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携带纤维蛋白原γ链十二肽的磷脂囊泡在体外和体内的止血作用。

Hemostatic effects of phospholipid vesicles carrying fibrinogen gamma chain dodecapeptide in vitro and in vivo.

作者信息

Okamura Yosuke, Maekawa Ippei, Teramura Yuji, Maruyama Hitomi, Handa Makoto, Ikeda Yasuo, Takeoka Shinji

机构信息

Graduate School of Science and Engineering, Waseda University, Tokyo, 169-8555, Japan.

出版信息

Bioconjug Chem. 2005 Nov-Dec;16(6):1589-96. doi: 10.1021/bc050178g.

Abstract

We studied prototypes of platelet substitutes that bear on their surface a dodecapeptide, HHLGGAKQAGDV (H12). The peptide is a fibrinogen gamma chain carboxy-terminal sequence (gamma400-411) and recognizes specifically the active form of glycoprotein (GP) IIb/IIIa on the surface of activated platelets. We conjugated H12 to the end of poly(ethylene glycol) chains on the surface of a phospholipid vesicle with an average diameter of 220 nm to prepare H12-PEG-vesicles. The half-life of the H12-PEG-vesicles was significantly prolonged by PEG modification, and the ability of H12 on the surface of the vesicle to recognize GPIIb/IIIa was maintained even though the surface was modified with PEG chains. The H12-PEG-veiscles enhanced the in vitro thrombus formation of platelets that were adhering to a collagen-immobilized plate, when thrombocytopenia-imitation blood was passed over the plate. Based on the flow cytometric analyses of PAC-1 binding and P-selectin expression, the H12-PEG-vesicles were shown not to cause platelet activation. Furthermore, the H12-PEG-vesicles dose-dependently shortened the tail bleeding time of thrombocytopenic rats. It was confirmed that the H12-PEG-vesicles had a hemostatic effect and may be a suitable candidate for an alternative to human platelet concentrates transfused into thrombocytopenic patients.

摘要

我们研究了血小板替代物的原型,其表面带有一个十二肽,即HHLGGAKQAGDV(H12)。该肽是纤维蛋白原γ链的羧基末端序列(γ400 - 411),可特异性识别活化血小板表面糖蛋白(GP)IIb/IIIa的活性形式。我们将H12连接到平均直径为220 nm的磷脂囊泡表面的聚乙二醇链末端,以制备H12 - PEG - 囊泡。通过聚乙二醇修饰,H12 - PEG - 囊泡的半衰期显著延长,并且即使囊泡表面用聚乙二醇链修饰,囊泡表面的H12识别GPIIb/IIIa的能力仍得以保持。当模拟血小板减少的血液流过固定有胶原蛋白的平板时,H12 - PEG - 囊泡增强了黏附在该平板上的血小板的体外血栓形成。基于PAC - 1结合和P - 选择素表达的流式细胞术分析,结果表明H12 - PEG - 囊泡不会引起血小板活化。此外,H12 - PEG - 囊泡剂量依赖性地缩短了血小板减少大鼠的尾部出血时间。证实H12 - PEG - 囊泡具有止血作用,可能是输给血小板减少患者的人血小板浓缩物替代品的合适候选物。

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