Darby S C, Keeling D M, Spooner R J D, Wan Kan S, Giangrande P L F, Collins P W, Hill F G H, Hay C R M
Department of Clinical and Laboratory Haematology, The Birmingham Children's Hospital, Birmingham, UK.
J Thromb Haemost. 2004 Jul;2(7):1047-54. doi: 10.1046/j.1538-7836.2004.00710.x.
Previous studies of the development of inhibitors and their impact on mortality have been small.
To examine the development of inhibitors in people with hemophilia in the UK and their effect on subsequent mortality.
6078 males with hemophilia A and 1172 males with hemophilia B registered in the UK Haemophilia Centre Doctors' Organisation database, 1977-98.
In severe hemophilia A inhibitors developed at rates of 34.4, 5.2 and 3.8 per 1000 years at ages <5, 5-14 and 15+years; cumulative risks at ages 5 and 75 were 16% and 36%. In hemophilia A the rate of inhibitor development decreased during 1977-90, but increased during the 1990s. In severe hemophilia B inhibitors developed at rates of 13.3 and 0.2 per 1000 years at ages <5 and 5+ and cumulative risks at ages 5 and 75 were 6% and 8%. With HIV, inhibitor development did not increase mortality. In severe hemophilia without HIV, inhibitor development doubled mortality during 1977-92, but during 1993-99 mortality was identical with and without inhibitors. In severe hemophilia without HIV but with inhibitors, mortality from causes involving bleeding decreased during 1977-99 (P = 0.001) as did mortality involving intracranial hemorrhage (P = 0.007).
These data provide estimates of the rate of inhibitor development in hemophilia A and hemophilia B, and they show that the rate of inhibitor development has varied over time, although the reasons for this remain unclear. They also show that in severe hemophilia the substantial increase in mortality previously associated with inhibitors is no longer present.
以往关于抑制剂的产生及其对死亡率影响的研究规模较小。
研究英国血友病患者中抑制剂的产生情况及其对后续死亡率的影响。
1977 - 1998年在英国血友病中心医生组织数据库中登记的6078例甲型血友病男性患者和1172例乙型血友病男性患者。
在重度甲型血友病中,年龄<5岁、5 - 14岁和15岁及以上者抑制剂产生率分别为每1000年34.4、5.2和3.8例;5岁和75岁时的累积风险分别为16%和36%。在甲型血友病中,1977 - 1990年抑制剂产生率下降,但在20世纪90年代有所上升。在重度乙型血友病中,年龄<5岁和5岁及以上者抑制剂产生率分别为每1000年13.3例和0.2例;5岁和75岁时的累积风险分别为6%和8%。感染HIV时,抑制剂的产生并未增加死亡率。在未感染HIV的重度血友病中,1977 - 1992年抑制剂的产生使死亡率增加了一倍,但在1993 - 1999年,有抑制剂和无抑制剂时的死亡率相同。在未感染HIV但有抑制剂的重度血友病中,1977 - 1999年因出血相关原因导致的死亡率下降(P = 0.001),颅内出血导致的死亡率也下降(P = 0.007)。
这些数据提供了甲型和乙型血友病中抑制剂产生率的估计值,表明抑制剂产生率随时间变化,尽管其原因尚不清楚。数据还表明,在重度血友病中,先前与抑制剂相关的死亡率大幅增加的情况已不复存在。
