Masaoka T, Shibata H, Oguma S, Nagai K, Kitani T, Horiuchi A, Yasunaga K, Yonezawa T, Kawagoe H
Invest New Drugs. 1985;3(2):197-201. doi: 10.1007/BF00174170.
A phase II study of mitoxantrone (Novantrone; dihydroxyanthracenedione) was conducted in 35 patients (22 male: 13 female) with acute leukemia. There were 35 evaluable cases with a mean age of 34 (range 8-61). Twenty-eight patients had acute non-lymphocytic leukemia (ANLL) and seven had acute lymphocytic leukemia (ALL). Mitoxantrone was administered intravenously 2-4 mg/m2 daily for five days and after the nadir a further 2-3 doses were added if necessary. All previously treated cases (22 patients) had been treated with anthracyclines; 13 had no previous treatment. Out of the 13 untreated cases there were six complete remissions (CRs) (46.2%) and five partial remissions (PRs) (38.5%), while out of 22 pretreated cases, four CRs (18.2%) and five PRs (22.7%) were obtained. In seven of the untreated cases the decrease of leukemic cells and neutrophil leukocytes were analysed. Mitoxantrone showed a longer duration of decrease and higher log decrease of leukemic cells in the bone marrow than daunorubicin or cytosine arabinoside. Seventy-three percent of patients showed gastrointestinal disturbances such as nausea or loss of appetite. In 38.1% SGPT elevation and in 8.8% abnormal ECG findings were observed. All side-effects were mild and reversible. From this data mitoxantrone seems a very promising agent in the treatment of acute leukemia and a phase III study is now being carried out.
对35例急性白血病患者(22例男性,13例女性)进行了米托蒽醌(诺凡托;二羟基蒽二酮)的II期研究。有35例可评估病例,平均年龄34岁(范围8 - 61岁)。28例患者患有急性非淋巴细胞白血病(ANLL),7例患有急性淋巴细胞白血病(ALL)。米托蒽醌静脉注射,每日2 - 4mg/m²,共5天,在最低点后如有必要再追加2 - 3剂。所有先前接受过治疗的病例(22例患者)均接受过蒽环类药物治疗;13例未曾接受过治疗。在13例未治疗的病例中,有6例完全缓解(CR)(46.2%),5例部分缓解(PR)(38.5%),而在22例先前接受过治疗的病例中,获得4例CR(18.2%)和5例PR(22.7%)。在7例未治疗的病例中分析了白血病细胞和中性粒细胞的减少情况。与柔红霉素或阿糖胞苷相比,米托蒽醌在骨髓中显示出白血病细胞减少持续时间更长且对数减少更高。73%的患者出现恶心或食欲不振等胃肠道不适。观察到38.1%的患者谷丙转氨酶升高,8.8%的患者心电图异常。所有副作用均轻微且可逆。根据这些数据,米托蒽醌似乎是治疗急性白血病非常有前景的药物,目前正在进行III期研究。
