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血小板糖蛋白Ib参与血小板微粒介导的中性粒细胞活化。

Involvement of platelet glycoprotein Ib in platelet microparticle mediated neutrophil activation.

作者信息

Lo Shyh-Chyi, Hung Ching-Yu, Lin Dong-Tsamn, Peng Hui-Chin, Huang Tur-Fu

机构信息

Department of Pharmacology, College of Medicine, National Taiwan University, No. 1, Jen-Ai Rd., Sec. 1, Taipei, Taiwan.

出版信息

J Biomed Sci. 2006 Nov;13(6):787-96. doi: 10.1007/s11373-006-9107-5. Epub 2006 Aug 9.

DOI:10.1007/s11373-006-9107-5
PMID:16897582
Abstract

Platelet microparticles (MPs) are membrane vesicles shed by platelets after activation, and carry antigens characteristic of intact platelets, such as glycoprotein (GP) IIb/IIIa, GPIb and P-selectin. Elevated platelet MPs have been observed in many disorders in which platelet activation is documented. Recently, platelet GPIb has been implicated in the mediation of platelet-leukocyte interaction via binding to its ligand Mac-1 on leukocyte. The role of GPIb for mediating adhesion-activation interactions between platelet MPs and leukocytes has not been clarified. In this study we investigate the role of GPIb in the interplay between platelet MPs and neutrophils. Platelet MPs were obtained from collagen-stimulated platelet-rich plasma (PRP). In a study model of neutrophil aggregation, platelet MPs can serve a bridge to support neutrophil aggregation under venous level shear stress, suggesting that platelet MPs may enhance leukocyte aggregation, which would bear clinical relevance in diseases where the platelet MPs are elevated. The level of aggregation can be reduced by GPIb blocking antibodies, AP1 and SZ2, but not by anti-CD18 mAb. The GPIb blocking antibodies also decreased platelet MP-mediated neutrophil activation, including beta2 integrin expression, adherence-dependent superoxide release and platelet MP-mediated neutrophil adherence to immobilized fibrinogen. Our data provide the evidence for the involvement of GPIb-Mac-1 interaction in the cross-talk between platelet MPs and neutrophils.

摘要

血小板微粒(MPs)是血小板激活后脱落的膜囊泡,携带完整血小板的特征性抗原,如糖蛋白(GP)IIb/IIIa、GPIb和P-选择素。在许多有血小板激活记录的疾病中都观察到血小板微粒升高。最近,血小板GPIb通过与白细胞上的配体Mac-1结合,参与介导血小板-白细胞相互作用。GPIb在介导血小板微粒与白细胞之间的黏附-激活相互作用中的作用尚未阐明。在本研究中,我们调查了GPIb在血小板微粒与中性粒细胞相互作用中的作用。血小板微粒从胶原刺激的富血小板血浆(PRP)中获得。在中性粒细胞聚集的研究模型中,血小板微粒可作为桥梁,在静脉水平剪切应力下支持中性粒细胞聚集,这表明血小板微粒可能增强白细胞聚集,这在血小板微粒升高的疾病中具有临床相关性。聚集水平可被GPIb阻断抗体AP1和SZ2降低,但不能被抗CD18单克隆抗体降低。GPIb阻断抗体还可降低血小板微粒介导的中性粒细胞激活,包括β2整合素表达、黏附依赖性超氧化物释放以及血小板微粒介导的中性粒细胞与固定化纤维蛋白原的黏附。我们的数据为GPIb-Mac-1相互作用参与血小板微粒与中性粒细胞之间的相互作用提供了证据。

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