEGF Agents.
作者信息
Sobolewska B, Fehrenbacher B, Münzer P, Kalbacher H, Geue S, Stellos Konstantinos, Schaller M, Ziemssen F
机构信息
Center for Ophthalmology, Eberhard Karls University Tuebingen, Tuebingen, Germany.
Department of Dermatology, Eberhard Karls University Tuebingen, Tuebingen, Germany.
出版信息
J Ophthalmol. 2021 Jun 14;2021:8811672. doi: 10.1155/2021/8811672. eCollection 2021.
PURPOSE
Growing evidence suggests different systemic exposure of anti-vascular endothelial growth factor (anti-VEGF) agents with repeated intravitreal application. Since the penetration of anti-VEGF agents through vascular barrier was reported, the interaction of anti-VEGF with nonresident platelets has become a topic of interest. The purpose of this study was to evaluate, with the help of visualization techniques, whether platelets take up the anti-VEGF agents ranibizumab, aflibercept, and bevacizumab.
METHODS
The uptake of anti-VEGF agents with or without VEGF treatment was investigated using immunofluorescence and immunogold staining in human platelets. The role of actin filaments and clathrin-coated vesicles in the transport of ranibizumab, aflibercept, and bevacizumab was evaluated by two pharmacologic inhibitors: staurosporine (protein kinase C inhibitor) and cytochalasin D.
RESULTS
All three anti-VEGF agents were taken up by platelets and colocalized with VEGF. Ranibizumab and aflibercept were mainly detected in alpha-granules; however, bevacizumab was equally localized in alpha-granules and in platelet vesicles. Both staurosporine and cytochalasin D completely inhibited the uptake of aflibercept into platelets. Both pharmacological inhibitors also decreased the transport of ranibizumab and bevacizumab into platelets. Bevacizumab was significantly more frequently colocalized within clathrin-coated vesicles than ranibizumab and aflibercept.
CONCLUSION
All three anti-VEGF agents are taken up by platelets and internalized in alpha-granules, which may result in a higher local exposure of anti-VEGF after the activation of platelets, potentially contributing to arterial thromboembolic events. Clathrin-coated vesicles seem to be more prominent in the transport of bevacizumab than ranibizumab and aflibercept. Nevertheless, whether the different localization and transport of bevacizumab are truly related to specific differences of receptor-mediated endocytosis has to be revealed by further research.
目的
越来越多的证据表明,重复玻璃体内注射抗血管内皮生长因子(抗VEGF)药物会导致不同的全身暴露情况。自从有报道称抗VEGF药物可穿透血管屏障以来,抗VEGF与非驻留血小板的相互作用已成为一个备受关注的话题。本研究的目的是借助可视化技术评估血小板是否摄取抗VEGF药物雷珠单抗、阿柏西普和贝伐单抗。
方法
使用免疫荧光和免疫金染色法在人血小板中研究有无VEGF处理时抗VEGF药物的摄取情况。通过两种药理抑制剂:星形孢菌素(蛋白激酶C抑制剂)和细胞松弛素D,评估肌动蛋白丝和网格蛋白包被小泡在雷珠单抗、阿柏西普和贝伐单抗转运中的作用。
结果
所有三种抗VEGF药物均被血小板摄取并与VEGF共定位。雷珠单抗和阿柏西普主要在α颗粒中检测到;然而,贝伐单抗在α颗粒和血小板小泡中的定位相同。星形孢菌素和细胞松弛素D均完全抑制阿柏西普进入血小板。这两种药理抑制剂也降低了雷珠单抗和贝伐单抗进入血小板的转运。贝伐单抗与网格蛋白包被小泡共定位的频率明显高于雷珠单抗和阿柏西普。
结论
所有三种抗VEGF药物均被血小板摄取并内化于α颗粒中,这可能导致血小板激活后抗VEGF的局部暴露增加,可能促成动脉血栓栓塞事件。网格蛋白包被小泡在贝伐单抗的转运中似乎比雷珠单抗和阿柏西普更突出。然而,贝伐单抗不同的定位和转运是否真的与受体介导的内吞作用的特定差异有关,还有待进一步研究揭示。
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