Palumbo Antonio, Avonto Ilaria, Bruno Benedetto, Ambrosini Maria Teresa, Bringhen Sara, Cavallo Federica, Falco Patrizia, Boccadoro Mario
Divisione di Ematologia, l'Università di Torino, Azienda Ospedaliera S. Giovanni Battista, Ospedale Molinette, Turin, Italy.
Eur J Haematol. 2006 Apr;76(4):273-7. doi: 10.1111/j.1600-0609.2005.00610.x.
Thalidomide combined with conventional chemotherapies including oral melphalan shows significant anti-myeloma activity. To address this issue, feasibility and efficacy of a three drug combination consisting of intravenous (i.v.) melphalan, thalidomide and prednisone [M(i.v.)PT] was evaluated in advanced myeloma patients.
Twenty-four advanced myeloma patients were treated with multiple cycles of a regimen consisting of low dose i.v. melphalan (20 mg/m2) at d 1, thalidomide at the dose of 50-100 mg/d given continuously and oral prednisone at the planned dose of 50 mg/d every other day. Intravenous melphalan was administered every fourth month. Median time from diagnosis was 40 months (range: 8-144 months). Fifteen patients (66%) had previously been treated with a combination of thalidomide and dexamethasone or with thalidomide alone.
Overall, on an intent-to treat basis, 14 patients responded: three achieved near complete remission (nCR), seven achieved partial response (PR), four minimal response (MR). Six patients showed stable disease (SD) and four-disease progression. Interestingly, of five patients who had previously progressed while on thalidomide and prednisone, one reached nCR, two PR and one MR. After a median follow up of 14 months, median progression free survival was 9 months. Response duration was longer than that induced by the previous line of treatment in eight patients (33%). Thalidomide-associated toxicity mainly consisted of constipation, tingling and sedation.
M(i.v.)PT is an effective regimen, which can overcome resistance to thalidomide plus prednisone in advanced myeloma with acceptable toxicity.
沙利度胺联合包括口服美法仑在内的传统化疗显示出显著的抗骨髓瘤活性。为解决这一问题,我们评估了由静脉注射美法仑、沙利度胺和泼尼松组成的三联方案[M(i.v.)PT]在晚期骨髓瘤患者中的可行性和疗效。
24例晚期骨髓瘤患者接受了多周期治疗方案,该方案包括第1天静脉注射低剂量美法仑(20mg/m²)、持续给予50 - 100mg/d的沙利度胺以及隔日口服50mg/d的泼尼松。每四个月给予一次静脉注射美法仑。从诊断到治疗的中位时间为40个月(范围:8 - 144个月)。15例患者(66%)先前接受过沙利度胺与地塞米松联合治疗或单独使用沙利度胺治疗。
总体而言,在意向性治疗基础上,14例患者有反应:3例达到接近完全缓解(nCR),7例达到部分缓解(PR),4例达到最小反应(MR)。6例患者疾病稳定(SD),4例疾病进展。有趣的是,在5例先前接受沙利度胺和泼尼松治疗时病情进展的患者中,1例达到nCR,2例达到PR,1例达到MR。中位随访14个月后,无进展生存期的中位数为9个月。8例患者(33%)的缓解持续时间长于上一线治疗方案诱导的缓解持续时间。沙利度胺相关毒性主要包括便秘、刺痛和镇静。
M(i.v.)PT是一种有效的方案,可克服晚期骨髓瘤对沙利度胺加泼尼松的耐药性,且毒性可接受。
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