Le Page Emmanuelle, Leray Emmanuelle, Taurin Grégory, Coustans Marc, Chaperon Jacques, Morrissey Sean P, Edan Gilles
Service de Neurologie, Hôpital Pontchaillou, rue Henri Le Guilloux, 35 033 Rennes Cedex, France.
J Neurol Neurosurg Psychiatry. 2008 Jan;79(1):52-6. doi: 10.1136/jnnp.2007.124958. Epub 2007 Sep 10.
Mitoxantrone was approved by the French health authority (AFSAPPS) in October 2003 to treat patients with aggressive multiple sclerosis (MS).
To report the long term effectiveness and safety of mitoxantrone as induction therapy in patients with aggressive relapsing-remitting MS, and to assess treatment response factors.
100 consecutive patients with aggressive relapsing-remitting MS received mitoxantrone 20 mg monthly combined with methylprednisolone 1 g for 6 months. Relapses, Expanded Disability Status Scale (EDSS) and drug safety were assessed every 6 months for up to at least 5 years. Within 6 months after induction, 73 patients received maintenance therapy (mitoxantrone every 3 months (n = 21); interferon beta (n = 25); azathioprine (n = 15); methotrexate (n = 7); glatiramer acetate (n = 5)).
During the 12 months following initiation of mitoxantrone, the annual relapse rate (ARR) was reduced by 91%, 78% of patients remained relapse free, MRI activity was reduced by 89%, the mean EDSS decreased by 1.2 points (p<10(-6)) and 64% of patients improved by 1 point or more on the EDSS. In the longer term, the ARR reduction was sustained (0.29-0.42 for up to 5 years), the median time to the first relapse was 2.8 years and disability remained improved after 5 years. Younger age and lower EDSS score at the start of mitoxantrone treatment were predictive of better treatment response. Three patients presented with an asymptomatic decrease in left ventricular ejection fraction to less than 50% (one reversible). One patient was diagnosed with acute myeloid leukaemia (remission 5 years after diagnosis).
Mitoxantrone monthly for 6 months as induction therapy followed by maintenance treatment showed sustained clinical benefit for up to 5 years with an acceptable adverse events profile in patients with aggressive relapsing-remitting MS.
米托蒽醌于2003年10月获法国卫生当局(AFSAPPS)批准,用于治疗侵袭性多发性硬化症(MS)患者。
报告米托蒽醌作为侵袭性复发缓解型MS患者诱导治疗的长期有效性和安全性,并评估治疗反应因素。
100例连续的侵袭性复发缓解型MS患者每月接受20mg米托蒽醌联合1g甲泼尼龙治疗6个月。每6个月评估复发情况、扩展残疾状态量表(EDSS)及药物安全性,为期至少5年。诱导治疗后6个月内,73例患者接受维持治疗(每3个月一次米托蒽醌(n = 21);干扰素β(n = 25);硫唑嘌呤(n = 15);甲氨蝶呤(n = 7);醋酸格拉替雷(n = 5))。
在开始使用米托蒽醌后的12个月内,年复发率(ARR)降低了91%,78%的患者无复发,MRI活动减少了89%,平均EDSS降低了1.2分(p<10(-6)),64%的患者EDSS改善1分或更多。从长期来看,ARR降低得以维持(长达5年为0.29 - 0.42),首次复发的中位时间为2.8年,5年后残疾状况仍有改善。米托蒽醌治疗开始时年龄较小和EDSS评分较低预示着治疗反应较好。3例患者出现左心室射血分数无症状性下降至低于50%(1例可逆)。1例患者被诊断为急性髓系白血病(诊断后5年缓解)。
对于侵袭性复发缓解型MS患者,米托蒽醌每月治疗6个月作为诱导治疗随后进行维持治疗,显示出长达5年的持续临床获益,且不良事件情况可接受。
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