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正常人和血管内凝血及血栓形成疾病患者血浆蛋白C抑制剂及两种活化蛋白C-抑制剂复合物的测定。

Determination of plasma protein C inhibitor and of two activated protein C-inhibitor complexes in normals and in patients with intravascular coagulation and thrombotic disease.

作者信息

España F, Vicente V, Tabernero D, Scharrer I, Griffin J H

机构信息

Committee on Vascular Biology, Research Institute of Scripps Clinic, La Jolla, CA 92037.

出版信息

Thromb Res. 1990 Aug 1;59(3):593-608. doi: 10.1016/0049-3848(90)90418-c.

Abstract

We developed an ELISA to quantitate complexes of activated protein C (APC) with a major plasma APC inhibitor, alpha 1-antitrypsin (alpha 1AT) in human plasma based on the sandwich principle using two different antibodies directed towards protein C and alpha 1AT, respectively. This ELISA test was specific for APC:alpha 1AT complexes and sensitive to greater than or equal to 150 pg complex. Fifty-one of 56 healthy donors had APC:alpha 1AT complex levels above the detection limit (3 ng/ml) ranging from 4 to 14 ng/ml (mean value +/- SD: 7.6 +/- 2.5 ng/ml). Patients (n = 10) with disseminated intravascular coagulation (DIC) had detectable levels of APC:alpha 1AT complex ranging from 21 to 125 ng/ml (median: 69 ng/ml). Complexes of APC with plasma protein C inhibitor (PCI) were also measured using an ELISA sandwich assay. None of the 30 healthy donors had detectable levels (greater than or equal to 5 ng/ml) of APC:PCI complex, and plasma samples from 9 of 10 DIC patients had detectable concentrations of APC:PCI complex ranging from 10 to 63 ng/ml (median: 22 ng/ml). APC:alpha 1AT complex was detected in 25 of 26 patients with deep venous thrombosis (DVT), with levels ranging from 5 to 136 ng/ml (median: 23 ng/ml), whereas APC:PCI was detected in only 6 DVT patients, with levels between 11 and 105 ng/ml. PCI antigen levels in 70 normals ranged from 56 to 175% (mean +/- SD: 99.1% +/- 24.2%). PCI antigen levels were decreased in DIC patients, in patients with cerebral arterial thrombosis, and in DVT patients undergoing heparin therapy, but not in patients with myocardial infarction. PCI antigen levels were decreased much further in DVT patients receiving heparin compared to those not receiving heparin, showing that heparin therapy is associated with a decrease in PCI levels. The detection in normal subjects and in thrombotic patients of circulating APC:inhibitor complexes supports the view that the protein C pathway is activated during DIC and DVT. Moreover, it emphasizes that both PCI and alpha 1AT are physiologic inhibitors of APC. Thus, measurement of APC complexes may provide sensitive parameters for specific detection of activation of the clotting and protein C pathways.

摘要

我们基于夹心原理,分别使用两种针对蛋白C和α1抗胰蛋白酶(α1AT)的不同抗体,开发了一种酶联免疫吸附测定法(ELISA),用于定量人血浆中活化蛋白C(APC)与主要血浆APC抑制剂α1抗胰蛋白酶形成的复合物。这种ELISA检测对APC:α1AT复合物具有特异性,对≥150 pg的复合物敏感。56名健康供者中有51人的APC:α1AT复合物水平高于检测限(3 ng/ml),范围为4至14 ng/ml(平均值±标准差:7.6±2.5 ng/ml)。10名弥散性血管内凝血(DIC)患者的APC:α1AT复合物水平可检测到,范围为21至125 ng/ml(中位数:69 ng/ml)。还使用ELISA夹心测定法测量了APC与血浆蛋白C抑制剂(PCI)的复合物。30名健康供者中无人检测到APC:PCI复合物水平(≥5 ng/ml),10名DIC患者中有9人的血浆样本检测到APC:PCI复合物浓度,范围为10至63 ng/ml(中位数:22 ng/ml)。26名深静脉血栓形成(DVT)患者中有25人检测到APC:α1AT复合物,水平范围为5至136 ng/ml(中位数:23 ng/ml),而仅6名DVT患者检测到APC:PCI,水平在11至105 ng/ml之间。70名正常人的PCI抗原水平范围为56%至175%(平均值±标准差:99.1%±24.2%)。DIC患者、脑动脉血栓形成患者以及接受肝素治疗的DVT患者的PCI抗原水平降低,但心肌梗死患者未降低。与未接受肝素治疗的DVT患者相比,接受肝素治疗的DVT患者的PCI抗原水平进一步降低,表明肝素治疗与PCI水平降低有关。在正常受试者和血栓形成患者中检测到循环中的APC:抑制剂复合物,支持了蛋白C途径在DIC和DVT期间被激活的观点。此外,这强调了PCI和α1AT都是APC的生理性抑制剂。因此,测量APC复合物可能为凝血和蛋白C途径激活的特异性检测提供敏感参数。

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