蜱源强效αIIbβ3整合素抑制剂对血小板黏附、血栓形成和纤维蛋白形成的抑制作用
Inhibition of platelet adhesion, thrombus formation, and fibrin formation by a potent αIIbβ3 integrin inhibitor from ticks.
作者信息
van den Kerkhof Danique L, Nagy Magdolna, Wichapong Kanin, Brouns Sanne L N, Heemskerk Johan W M, Hackeng Tilman M, Dijkgraaf Ingrid
机构信息
Department of Biochemistry Cardiovascular Research Institute Maastricht (CARIM) Maastricht University Maastricht The Netherlands.
出版信息
Res Pract Thromb Haemost. 2020 Dec 18;5(1):231-242. doi: 10.1002/rth2.12466. eCollection 2021 Jan.
BACKGROUND
Ticks puncture the skin of their hosts and secrete saliva, containing antiplatelet proteins, into the blood. Here, we studied disagregin, a potent platelet-inhibiting protein derived from the salivary glands of , an African soft tick. Whereas conventional αIIbβ3 antagonists contain an Arg-Gly-Asp (RGD) sequence for platelet integrin binding, disagregin contains an Arg-Glu-Asp (RED) sequence, hypothesizing a different mode of inhibitory action.
OBJECTIVES
We aimed to compare the inhibitory effects of disagregin and its RGD variant (RGD-disagregin) on platelet activation and to unravel the molecular basis of disagregin-αIIbβ3 integrin interactions.
METHODS
Disagregin and RGD-disagregin were synthesized by tert-butyloxycarbonyl -based solid-phase peptide synthesis. Effects of both disagregins on platelet aggregation were assessed by light transmission aggregometry in human platelet-rich plasma. Whole-blood thrombus formation was investigated by perfusing blood over collagen I with and without tissue factor at a high wall-shear rate (1000 s) in the presence of disagregin, RGD-disagregin, or eptifibatide.
RESULTS
Disagregin showed inhibition of collagen- and ADP-induced platelet aggregation with half maximal inhibitory concentration values of 64 and 99 nM, respectively. This resembled the complete antiaggregatory effect of eptifibatide. Multiparameter assessment of thrombus formation showed highly suppressed platelet adhesion and aggregate formation with both disagregins, in contrast to eptifibatide treatment, which incompletely blocked aggregation under flow. Fibrin formation under flow was delayed by both disagregin and RGD-disagregin ( < .01) and eptifibatide ( < .05).
CONCLUSIONS
Both αIIbβ3-blocking disagregins have a strong potential to suppress collagen-tissue factor-mediated platelet adhesion, thrombus formation, and fibrin formation. Both disagregins can be seen as potential new αIIbβ3 inhibitors.
背景
蜱虫会刺破宿主皮肤,并将含有抗血小板蛋白的唾液分泌到血液中。在此,我们研究了去整合素,一种源自非洲软蜱唾液腺的强效血小板抑制蛋白。传统的αIIbβ3拮抗剂含有用于血小板整合素结合的精氨酸 - 甘氨酸 - 天冬氨酸(Arg - Gly - Asp,RGD)序列,而去整合素含有精氨酸 - 谷氨酸 - 天冬氨酸(Arg - Glu - Asp,RED)序列,推测其具有不同的抑制作用模式。
目的
我们旨在比较去整合素及其RGD变体(RGD - 去整合素)对血小板活化的抑制作用,并阐明去整合素与αIIbβ3整合素相互作用的分子基础。
方法
通过基于叔丁氧羰基的固相肽合成法合成去整合素和RGD - 去整合素。在富含人血小板的血浆中,通过光透射聚集法评估两种去整合素对血小板聚集的影响。在高壁剪切率(1000 s⁻¹)下,在有或无组织因子的情况下,将血液灌注在I型胶原上,研究全血血栓形成,同时加入去整合素、RGD - 去整合素或依替巴肽。
结果
去整合素对胶原和ADP诱导的血小板聚集均有抑制作用,其半数最大抑制浓度值分别为64 nM和99 nM。这类似于依替巴肽的完全抗聚集作用。血栓形成的多参数评估显示,与依替巴肽处理相比,两种去整合素均能高度抑制血小板黏附和聚集体形成,依替巴肽在流动状态下不能完全阻断聚集。去整合素、RGD - 去整合素(P < 0.01)和依替巴肽(P < 0.05)均可延迟流动状态下的纤维蛋白形成。
结论
两种αIIbβ3阻断性去整合素均具有强大潜力,可抑制胶原 - 组织因子介导的血小板黏附、血栓形成和纤维蛋白形成。两种去整合素均可被视为潜在的新型αIIbβ3抑制剂。
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