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对玻连蛋白受体(αvβ3)在人血小板和巨核细胞中分布的超微结构分析显示存在一个细胞内池以及α-颗粒膜的标记。

Ultrastructural analysis of the distribution of the vitronectin receptor (alpha v beta 3) in human platelets and megakaryocytes reveals an intracellular pool and labelling of the alpha-granule membrane.

作者信息

Poujol C, Nurden A T, Nurden P

机构信息

UMR 5533 CNRS, Hôpital Cardiologique, Pessac, France.

出版信息

Br J Haematol. 1997 Mar;96(4):823-35. doi: 10.1046/j.1365-2141.1997.d01-2109.x.

Abstract

The vitronectin receptor (VnR or alpha v beta 3) belongs to the cytoadhesin subclass of the integrin family. This subclass consists of two receptors which have the beta 3 subunit in common: GP IIb-IIIa complexes (or alpha IIb beta 3) and VnR. We report the subcellular distribution of VnR within human platelets as determined by immunogold staining of ultrathin frozen sections and transmission electron microscopy. Monoclonal antibodies directed against: (i) the alpha v subunit (LM142, AMF7, CLB-706), or (ii) an epitope specific to the complex (LM609) were used. Although VnR is present on platelets, it is a minor component. We therefore first compared several different staining procedures to detect this integrin. Optimal localization of VnR was obtained using a multistep procedure in which biotinylated anti-mouse IgG and a monoclonal anti-biotin antibody provided staining enhancement. Results showed that although present on the surface, alpha v beta 3 was mostly detected in internal membrane systems including those of alpha-granules. Occasionally, platelet sections showed special vesicular structures covered by gold particles. These were often localized at the edge or immediately under the plasma membrane and their origin remains unclear. An internal pool of alpha v beta 3 was confirmed by flow cytometry and by using platelets from a patient with type I Glanzmann's thrombasthenia arising from a GP IIb gene defect. We also investigated the presence of VnR in megakaryocytes (MK) obtained from normal human bone marrow. A fluorescence study showed VnR in small MK with unilobulated nuclei, suggesting that synthesis of this integrin occurs early during megakaryocytopoiesis. In mature cells, VnR expression had decreased relative to GP IIb-IIIa, although intracellular staining was present in EM and alpha-granules were again labelled.

摘要

玻连蛋白受体(VnR或αvβ3)属于整合素家族的细胞粘附分子亚类。该亚类由两个共用β3亚基的受体组成:糖蛋白IIb-IIIa复合物(或αIIbβ3)和VnR。我们通过超薄冷冻切片的免疫金染色和透射电子显微镜确定了人血小板内VnR的亚细胞分布。使用了针对:(i)αv亚基(LM142、AMF7、CLB-706),或(ii)复合物特异性表位(LM609)的单克隆抗体。尽管VnR存在于血小板上,但它是次要成分。因此,我们首先比较了几种不同的染色方法来检测这种整合素。使用多步骤方法获得了VnR的最佳定位,其中生物素化的抗小鼠IgG和单克隆抗生物素抗体增强了染色效果。结果表明,虽然αvβ3存在于表面,但大多在内膜系统中检测到,包括α颗粒的内膜系统。偶尔,血小板切片显示有被金颗粒覆盖的特殊囊泡结构。这些结构通常位于边缘或紧邻质膜下方,其来源尚不清楚。通过流式细胞术以及使用来自一名因GP IIb基因缺陷导致的I型血小板无力症患者的血小板,证实了αvβ3的内部池。我们还研究了从正常人骨髓获得的巨核细胞(MK)中VnR的存在情况。荧光研究显示,在具有单核叶的小巨核细胞中有VnR,这表明这种整合素的合成在巨核细胞生成早期就已发生。在成熟细胞中,相对于糖蛋白IIb-IIIa,VnR的表达有所下降,尽管在电子显微镜下存在细胞内染色,并且α颗粒再次被标记。

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