Mauro Francesca R, Foa Robin, Meloni Giovanna, Gentile Massimo, Giammartini Elena, Giannarelli Diana, De Propris Maria Stefania, Rapanotti Maria Cristina, de Fabritiis Paolo, Mandelli Franco
Dipartimento di Biotecnologie Cellulari ed Ematologia, University La Sapienza, via Benevento 6, 00161 Rome, Italy.
Haematologica. 2002 Sep;87(9):926-33.
The objective of improving the quality of responses of chronic lymphocytic leukemia (CLL) patients has led to the design of protocols that combine fludarabine (FDR) with synergistic drugs. We evaluated the efficacy and toxicity of a schedule that includes fludarabine, ara-C, novantrone and dexamethasone (FAND) for the management of previously treated CLL patients under 60 years old.
Thirty-one patients underwent FAND treatment. Twenty-three patients had active disease (relapsed patients: 9; unresponsive to prior therapy: 14). Eight patients had a partial response (PR) to prior therapy and were treated with the aim of further reducing residual disease. The FAND schedule included fludarabine (25 mg/m(2) i.v. days 1-3), ara-C (1 g/m(2) i.v. day 1: 8 patients; days 1-2: 23 patients), novantrone (10 mg/m(2) i.v. day 1) and dexamethasone (20 mg i.v. days 1-3). Infection prophylaxis consisted of fluconazole, acyclovir, trimethoprim/sulfamethoxasole and granulocyte colony-stimulating factor (G-CSF) in the presence of severe neutropenia.
A response was observed in 7/14 refractory patients (complete response-CR: 29%), in all 9 relapsed patients (CR: 78%) and in 7/8 patients (CR: 87.5%) treated in PR. Taken together, 18 CRs were obtained and in 14 (78%) this was associated with a flow cytometric remission (CD5+/CD20(weak+) PB lymphocytes: <10%). Severe granulocytopenia occurred after 86 of the 124 administered courses (69%), but only after 10/86 courses (12%) were major infections recorded. In 10/15 mobilized patients (cyclophosphamide + G-CSF: 6 patients; FAND + G-CSF: 9 patients) after FAND > or = 2 x 10(6)/kg CD34+ cells were collected. Nine patients were autografted in CR and showed a longer response duration than the 9 patients in CR who did not receive further therapy after FAND (53 vs 30% at 41 months; p = 0.05).
FAND associated with extensive infection prophylaxis and G-CSF support is a highly cytoreductive and well-tolerated treatment for CLL patients and in most cases does not hamper subsequent stem cell mobilization.
提高慢性淋巴细胞白血病(CLL)患者缓解质量的目标促使了将氟达拉滨(FDR)与协同药物联合使用的方案设计。我们评估了包含氟达拉滨、阿糖胞苷、去甲氧基柔红霉素和地塞米松(FAND)的方案对60岁以下既往接受过治疗的CLL患者的疗效和毒性。
31例患者接受了FAND治疗。23例患者疾病处于活动期(复发患者:9例;对既往治疗无反应者:14例)。8例患者对既往治疗有部分缓解(PR),此次治疗旨在进一步减少残留疾病。FAND方案包括氟达拉滨(25mg/m²静脉滴注,第1 - 3天)、阿糖胞苷(1g/m²静脉滴注,第1天:8例患者;第1 - 2天:23例患者)、去甲氧基柔红霉素(10mg/m²静脉滴注,第1天)和地塞米松(20mg静脉滴注,第1 - 3天)。预防感染包括使用氟康唑、阿昔洛韦、甲氧苄啶/磺胺甲恶唑以及在严重中性粒细胞减少时使用粒细胞集落刺激因子(G - CSF)。
14例难治性患者中有7例出现缓解(完全缓解 - CR:29%),9例复发患者全部缓解(CR:78%),8例PR患者中有7例缓解(CR:87.5%)。总计获得18例CR,其中14例(78%)伴有流式细胞术缓解(CD5⁺/CD20⁽弱⁺⁾外周血淋巴细胞:<10%)。124个给药疗程中有86个(69%)出现严重粒细胞减少,但仅10/86个疗程(12%)记录到严重感染。15例动员患者中有10例(环磷酰胺 + G - CSF:6例;FAND + G - CSF:9例)在FAND治疗后收集到≥2×10⁶/kg CD34⁺细胞。9例CR患者接受自体造血干细胞移植,其缓解持续时间长于FAND治疗后未接受进一步治疗的9例CR患者(41个月时分别为53%和30%;p = 0.05)。
FAND联合广泛的感染预防措施和G - CSF支持对CLL患者是一种高度细胞减灭且耐受性良好的治疗方法,并且在大多数情况下不妨碍随后的干细胞动员。
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