Baron Frédéric, Sautois Brieuc, Baudoux Etienne, Matus Geoffrey, Fillet Georges, Beguin Yves
Department of Medicine, Division of Hematology, University of Liège, Liège, Belgium.
Exp Hematol. 2002 Jun;30(6):546-54. doi: 10.1016/s0301-472x(02)00795-6.
Allogeneic hematopoietic stem cell transplantation (HSCT) is associated with prolonged anemia caused by defective erythropoietin (Epo) production. We enrolled 34 recipients of an allogeneic HSCT in three consecutive trials to determine the optimal utilization of recombinant human erythropoietin (rhEpo) therapy in this setting.
In the first trial (n = 7), rhEpo 1400 U/kg/week was given from day 1 until a hemoglobin (Hb) level of 10 g/dL was achieved, for a maximum of 60 days. In the second trial, rhEpo 500 U/kg/week was given to achieve Hb levels of 13 to 14 g/dL in 13 anemic patients with fatigue 56 to 1440 days after transplant. In the third trial, rhEpo was scheduled to start on day 35 in 14 patients at a dose of 500 U/kg/week with the aim of achieving Hb levels of 13 to 14 g/dL.
In trial 1, erythroid recovery to 1% reticulocytes and red blood cell transfusion independence were faster, but the number of transfusions was not reduced compared to 10 controls. Responses were brisk in trial 2, with transfusion independence achieved after a median of 1 week in 12 of 13 patients, and 2-g Hb increments or Hb values of 11, 12, and 13 g/dL after 6, 7, 10, and 10 weeks, respectively. Transfusions were significantly reduced in the first month of rhEpo therapy. In trial 3, transfusion independence was obtained after a median of 1 week in 13 of 14 patients, and 2-g Hb increments or Hb values of 11, 12, and 13 g/dL after 3, 4, 6, and 8 weeks, respectively. Transfusions rates were considerably reduced compared to the previous month in the same patients or compared to controls undergoing peripheral blood or marrow transplant without rhEpo.
Anemia after allogeneic HSCT is exquisitely sensitive to rhEpo. The benefit is minimal when it is given early post-transplant, as used in all trials to date. However, the rate of major response is greater than 90% when rhEpo is started after day 35. These data provide the basis on which to conduct a prospective, randomized, placebo-controlled trial of rhEpo therapy after allogeneic HSCT.
异基因造血干细胞移植(HSCT)常伴有因促红细胞生成素(Epo)生成缺陷导致的长期贫血。我们在三项连续试验中纳入了34例异基因HSCT受者,以确定在这种情况下重组人促红细胞生成素(rhEpo)治疗的最佳应用方式。
在第一项试验(n = 7)中,从第1天开始给予rhEpo 1400 U/kg/周,直至血红蛋白(Hb)水平达到10 g/dL,最长持续60天。在第二项试验中,对13例移植后56至1440天出现贫血且伴有疲劳的患者给予rhEpo 500 U/kg/周,以使Hb水平达到13至14 g/dL。在第三项试验中,计划对14例患者在第35天开始给予rhEpo,剂量为500 U/kg/周,目标是使Hb水平达到13至14 g/dL。
在试验1中,红系恢复至网织红细胞1%及不再依赖红细胞输血的时间较快,但与10例对照相比,输血次数并未减少。试验2中的反应迅速,13例患者中有12例在中位时间1周后实现了不再依赖输血,在6、7、10和10周后Hb分别增加2 g或达到11、12和13 g/dL。在rhEpo治疗的第一个月,输血次数显著减少。在试验3中,14例患者中有13例在中位时间1周后实现了不再依赖输血,在3、4、6和8周后Hb分别增加2 g或达到11、12和13 g/dL。与同一患者前一个月相比,或与未接受rhEpo的外周血或骨髓移植对照相比,输血率大幅降低。
异基因HSCT后的贫血对rhEpo极为敏感。如迄今为止所有试验中那样,在移植后早期给予rhEpo,获益极小。然而,在第35天后开始使用rhEpo时,主要反应率大于90%。这些数据为开展异基因HSCT后rhEpo治疗的前瞻性、随机、安慰剂对照试验提供了依据。
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