粒细胞集落刺激因子在肝移植受者中疗效与安全性的随机、安慰剂对照、双盲、多中心试验
Randomized, placebo-controlled, double-blind, multicenter trial of efficacy and safety of granulocyte colony-stimulating factor in liver transplant recipients.
作者信息
Winston D J, Foster P F, Somberg K A, Busuttil R W, Levy M F, Sheiner P A, Reddy K R, Fotheringham N, Armstrong M, Logan E
机构信息
Department of Medicine, the Dumont-UCLA Transplant Center, UCLA Medical Center, Los Angeles, California 90095, USA.
出版信息
Transplantation. 1999 Nov 15;68(9):1298-304. doi: 10.1097/00007890-199911150-00014.
BACKGROUND
Infection and rejection are two common complications after liver transplants. In a preliminary study, administration of granulocyte colony-stimulating factor (G-CSF) to liver transplant recipients was associated with a decrease in sepsis episodes, sepsis-related deaths, and rejection compared with a historical control group of patients. The purpose of this study was to evaluate further the efficacy of G-CSF in liver transplant patients in a randomized, placebo-controlled, double-blind, multicenter trial.
METHODS
Adult patients with a United Network Organ Sharing classification of 1 or 2 were randomized to receive a placebo, 100 microg/day of G-CSF or 300 microg/day of G-CSF. The study drug was started preoperatively and then continued after the transplant for a maximum of 21 days. Patients were evaluated for microbiologically-documented infection, biopsy-proven rejection, number of treatments for rejection, length of stay in the intensive care unit and hospital, graft survival, death, and adverse events.
RESULTS
During the first 30 days after the transplant, the median peak white blood cell count was 16.5x10(9)/L, 34.6x10(9)L, and 54.8x10(9)/L for the placebo, low-dose G-CSF, and high-dose G-CSF patients, respectively. The incidence of infection was 30% in G-CSF patients (34 of 114 patients) and 34% in placebo patients (20 of 58 patients). Except for more nosocomial pneumonias in the G-CSF patients (7 in 114 patients vs. 0 in 58 patients, P=0.056), the types of infections and causative organisms were also similar in both treatment groups. Although the number of treatments for clinically suspected or proven rejection was similar in the G-CSF and placebo patients, biopsy-proven rejection occurred more often in G-CSF patients (34 of 114 patients or 30%) than placebo patients (11 of 58 patients or 19%) (P=0.093). There were no cases of graft loss caused by rejection. G-CSF had no effect on length of stay in the intensive-care unit or hospital. There were 22 G-CSF patients (18%) and 10 placebo patients (15%) who died within 120 days after the transplant. No serious adverse events were attributed to G-CSF.
CONCLUSION
Despite producing substantial increases in the white blood cell count after the transplant, G-CSF had no beneficial effects on infection, rejection, or survival in this study. Biopsy-proven rejection and nosocomial pneumonias were more common in patients treated with G-CSF compared with those taking the placebo. No serious adverse events were attributed to G-CSF.
背景
感染和排斥反应是肝移植术后两种常见的并发症。在一项初步研究中,与历史对照组患者相比,对肝移植受者给予粒细胞集落刺激因子(G-CSF)可使脓毒症发作、脓毒症相关死亡及排斥反应减少。本研究的目的是在一项随机、安慰剂对照、双盲、多中心试验中进一步评估G-CSF对肝移植患者的疗效。
方法
器官共享联合网络分级为1级或2级的成年患者被随机分为接受安慰剂、每日100微克G-CSF或每日300微克G-CSF治疗。研究药物在术前开始使用,移植后继续使用,最长使用21天。对患者进行微生物学证实的感染、活检证实的排斥反应、排斥反应治疗次数、重症监护病房和医院住院时间、移植物存活情况、死亡情况及不良事件的评估。
结果
移植后的前30天内,安慰剂组、低剂量G-CSF组和高剂量G-CSF组患者的白细胞计数峰值中位数分别为16.5×10⁹/L、34.6×10⁹/L和54.8×10⁹/L。G-CSF组患者的感染发生率为30%(114例患者中的34例),安慰剂组为34%(58例患者中的20例)。除G-CSF组患者的医院获得性肺炎更多(114例患者中的7例 vs. 58例患者中的0例,P = 0.056)外,两个治疗组的感染类型和病原体也相似。尽管G-CSF组和安慰剂组患者临床上疑似或证实的排斥反应治疗次数相似,但活检证实的排斥反应在G-CSF组患者中更常见(114例患者中的34例或30%),高于安慰剂组(58例患者中的11例或19%)(P = 0.093)。没有因排斥反应导致移植物丢失的病例。G-CSF对重症监护病房或医院的住院时间没有影响。有22例G-CSF组患者(18%)和10例安慰剂组患者(15%)在移植后120天内死亡。没有严重不良事件归因于G-CSF。
结论
尽管移植后G-CSF使白细胞计数大幅增加,但在本研究中G-CSF对感染、排斥反应或存活没有有益影响。与服用安慰剂的患者相比,G-CSF治疗的患者活检证实的排斥反应和医院获得性肺炎更常见。没有严重不良事件归因于G-CSF。
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