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多发性骨髓瘤患者的异常纤维蛋白结构与纤维蛋白溶解抑制

Abnormal fibrin structure and inhibition of fibrinolysis in patients with multiple myeloma.

作者信息

Carr M E, Dent R M, Carr S L

机构信息

Coagulation Special Studies Laboratory, Department of Medicine, Medical College of Virginia 23298-0230, USA.

出版信息

J Lab Clin Med. 1996 Jul;128(1):83-8. doi: 10.1016/s0022-2143(96)90116-x.

Abstract

Abnormal clot structures have been reported in patients with multiple myeloma, and purified immunoglobulin G (IgG) has been shown to influence fibrin assembly in purified systems. Recently fibrin structure has been demonstrated to be a major determinant of fibrinolytic rates. This study examined the effects of purified polyclonal and monoclonal myeloma IgG on fibrin structure and fibrinolysis in plasma clots. Clotting was initiated by the addition of thrombin (1.0 NIH units/ml) and calcium (10 mmol/L). Gelation was monitored as a time-dependent increase in optical density (633 nm). Fibrin fiber size (mu = mass-length ratio) was measured by scanning the gel from 800 to 400 nm. Two preparations of polyclonal IgG and plasma samples from 10 patients with myeloma were studied. Both Sandoglobulin (Sandoz Pharmaceuticals Corp.) and Gamimmune (Miles Inc., Cutter Biological) decreased final gel turbidity as the IgG concentration increased from 0 to 15 mg/ml. Because of its high maltose content, Gamimmune produced more-pronounced effects. Over a concentration range of 0 to 15 mg IgG per milliliter, mu decreased from 1.25 to 0.59 x 10(13) daltons/cm for Sandoglobulin and from 1.30 to 0.18 x 10(13) daltons/cm for Gamimmune. Polyclonal IgG at 15 mg/ml prolonged clot lysis induced by tissue-type plasminogen activator (tPA) from 800 seconds to > 12 hours. Similar effects were noted in myeloma clots. mu values in myeloma clots were significantly smaller than mu values in comparable normal clots. mu became smaller and lysis times became increasingly prolonged as the IgG level increased. High IgG concentrations induce thin fiber formation and impair fibrinolysis in plasma gels. These results demonstrate that fibrinolysis is inhibited in myeloma clots and that the degree of inhibition is correlated with IgG-mediated alterations in fibrin structure. Thin fibrin fibers may contribute to thrombotic risk in myeloma.

摘要

据报道,多发性骨髓瘤患者存在异常的凝块结构,并且在纯化系统中已表明纯化的免疫球蛋白G(IgG)会影响纤维蛋白组装。最近,已证明纤维蛋白结构是纤维蛋白溶解速率的主要决定因素。本研究检测了纯化的多克隆和单克隆骨髓瘤IgG对血浆凝块中纤维蛋白结构和纤维蛋白溶解的影响。通过加入凝血酶(1.0 NIH单位/毫升)和钙(10毫摩尔/升)启动凝血。将凝胶化监测为光密度(633纳米)随时间的增加。通过扫描800至400纳米的凝胶来测量纤维蛋白纤维大小(μ =质量-长度比)。研究了两种多克隆IgG制剂以及10例骨髓瘤患者的血浆样本。随着IgG浓度从0增加到15毫克/毫升,Sandoglobulin(山德士制药公司)和Gamimmune(迈尔斯公司,卡特生物制品)均降低了最终凝胶浊度。由于其高麦芽糖含量,Gamimmune产生的作用更明显。在每毫升0至15毫克IgG的浓度范围内,Sandoglobulin的μ从1.25降至0.59×10¹³道尔顿/厘米,Gamimmune的μ从1.30降至0.18×10¹³道尔顿/厘米。15毫克/毫升的多克隆IgG将组织型纤溶酶原激活剂(tPA)诱导的凝块溶解时间从800秒延长至>12小时。在骨髓瘤凝块中也观察到类似的作用。骨髓瘤凝块中的μ值明显小于可比的正常凝块中的μ值。随着IgG水平升高,μ变小且溶解时间越来越长。高IgG浓度诱导血浆凝胶中形成细纤维并损害纤维蛋白溶解。这些结果表明骨髓瘤凝块中的纤维蛋白溶解受到抑制,并且抑制程度与IgG介导的纤维蛋白结构改变相关。细纤维蛋白可能会增加骨髓瘤患者的血栓形成风险。

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