Studies on the medical treatment of deep vein thrombosis.

S Schulman
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Abstract

The aim of these studies was to investigate different regimens of thrombolytic therapy and oral anticoagulation, and to evaluate the effects of streptokinase (SK), heparin and warfarin in the treatment of deep vein thrombosis (DVT). Low-dose SK, although controlled according to the fibrinogen levels, did not provide improved thrombolysis compared to conventional high-dose SK, and more postthrombotic changes were registered after an average of 3 years. Furthermore, serious hemorrhagic side-effects occurred, which makes this regimen inexpedient. Various regimens of local venous infusion of SK were tried, and with a dose of 4,000 IU/h for 72 h in combination with heparin a thrombolytic effect was achieved, albeit not greater than usually observed with conventional SK. Systemic hypofibrinogenemia and hemorrhage were not avoided. A hitherto not described side-effect with bullous dermatitis was reported. Venographic severity of calf vein thrombosis displayed a statistically significant correlation to long-term hemodynamic changes, as assessed with foot volumetry, after an average of 5 years. This correlation was stronger for the size of the thrombus after initial treatment than for the size at diagnosis. Thus it seems important to treat calf vein thrombosis with heparin in order to limit the extent of the thrombus, thereby reducing long-term sequelae. During heparin treatment, an average reduction of the thrombi of 17% was observed. This reduction was significantly correlated to a short duration of symptoms but not to parameters of heparin therapy or fibrinolytic components. However, patients with substantial thrombolysis had high plasmin-alpha 2-antiplasmin (PAP) levels, and those with high tissue plasminogen activator (t-PA) inhibitor levels and remarkably also those with high t-PA antigen levels had no lysis. The concentration of t-PA antigen showed a significant increase during heparin infusion, whereas that of PAP and t-PA inhibitor was not influenced. By applying more intensive initial oral anticoagulation, stable therapeutic prothrombin time (PT)-levels were achieved one day earlier and the duration of heparin infusion could be equally reduced compared to the conventional regimen (4.4-5 days vs 5.4-6 days). The activity of coagulation factors II, VII, IX and X had dropped to the same level with both regimens the day heparin was discontinued, observed. The effectiveness of oral anticoagulation after DVT was studied in 596 patients treated for a total of 4450 months.(ABSTRACT TRUNCATED AT 400 WORDS)

深静脉血栓的内科治疗研究。
这些研究的目的是探讨不同的溶栓治疗方案和口服抗凝治疗方案,并评估链激酶(SK)、肝素和华法林治疗深静脉血栓(DVT)的效果。低剂量SK虽然根据纤维蛋白原水平进行控制,但与常规高剂量SK相比,并没有改善溶栓效果,平均3年后出现更多血栓后变化。此外,严重的出血性副作用发生,这使得这种方案不合适。我们尝试了各种局部静脉输注SK的方案,并以4000 IU/h的剂量与肝素联合使用72小时,达到了溶栓效果,尽管并不比通常观察到的传统SK更大。系统性低纤维蛋白原血症和出血并没有避免。一个迄今未描述的副作用与大疱性皮炎报道。平均5年后,用足部容积法评估,小腿静脉血栓形成的静脉造影严重程度与长期血流动力学变化有统计学意义。与诊断时的血栓大小相比,初始治疗后血栓大小的相关性更强。因此,用肝素治疗小腿静脉血栓似乎很重要,以限制血栓的范围,从而减少长期后遗症。在肝素治疗期间,观察到血栓平均减少17%。这种减少与症状持续时间短显著相关,但与肝素治疗或纤溶成分参数无关。然而,大量溶栓的患者有较高的纤溶酶α - 2-抗纤溶酶(PAP)水平,而组织型纤溶酶原激活物(t-PA)抑制剂水平高的患者和t-PA抗原水平高的患者没有溶栓。肝素输注后t-PA抗原浓度显著升高,而PAP和t-PA抑制剂浓度不受影响。通过应用更强化的初始口服抗凝,稳定的治疗凝血酶原时间(PT)水平可以提前一天达到,与常规方案相比,肝素输注的持续时间可以同样减少(4.4-5天vs 5.4-6天)。在停用肝素的当天,两种治疗方案的凝血因子II、VII、IX和X的活性均降至相同水平。对596例DVT术后口服抗凝治疗的疗效进行了研究,共治疗4450个月。(摘要删节为400字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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