干扰素α -2b治疗ph1阳性慢性髓性白血病的发展模式

Enrica Morra , Giuliana Alimena , Mario Lazzarino , Anna Marina Liberati , Enrico Montefusco , Paolo Bernasconi , Marco Mancini , Emilio Donti , Serena Merante , Ferdinando Dianzani , Fausto Grignani , Carlo Bernasconi , Franco Mandelli
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引用次数: 6

摘要

我们已对126例ph1阳性慢性髓性白血病患者单独或联合化疗使用干扰素α -2b。71例早期慢性期(CP)患者(<诊断后12个月),41例(58%)获得完全血液学缓解(CHR)。每日干扰素比间歇给药更有效。在先前未接受治疗的患者中,诊断时的风险状况显著影响疗效。71例患者中有34例(48%)细胞遗传学改善,Ph1+有丝分裂的中位数从100%下降到66%,其中1例完全抑制了Ph1。46例晚期CP患者(>诊断后12个月),32例(70%)单独使用干扰素或联合化疗达到CHR。10例经化疗控制良好的患者,单用干扰素均获得稳定的CHR。在36例对常规化疗有部分反应的患者中,22例(61%)在干扰素加低剂量羟基脲治疗下获得CHR。16例晚期CP患者(35%)达到Ph1嵌合(中位Ph1+细胞75%)。在接受干扰素加化疗的9例加速期患者中,1例达到CHR, 2例部分缓解。在平均36个月的随访中,41例早期CP CHR患者中,15例接受干扰素治疗,12例接受自体骨髓移植(BMT), 2例接受同种异体骨髓移植。41名CHR患者中有8名(19%)发生了母细胞转化(BT),而30名患者中有17名(57%)对干扰素无反应或部分反应。在中位22个月的随访中,32例晚期CP患者获得CHR, 26例继续使用干扰素,1例患有同种异体BMT, 1例患有自体BMT, 1例发展为BT(14例少于CHR的患者中有5例)。这些研究证实了干扰素在慢性粒细胞白血病中的血液学和细胞遗传学疗效,并表明治疗开始时的疾病状态是决定治疗成功的关键。
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Evolving modalities of treatment with interferon alfa-2b for Ph1-positive chronic myelogenous leukaemia

We have administered interferon alfa-2b, alone or in combination with chemotherapy, to 126 Ph1-positive chronic myelogenous leukaemia patients. Of 71 early chronic phase (CP) patients (< 12 months from diagnosis), 41 (58%) obtained a complete haematological response (CHR). Daily interferon was more effective than intermittent administration. In previously untreated patients, the response was significantly influenced by risk status at diagnosis. Thirty-four out of 71 (48%) patients improved cytogenetically, the median of Ph1+ mitoses declining from 100% to 66% with complete Ph1-suppression in one case. Of 46 late CP patients (> 12 months from diagnosis), 32 (70%) achieved CHR with interferon alone or combined with chemotherapy. All 10 patients with disease well controlled by chemotherapy obtained stable CHR with interferon alone. Of 36 partial responders to conventional chemotherapy, 22 (61%) obtained CHR on interferon plus low-dose hydroxyurea. Ph1 mosaicism was reached by 16 (35%) late CP patients (median Ph1+ cells 75%). Of nine accelerated phase patients on interferon plus chemotherapy, one attained CHR, and two responded partially. At a median follow up of 36 months, of 41 CHR patients in early CP, 15 are controlled on interferon, 12 have had autologous bone marrow transplantation (BMT), and two allogeneic BMT. Blastic transformation (BT) has occurred in eight of 41 CHR patients (19%) versus 17 of 30 (57%) non-responders and partial responders to interferon. At a median follow up of 22 months, of 32 late CP patients obtaining CHR, 26 remain on interferon, one had allogeneic BMT, one had autologous BMT, and one developed BT (versus five out of 14 with less than CHR). These studies confirm the haematological and cytogenetic efficacy of interferon in CML and indicate that the disease status at the start of treatment is critical in determining the success of therapy.

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