首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Prevalence, isotype, and functionality of antiheparin-platelet factor 4 antibodies in patients treated with heparin and clinically suspected for heparin-induced thrombocytopenia. The pathogenic role of IgG.
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Prevalence, isotype, and functionality of antiheparin-platelet factor 4 antibodies in patients treated with heparin and clinically suspected for heparin-induced thrombocytopenia. The pathogenic role of IgG.

机译:抗肝素-血小板因子4抗体的患病率,同种型和功能在接受肝素治疗且临床怀疑为肝素诱导的血小板减少症的患者中。 IgG的致病作用。

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Antibodies to heparin-platelet factor 4 (PF4) complexes have been observed in patient with heparin-induced thrombocytopenia (HIT) syndrome. These antibodies may be of various isotypes and differ with respect to their ability to activate platelets/endothelial cells. This study determined the isotypes and functionality of antiheparin-platelet factor 4 (AHPF4) antibodies in 111 patients treated with heparin and clinically suspected for HIT. In this patient population, 50% had detectable AHPF4 cumulative IgA, IgG, and IgM (determined by enzyme-linked immunosorbent assay, ELISA), but only 35% was positive when tested with the (14)C-serotonin release assay (SRA). Using antihuman Ig specific for different isotypes, we found that 50% of the 111 samples was positive for IgG, 45% for IgM, and 37% for IgA. In 50 normal human serum (NHS) samples, only two were positive for IgG, but 33 were positive for IgM, indicating a potential humoral response to the heparin-PF4 complex prior to heparin administration. Patientsthat were ELISA(+) for AHPF4 antibody titer were subdivided into SRA-positive (+) and SRA-negative (-) groups. The SRA(+) group had a mean ELISA optical density (OD) for AHPF4 IgA/IgG/IgM of 2.1, while the SRA(-) group had a mean OD of 0.8 (P<.001). The SRA(+) group had greater mean OD values for all three individual isotypes. Using flow cytometry, we determined the ability of different patient samples to activate platelets. Samples that contained IgG and were SRA(+) activated platelets (as measured by microparticle generation and P-selectin expression) in the presence of therapeutic concentrations of heparin. NHS and samples containing IgA and/or IgM that were SRA(-) were not able to produce microparticles nor were they able to increase expression of P-selectin. Together, these data indicate that IgG is the principal mediator of platelet activation in patients with HIT, with IgA and IgM playing a less significant role in the pathophysiology of this syndrome.
机译:在肝素诱导的血小板减少症(HIT)综合征患者中已观察到肝素-血小板因子4(PF4)复合物的抗体。这些抗体可以是各种同种型,并且它们活化血小板/内皮细胞的能力不同。这项研究确定了111例接受肝素治疗并临床怀疑为HIT的患者中抗肝素-血小板因子4(AHPF4)抗体的同种型和功能。在该患者人群中,有50%的患者具有可检测的AHPF4累积IgA,IgG和IgM(通过酶联免疫吸附测定,ELISA确定),但在使用(14)​​C-5-羟色胺释放测定(SRA)进行检测时,只有35%呈阳性。使用对不同同种型具有特异性的抗人Ig,我们发现111个样品中有50%的IgG阳性,IgM的45%,IgA的37%。在50份正常人血清(NHS)样品中,只有2份IgG阳性,但33份IgM阳性,表明在给予肝素之前可能对肝素-PF4复合物产生体液反应。 ELISA(+)检测AHPF4抗体滴度的患者分为SRA阳性(+)和SRA阴性(-)组。 SRA(+)组的AHPF4 IgA / IgG / IgM的ELISA平均光密度(OD)为2.1,而SRA(-)组的OD平均值为0.8(P <.001)。 SRA(+)组对所有三个同种型的平均OD值均较高。使用流式细胞仪,我们确定了不同患者样品激活血小板的能力。在存在治疗浓度的肝素的情况下,包含IgG且为SRA(+)活化的血小板(通过微粒生成和P-选择素表达测量)的样品。 NHS和包含IRA的IgA和/或IgM的样品既不能产生微粒,也不能增加P-选择蛋白的表达。总之,这些数据表明,IgG是HIT患者血小板活化的主要介质,而IgA和IgM在该综合征的病理生理中的作用较小。

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