[米托蒽醌作为侵袭性复发缓解型多发性硬化症的诱导疗法:对100例连续患者的描述性分析]
[Mitoxantrone as induction therapy in aggressive relapsing remitting multiple sclerosis: a descriptive analysis of 100 consecutive patients].
作者信息
Le Page E, Leray E, Taurin G, Coustans M, Chaperon J, Edan G
机构信息
Service de Neurologie, Hôpital Pontchaillou, Rennes.
出版信息
Rev Neurol (Paris). 2006 Feb;162(2):185-94. doi: 10.1016/s0035-3787(06)74998-0.
INTRODUCTION
On the basis of the French and British (FB) MS Trial, Mitoxantrone (MITOX) was approved by the AFSAPPS in October 2003 in patients with aggressive multiple sclerosis (MS), given as induction therapy monthly for 6 months (ELSEP). We report an observational study of 100 aggressive relapsing remitting (RR) MS patients treated by induction therapy with MITOX and followed up to 5 years.
METHODS
One hundred patients with aggressive RR MS received an induction therapy with MITOX 20 mg monthly combined with methylprednisolone 1 g for 6 months. MRI data within 12 months before and 6 months after MITOX induction were collected (mean cumulative dose 65 mg/m2). Clinical evaluation was performed every 6 months and data (relapses and EDSS scores) were prospectively recorded in the EDMUS Database. After MITOX, a maintenance therapy was given to 57 patients (MITOX every 3 months: 21; Interferon beta: 13; Azathioprine: 14; Methotrexate: 7; Glatiramer acetate: 2). The mean follow-up period was of 3.8 years.
RESULTS
Patients were treated at a mean age of 27 +/- 9 years after 5 +/- 3 years of MS duration. Within the 12 months preceding MITOX onset, the annual relapse rate (ARR) was 3.2, the mean EDSS increased by 2.2 +/- 1 points (to a score of 4 at M0), 87 patients worsened by 1 point EDSS or more and 85 percent of patients had Gd enhancing lesions on MRI. During the 12 months following MITOX onset, the inflammatory activity of the disease dropped dramatically with a reduction of the ARR by 91 percent whereas 76 percent of patients were free of new relapse and MRI activity was reduced by 89 percent. In addition, the mean EDSS decreased by 1.2 points (p<10-6) and 60 percent of patients improved by 1 point EDSS or more. At a longer term, the reduction of the ARR was confirmed (0.28-0.37 up to 5 years) and the median time to the first relapse was 2.8 years. A significant improvement of disability was maintained until 4 years and got back to the initial level at year 5. The ARR was significantly lower (0.09) for patients treated with MITOX every 3 months as maintenance therapy than for patients treated by other disease modifying therapies (0.33-0.39) or not (0.43) after the induction. Three patients presented an asymptomatic decrease of the left ventricular ejection fraction under 50 percent, reversible in one case.
CONCLUSION
MITOX as induction therapy monthly for 6 months was safe and had a rapid and strong impact on the inflammatory process and on the evolution of disability. The drug might be a good candidate as induction therapy followed by a maintenance therapy in patients with aggressive MS.
引言
基于法国和英国(FB)多发性硬化症试验,米托蒽醌(MITOX)于2003年10月被法国药品安全局批准用于治疗侵袭性多发性硬化症(MS)患者,作为诱导疗法,每月给药一次,共6个月(ELSEP)。我们报告了一项对100例接受MITOX诱导疗法治疗并随访5年的侵袭性复发缓解型(RR)MS患者的观察性研究。
方法
100例侵袭性RR MS患者接受了每月20 mg MITOX联合1 g甲基强的松龙的诱导疗法,为期6个月。收集了MITOX诱导前12个月内和诱导后6个月内的MRI数据(平均累积剂量65 mg/m²)。每6个月进行一次临床评估,并将数据(复发情况和扩展残疾状态量表[EDSS]评分)前瞻性记录在EDMUS数据库中。MITOX治疗后,57例患者接受了维持治疗(每3个月一次MITOX:21例;干扰素β:13例;硫唑嘌呤:14例;甲氨蝶呤:7例;醋酸格拉替雷:2例)。平均随访期为3.8年。
结果
患者在MS病程5±3年后接受治疗,平均年龄为27±9岁。在MITOX开始前的12个月内,年复发率(ARR)为3.2,平均EDSS增加2.2±1分(在M0时评分为4分),87例患者EDSS恶化1分或更多,85%的患者MRI上有钆增强病灶。在MITOX开始后的12个月内,疾病的炎症活动显著下降,ARR降低了91%,而76%的患者无新的复发,MRI活动降低了89%。此外,平均EDSS下降了1.2分(p<10⁻⁶),60%的患者EDSS改善1分或更多。从长期来看,ARR的降低得到了证实(直至5年时为0.28 - 0.37),首次复发的中位时间为2.8年。残疾状况的显著改善一直维持到4年,并在第5年恢复到初始水平。作为维持治疗,每3个月接受一次MITOX治疗的患者的ARR(0.09)显著低于诱导后接受其他疾病修饰疗法(0.33 - 0.39)或未接受维持治疗(0.43)的患者。3例患者出现左心室射血分数无症状性下降至50%以下,其中1例可逆。
结论
每月一次共6个月的MITOX诱导疗法是安全的,对炎症过程和残疾进展有迅速且强烈的影响。该药物可能是侵袭性MS患者诱导治疗后进行维持治疗的良好选择。
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