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α-颗粒膜与血小板质膜相似,且含有糖蛋白Ib、IX和V。

Alpha-granule membrane mirrors the platelet plasma membrane and contains the glycoproteins Ib, IX, and V.

作者信息

Berger G, Massé J M, Cramer E M

机构信息

INSERM U91, Hôpital Henri Mondor, Créteil, France.

出版信息

Blood. 1996 Feb 15;87(4):1385-95.

PMID:8608228
Abstract

We have recently shown that several components from the platelet plasma membrane were also present at different rates in the alpha-granule membrane. This is the case for the glycoprotein (GP) IIb-IIIa (CD41), CD36, CD9, PECAM1, and Rap1b, while the GPIB-IX-V complex was considered to escape the rule. In this investigation, we studied the subcellular localization of GPIb, GPIX, and GPV in the resting platelets of normal subjects, patients with Bernard-Soulier syndrome, patients with Gray platelet syndrome, and human cultured megakaryocytes. Ultra-thin sections of the cells were labeled with antibodies directed against glycocalicin, GPIb, GPIX, and GPV. We have shown that a significant and reproducible labeling for the three GPs was associated with the alpha-granule membrane, accounting for approximately 10% of the total labeling. Furthermore, GPIb labeling appears Willebrand factor (vWF). After thrombin activation, vWF remained close to the limiting membrane of the open canalicular system (OCS), suggesting an early association of both receptor and ligand. Plasma membrane and alpha-granule labeling was virtually absent from the Bernard-Soulier platelets (characterized by a GPIb deficiency), thus proving the specificity of the reaction. In Gray platelets (storage granule deficiency syndrome), the small residual alpha-granules were also occasionally labeled for GPIb, GPIX, and GPIX. Cultured megakaryocytes that displayed the classical GPIb distribution, eg, demarcation and plasma membranes, exhibited also a discrete labeling associated to the alpha-granules. In conclusion, this study shows that, evenly for these three GPs, the alpha-granule membrane mirrors the plasma membrane composition. This might occur through an endocytotic process affecting each plasma membrane protein to a different extent and could have a physiologic relevance in further presentation of a receptor bound to its alpha-granule ligand to the platelet surface.

摘要

我们最近发现,血小板质膜的几种成分在α-颗粒膜中也以不同比例存在。糖蛋白(GP)IIb-IIIa(CD41)、CD36、CD9、PECAM1和Rap1b就是这种情况,而GPIB-IX-V复合物则被认为是个例外。在本研究中,我们研究了正常受试者、伯纳德-索利尔综合征患者、灰色血小板综合征患者以及人培养巨核细胞静息血小板中GPIb、GPIX和GPV的亚细胞定位。用针对糖钙蛋白、GPIb、GPIX和GPV的抗体标记细胞的超薄切片。我们发现,这三种糖蛋白的显著且可重复的标记与α-颗粒膜相关,约占总标记的10%。此外,GPIb标记似乎与血管性血友病因子(vWF)有关。凝血酶激活后,vWF仍靠近开放管道系统(OCS)的限制膜,这表明受体和配体之间存在早期关联。伯纳德-索利尔血小板(其特征为GPIb缺乏)几乎没有质膜和α-颗粒标记,从而证明了反应的特异性。在灰色血小板(储存颗粒缺乏综合征)中,少量残留α-颗粒偶尔也会被GPIb、GPIX和GPIX标记。显示出经典GPIb分布(如分界膜和质膜)的培养巨核细胞,其α-颗粒也有离散标记。总之,本研究表明,即使对于这三种糖蛋白,α-颗粒膜也反映了质膜的组成。这可能是通过一种内吞过程发生的,该过程对每种质膜蛋白的影响程度不同,并且在将与α-颗粒配体结合的受体进一步呈递给血小板表面方面可能具有生理相关性。

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