Ravoet Christophe, Mineur Philippe, Robin Valérie, Debusscher Louisette, Bosly André, André Marc, El Housni Hakim, Soree Anne, Bron Dominique, Martiat Philippe
Jules Bordet Institute, Rue Héger-Bordet, 1, 1000 Brussels, Belgium.
Ann Hematol. 2008 Nov;87(11):881-5. doi: 10.1007/s00277-008-0536-2. Epub 2008 Jul 19.
Although an activating mutation of Ras is commonly observed in myelodysplastic syndrome (MDS), the role of Ras in the natural history of MDS remains largely unknown. We prospectively studied efficiency and tolerance of lonafarnib, a compound able to inhibit Ras signalling pathway through an inhibition of farnesyl transferase, in patients with MDS or secondary acute myeloid leukaemia (sAML). Lonafarnib was administered orally at a dose of 200 mg twice daily for three courses of 4 weeks (separated by 1 to 4 weeks without treatment). Sixteen patients were included: FAB/RAEB (n = 10), RAEB-T (n = 2), sAML (n = 2) and chronic myelomonocytic leukaemia (CMML; n = 2); WHO/RAEB-1 (n = 4), RAEB-2 (n = 5), AML (n = 5), CMML (n = 2). Median age was 70 (53-77) years. The karyotype was complex or intermediate in 11 patients, and the International Prognostic Scoring Systems (IPSS) risk groups were low in two patients, INT-1 in one patient, INT-2 in four patients and high in six patients (unknown or not applicable in three patients). Among the 14 patients tested, five had Ras mutations in codons 12, 13 or 61 of N-Ras, K-Ras or H-Ras. One patient was excluded of the analysis for protocol violation, and 15 patients were assessable for tolerance. Gastrointestinal toxicities (diarrhoea, nausea and anorexia) and myelosuppression were the major side effects. Other toxicities included infections, fatigue, increase of liver enzymes, arrhythmia and skin rash. One patient died of infection, and the treatment was stopped in one other who developed atrial fibrillation. Doses were reduced in all but one patient treated with more than one course of farnesyl transferase inhibitor. Responses were assessable in 12 patients. A partial response in one sAML patient and a very transient decrease of blast cell count with normalisation of karyotype in one MDS patient were observed. No relation between improvement of marrow parameters and detected Ras mutations was observed. Lonafarnib alone, administered following our schedule, has shown limited activity in patients with MDS or secondary AML. Gastrointestinal and haematological toxicities appear the limiting toxicity in this population of patients.
尽管在骨髓增生异常综合征(MDS)中常见Ras激活突变,但Ras在MDS自然病程中的作用仍 largely未知。我们前瞻性地研究了 lonafarnib(一种能够通过抑制法尼基转移酶来抑制Ras信号通路的化合物)在MDS或继发性急性髓系白血病(sAML)患者中的疗效和耐受性。Lonafarnib以每日两次、每次200 mg的剂量口服,共三个疗程,每个疗程4周(疗程之间间隔1至4周不治疗)。纳入了16例患者:FAB/RAEB(n = 10)、RAEB-T(n = 2)、sAML(n = 2)和慢性粒单核细胞白血病(CMML;n = 2);WHO/RAEB-1(n = 4)、RAEB-2(n = 5)、AML(n = 5)、CMML(n = 2)。中位年龄为70(53 - 77)岁。11例患者的核型复杂或为中间型,国际预后评分系统(IPSS)风险组中,2例患者为低危,1例患者为INT-1,4例患者为INT-2,6例患者为高危(3例患者未知或不适用)。在14例接受检测的患者中,5例患者的N-Ras、K-Ras或H-Ras的第12、13或61密码子存在Ras突变。1例患者因违反方案被排除在分析之外,15例患者可评估耐受性。胃肠道毒性(腹泻、恶心和厌食)和骨髓抑制是主要的副作用。其他毒性包括感染、疲劳、肝酶升高、心律失常和皮疹。1例患者死于感染,另1例出现房颤的患者停止了治疗。除1例接受多个疗程法尼基转移酶抑制剂治疗的患者外,所有患者均降低了剂量。12例患者可评估反应。观察到1例sAML患者出现部分缓解,1例MDS患者原始细胞计数非常短暂地下降且核型正常化。未观察到骨髓参数改善与检测到的Ras突变之间的关联。按照我们的方案单独使用Lonafarnib,在MDS或继发性AML患者中显示出有限的活性。胃肠道和血液学毒性似乎是该患者群体中的限制性毒性。
