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英国医学研究委员会关于α-干扰素n1治疗慢性粒细胞白血病的随机多中心试验:无论细胞遗传学反应如何,生存率均有所提高。英国医学研究委员会成人白血病治疗试验工作小组。

UK Medical Research Council randomised, multicentre trial of interferon-alpha n1 for chronic myeloid leukaemia: improved survival irrespective of cytogenetic response. The UK Medical Research Council's Working Parties for Therapeutic Trials in Adult Leukaemia.

作者信息

Allan N C, Richards S M, Shepherd P C

机构信息

CML Trial Office, Western General Hospital, Edinburgh, UK.

出版信息

Lancet. 1995 Jun 3;345(8962):1392-7. doi: 10.1016/s0140-6736(95)92596-1.

Abstract

Interferon-alpha may be better than cytotoxic drugs in the long-term management of patients with chronic myeloid leukaemia (CML) in chronic phase. To test this possibility 587 patients with CML in chronic phase were randomly allocated to receive lymphoblastoid cell-line interferon-alpha n1 (IFN-alpha, n = 293) or chemotherapy with busulphan or hydroxyurea (no IFN-alpha, n = 294) as maintenance after initial induction treatment with cytotoxic drugs. There was a significant survival benefit for patients in the IFN-alpha arm when analysed on the basis of intention to treat (2p = 0.0009). The median survival for those allocated IFN-alpha was 61 months and no IFN-alpha was 41 months. Out of 269 patients with Philadelphia-positive CML in the IFN-alpha arm with at least 6 months follow-up, 211 were evaluable for haematological response: 145 (68%) achieved good responses (A+ or A type), 37 (18%) had partial responses (B type) and 29 (14%) had poor responses (C type). Patients with types A and B responses had a better survival than those in the no IFN-alpha arm; patients with type C responses had survival equivalent to the no IFN-alpha arm. Of these 269 patients, 26 of whom had not started IFN-alpha, 59 (22%) achieved a significant degree of cytogenetic response but 210 (78%) did not have a response. Cytogenetic responders survived significantly longer than non-responders and even non-responders survived longer than patients in the no IFN-alpha arm. Since cytogenetic non-responders had worse than average prognostic features, they may also benefit from IFN-alpha therapy. We conclude that treatment with IFN-alpha prolongs the survival of patients with CML; benefits of IFN-alpha are not confined to cytogenetic responders but may extend to most, if not all patients receiving IFN-alpha treatment; and cytogenetic response to IFN-alpha treatment identifies patients with a relatively good prognosis.

摘要

在慢性期慢性髓性白血病(CML)患者的长期管理中,α干扰素可能优于细胞毒性药物。为了验证这一可能性,587例慢性期CML患者在接受细胞毒性药物初始诱导治疗后,被随机分配接受淋巴母细胞系α干扰素(IFN-α,n = 293)或白消安或羟基脲化疗(不使用IFN-α,n = 294)作为维持治疗。在意向性治疗分析的基础上,IFN-α组患者有显著的生存获益(P = 0.0009)。分配到IFN-α组的患者中位生存期为61个月,未使用IFN-α组为41个月。在IFN-α组中,269例费城染色体阳性的CML患者至少随访6个月,其中211例可评估血液学反应:145例(68%)达到良好反应(A+或A型),37例(18%)有部分反应(B型),29例(14%)反应不佳(C型)。A和B型反应的患者比未使用IFN-α组的患者生存期更长;C型反应的患者生存期与未使用IFN-α组相当。在这269例患者中,26例尚未开始使用IFN-α,59例(22%)达到显著程度的细胞遗传学反应,但210例(78%)无反应。细胞遗传学反应者的生存期明显长于无反应者,甚至无反应者的生存期也长于未使用IFN-α组的患者。由于细胞遗传学无反应者的预后特征比平均水平差,他们可能也从IFN-α治疗中获益。我们得出结论,IFN-α治疗可延长CML患者的生存期;IFN-α的益处不仅限于细胞遗传学反应者,可能还扩展到大多数(如果不是全部)接受IFN-α治疗的患者;对IFN-α治疗的细胞遗传学反应可识别预后相对较好的患者。

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