Leahey A M, Bunin N J
Department of Pediatrics, University of Pennsylvania, Philadelphia, USA.
Bone Marrow Transplant. 1996 Jun;17(6):1101-4.
Nine pediatric patients were treated with recombinant human tissue plasminogen activator (tPA) for severe hepatic veno-occlusive disease (VOD) which developed after bone marrow transplantation. Recombinant human tPA (5-10 mg/day x 2-4 days) and heparin were begun a median of 15 days (range, 11-32 days) post-transplant. A second course was given if the patient did not respond. The median total serum bilirubin and percent weight gain above baseline were 5.5 mg/dl (range, 1.3-26.1 mg/dl) and 22% (range, 7-44%) respectively at the start of tPA administration. Three patients had their heparin infusion interrupted or discontinued for bleeding symptoms, none of which were life-threatening. Five of the nine patients had complete resolution of their VOD. Another patient was salvaged with a partial maternal liver transplant. We conclude that the incidence and severity of bleeding complications with these doses of tPA and heparin do not preclude their use in pediatric patients. Further study in a larger group setting will be necessary to determine the optimal dosing regimen as well as treatment efficacy.
9名儿科患者因骨髓移植后发生的严重肝静脉闭塞病(VOD)接受了重组人组织型纤溶酶原激活剂(tPA)治疗。重组人tPA(5 - 10毫克/天×2 - 4天)和肝素在移植后中位15天(范围11 - 32天)开始使用。如果患者无反应则给予第二个疗程。在开始使用tPA时,血清总胆红素中位数和高于基线的体重增加百分比分别为5.5毫克/分升(范围1.3 - 26.1毫克/分升)和22%(范围7 - 44%)。3名患者因出血症状中断或停止了肝素输注,均无生命危险。9名患者中有5名VOD完全缓解。另一名患者通过部分母肝移植获救。我们得出结论,这些剂量的tPA和肝素引起的出血并发症的发生率和严重程度并不妨碍其在儿科患者中的使用。有必要在更大规模的群体中进行进一步研究,以确定最佳给药方案以及治疗效果。
