文章摘要
乔晓红谢晓恬△ 石苇唐晋清.集落刺激因子治疗重型再生障碍性贫血疗效和安全性的Meta 分析[J].,2012,12(18):3553-3558
集落刺激因子治疗重型再生障碍性贫血疗效和安全性的Meta 分析
Meta Analysis of the Effect of Colony Stimulating Factor on AplasticAnemia Patients
  
DOI:
中文关键词: 集落刺激因子  再生障碍性贫血  Meta 分析  免疫抑制治疗
英文关键词: Colony stimulating factor  Aplastic anemia  Meta analysis  Immunosuppressive therapy
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作者单位
乔晓红谢晓恬△ 石苇唐晋清 同济大学附属同济医院儿科 
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中文摘要:
      目的:通过Meta 分析评价粒系或粒单系集落刺激因子(G-CSF 或GM-CSF)对接受免疫抑制治疗(IST)的重型再生障碍性贫 血(SAA)患者的疗效和安全性。方法:使用相关检索词检索MEDLINE、Cochrane Library、EMBASE、CNKI 及CBM 数据库,检索 时间1990 年1 月~2011 年12 月。纳入G-CSF 或GM-CSF 治疗SAA 的随机对照研究。用Review Manager4.2 统计软件对数据进 行Meta 分析。结果:共纳入4 篇文献,共466 例SAA 患者。Meta 分析结果显示:①IST 疗效:G-CSF/GM-CSF 组与对照组的SAA 患者对比,近远期疗效与生存率均无显著差异:总体生存率[OR=1.15,95%CI(0.73,1.82),P=0.54]、完全缓解率[OR=1.20,95%CI (0.71,2.02),P=0.50]、早期总体有效率[OR=1.61,95%CI(0.85,3.03),P=0.14]、远期总体有效率[OR=1.17,95%CI(0.78,1.74), P=0.45];②IST 相关感染:IST 治疗早期感染发生率、严重感染发生率、感染相关死亡率方面均未优于对照组;③G-CSF/GM-CSF 组的复发率低于对照组,差异显著[OR=0.57,95%CI(0.35,0.93),P=0.02];④G-CSF/GM-CSF 组远期随访发生克隆性病变的发生 率与对照组无统计学差异,恶性肿瘤(MDS/AML)发生率[OR=0.90,95%CI(0.41,1.99),P=0.79]、PNH 发生率[OR=1.48,95%CI (0.65,3.33),P=0.35]。结论:G-CSF/GM-CSF 应用于接受IST 治疗的SAA 患者,尚不能证明具有提高总体生存率、完全缓解率、总 体有效率、减少感染和感染相关死亡率等优势。虽然有可能降低复发率,也不增加远期克隆性病变发生率,但还需要更严格设计 的大样本双盲随机对照试验,并进行更为长期的随访研究。
英文摘要:
      Objective: Immunosuppressive therapy is the treatment for aplastic anemia patients ineligible for transplantation. The role of granulocyte colony stimulating factor (G-CSF) and granulocyte-monocyte colony stimulating factor (GM-CSF) as adjunct to treatment in these patients is unclear. Methods: All randomized controlled trials on the effect of G-CSF or GM-CSF on severe aplastic anemia obtained by searching MEDLINE, Cochrane Library, EMBASE, CNKI and CBM were included. Meta analysis was done by Review Manager 4.2 Software. Results: Four trials with totally 466 severe aplastic anemia patients were included. ① The addition of colony stimulating factor yielded no difference in overall survival [OR 1.15, 95%CI (0.73-1.82), P=0.54]. There was no difference in overall hematologic response, complete remission. ②There was no difference in the occurrence of infections. ③Colony stimulating factor significantly decreased the risk for relapse [OR 0.57,95%CI(0.35,0.93),P=0.02]. ④Colony stimulating factor were not associated with higher occurrence of myelodysplastic syndrome and acute myeloid leukemia [OR 0.90, 95% CI (0.41,1.99), P=0.79]or paroxysmal nocturnal hemoglobinuria[OR 1.48, 95%CI(0.65,3.33), P=0.35]. Conclusion: The addition of colony stimulating factor does not affect mortality, response rate or infections occurrence. Well designed double blind and randomized controlled trials with large sample size and long-term follow-up are needed for further evaluation of the efficacy and safety of the colony stimulating factor therapy.
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