Voso Maria Teresa, Santini Valeria, Finelli Carlo, Musto Pellegrino, Pogliani Enrico, Angelucci Emanuele, Fioritoni Giuseppe, Alimena Giuliana, Maurillo Luca, Cortelezzi Agostino, Buccisano Francesco, Gobbi Marco, Borin Lorenza, Di Tucci Anna, Zini Gina, Petti Maria Concetta, Martinelli Giovanni, Fabiani Emiliano, Fazi Paola, Vignetti Marco, Piciocchi Alfonso, Liso Vincenzo, Amadori Sergio, Leone Giuseppe
Istituto di Ematologia, Universita Cattolica S. Cuore, Rome, Italy.
Clin Cancer Res. 2009 Aug 1;15(15):5002-7. doi: 10.1158/1078-0432.CCR-09-0494. Epub 2009 Jul 28.
Epigenetic changes play a role and cooperate with genetic alterations in the pathogenesis of myelodysplastic syndromes (MDS). We conducted a phase II multicenter study on the combination of the DNA-methyltransferase inhibitor 5-azacytidine (5-AZA) and the histone deacetylase inhibitor valproic acid (VPA) in patients with higher risk MDS.
We enrolled 62 patients with MDS (refractory anemia with excess blasts, 39 patients; refractory anemia with excess blasts in transformation, 19 patients; and chronic myelomanocytic leukemia (CMML), 4 patients) and an International Prognostic Scoring System (IPSS) rating of Intermediate-2 (42 patients) or high (20 patients). VPA was given to reach a plasma concentration of >50 microg/mL, then 5-AZA was added s.c. at 75 mg/m(2) for 7 days in eight monthly cycles.
The median overall survival was 14.4 months. At a median follow-up of 12 months (range, 0.7-21.0), the disease progressed in 20 patients, with 21% cumulative incidence of progression. Of 26 patients who completed eight cycles, 30.7% obtained complete or partial remission, 15.4% had a major hematologic improvement, whereas 38.5% showed stable disease. Drug-related toxicity was mild. Favorable prognostic factors for survival were IPSS Intermediate-2 and plasma VPA of > or =50 microg/mL (log rank = 0.013 and 0.007, respectively). Analysis of polymorphisms important for the metabolism of the drugs used in the trial showed that carriers of the CYP2C19*2 variant of cytochrome P450 required higher VPA doses to achieve the target VPA plasma concentration of 50 microg/mL on day 1 of 5-AZA treatment (P = 0.0021).
Our data show that the 5-AZA/VPA combination is active and safe in patients with MDS with a poor prognosis. Achievement of VPA therapeutic levels may indeed increase 5-AZA efficacy.
表观遗传学改变在骨髓增生异常综合征(MDS)的发病机制中发挥作用,并与基因改变相互协作。我们开展了一项II期多中心研究,探究DNA甲基转移酶抑制剂5-氮杂胞苷(5-AZA)与组蛋白去乙酰化酶抑制剂丙戊酸(VPA)联合应用于高危MDS患者的疗效。
我们纳入了62例MDS患者(难治性贫血伴原始细胞增多,39例;难治性贫血伴原始细胞增多转化型,19例;慢性粒-单核细胞白血病(CMML),4例),国际预后评分系统(IPSS)评分为中危-2(42例)或高危(20例)。给予VPA使血浆浓度>50μg/mL,然后在八个月周期内,于第1天皮下注射5-AZA,剂量为75mg/m²,共7天。
中位总生存期为14.4个月。中位随访12个月(范围0.7 - 21.0)时,20例患者疾病进展,累积进展发生率为21%。在26例完成八个周期治疗的患者中,30.7%获得完全或部分缓解,15.4%有主要血液学改善,而38.5%疾病稳定。药物相关毒性较轻。生存的有利预后因素为IPSS中危-2以及血浆VPA≥50μg/mL(对数秩检验分别为0.013和0.007)。对试验中所用药物代谢重要的多态性分析表明,细胞色素P450 CYP2C19*2变异体携带者在5-AZA治疗第1天需要更高的VPA剂量才能达到50μg/mL的目标VPA血浆浓度(P = 0.0021)。
我们的数据表明,5-AZA/VPA联合方案对预后不良的MDS患者有效且安全。达到VPA治疗水平可能确实会提高5-AZA的疗效。
