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血小板Fc和补体受体与涉及AB0系统的循环免疫复合物的相互作用。

Interaction of platelet fc and complement receptors with circulating immune complexes involving the AB0 system.

作者信息

Heal J M, Masel D, Blumberg N

机构信息

American Red Cross, Rochester Region, NY 14607, USA.

出版信息

Vox Sang. 1996;71(4):205-11. doi: 10.1046/j.1423-0410.1996.7140205.x.

Abstract

When platelets that are AB0-nonidentical are transfused, circulating immune complexes (CIC) are formed. In the present study we examined the ability of polyclonal antibodies to two C1q receptors on platelets, cC1q-R and gC1q-R, and a monoclonal IgG Fc gamma RII (CD32) antibody directed against the platelet Fc receptor to inhibit the uptake of CIC involving the AB0 blood group system by normal platelets. Four types of immune complexes of varying purity were made in vitro. In addition serum from 5 refractory group A patients who had demonstrable AB0 CIC, 5 patients who had received only AB0-identical platelets and had no AB0 CIC and 6 normal donors were evaluated. After exposure of normal platelets to serum of patients with demonstrable AB0 CIC there were increased levels of platelet-associated IgG. This binding was partially inhibited by preincubation of the platelets with either anti-cC1q-R (3/5 patients), gC1q-R (3/5 patients) or IgG Fc gamma RII in 4/5 patients. However, the pattern of inhibition by the three antibodies was variable. Using the artificial immune complexes a more consistent pattern was obtained. The binding of four types of artificial immune complexes to platelets was reduced by 67-99% after preincubation of the platelets with antibodies to the complement and Fc receptors. The present work supports the hypothesis that AB0 CIC bind to Fc and complement receptors on the platelet and if confirmed would suggest a pathophysiological mechanism for the clinical observations of the important role of AB0 in platelet transfusion.

摘要

当输注ABO血型不匹配的血小板时,会形成循环免疫复合物(CIC)。在本研究中,我们检测了针对血小板上两种C1q受体(cC1q-R和gC1q-R)的多克隆抗体以及一种针对血小板Fc受体的单克隆IgG FcγRII(CD32)抗体抑制正常血小板摄取涉及ABO血型系统的CIC的能力。体外制备了四种纯度不同的免疫复合物。此外,还评估了5例有可检测到的ABO CIC的难治性A型患者、5例仅接受ABO血型匹配血小板且无ABO CIC的患者以及6名正常供者的血清。正常血小板暴露于有可检测到的ABO CIC的患者血清后,血小板相关IgG水平升高。用抗cC1q-R(3/5例患者)、gC1q-R(3/5例患者)或IgG FcγRII(4/5例患者)对血小板进行预孵育,可部分抑制这种结合。然而,三种抗体的抑制模式各不相同。使用人工免疫复合物获得了更一致的模式。用针对补体和Fc受体的抗体对血小板进行预孵育后,四种人工免疫复合物与血小板的结合减少了67%-99%。目前的工作支持了ABO CIC与血小板上的Fc和补体受体结合的假说,如果得到证实,将提示ABO在血小板输注中重要作用的临床观察的病理生理机制。

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