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激活诱导的血小板表面受体表达变化以及大血小板亚群对激活的贡献。

Activation-induced changes in platelet surface receptor expression and the contribution of the large-platelet subpopulation to activation.

作者信息

Moroi Masaaki, Farndale Richard W, Jung Stephanie M

机构信息

Department of Biochemistry University of Cambridge Cambridge UK.

出版信息

Res Pract Thromb Haemost. 2020 Jan 27;4(2):285-297. doi: 10.1002/rth2.12303. eCollection 2020 Feb.

Abstract

OBJECTIVE

Platelet surface receptors are also present subcellularly in organelle membranes and can be expressed on the surface upon platelet activation. However, some receptors were reported to be decreased after activation. We analyzed the mechanism of activation-dependent expression for different receptors.

METHODS

Flow cytometry using platelet-rich plasma or washed platelets was used to analyze receptor-expression changes after platelet activation by glycoprotein (GP) VI-specific agonists, crosslinked collagen-related peptide (CRP-XL) and convulxin (Cvx), and thrombin. Platelets prelabeled with fluorescent antibody specific for a receptor were allowed to adhere on immobilized collagen or fibrinogen and post-stained with antibody against the same receptor labeled with another fluorophore, allowing us to differentiate preexisting receptors from newly expressed receptors.

RESULTS

Surface expression of αIIbβ3 increased in CRP-XL-, Cvx-, or thrombin-stimulated platelets, but GPIb decreased due to shedding and internalization. Both total and dimeric GPVI increased in thrombin-induced platelets, but decreased in platelets stimulated by Cvx, as a result of internalization. The larger platelets showed a greater increase in surface receptor (α2β1, αIIbβ3, GPVI, GPIb) expression upon activation compared to the smaller ones. Pre- and postlabeling with antibody specific for the same receptor, but conjugated with different fluorophores, allowed us to differentiate the receptors expressed on the surface of resting platelets from receptors newly exposed to the surface upon platelet activation.

CONCLUSIONS

Increased receptor expressions after activation are mainly manifested in the larger platelets. On platelets adhered on fibrinogen, the newly expressed receptors, especially GPVI, are localized in the lamellipodia of the spread platelets.

摘要

目的

血小板表面受体也存在于细胞器膜的亚细胞结构中,并且在血小板激活后可在表面表达。然而,有报道称一些受体在激活后会减少。我们分析了不同受体激活依赖性表达的机制。

方法

使用富含血小板血浆或洗涤后的血小板进行流式细胞术,以分析血小板被糖蛋白(GP)VI特异性激动剂、交联胶原相关肽(CRP-XL)、convulxin(Cvx)和凝血酶激活后受体表达的变化。用针对某一受体的荧光抗体预先标记的血小板,使其黏附于固定化的胶原或纤维蛋白原上,然后用标记有另一种荧光团的针对同一受体的抗体进行复染,这使我们能够区分预先存在的受体和新表达的受体。

结果

在CRP-XL、Cvx或凝血酶刺激的血小板中,αIIbβ3的表面表达增加,但由于脱落和内化,GPIb减少。在凝血酶诱导的血小板中,总GPVI和二聚体GPVI均增加,但在Cvx刺激的血小板中,由于内化作用而减少。与较小的血小板相比,较大的血小板在激活后表面受体(α2β1、αIIbβ3、GPVI、GPIb)表达的增加幅度更大。用针对同一受体但与不同荧光团偶联的抗体进行预标记和后标记,使我们能够区分静息血小板表面表达的受体和血小板激活后新暴露于表面的受体。

结论

激活后受体表达增加主要表现在较大的血小板中。在黏附于纤维蛋白原的血小板上,新表达的受体,尤其是GPVI,定位于铺展血小板的片状伪足中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f45b/7040538/321e25acbd0f/RTH2-4-285-g001.jpg

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