米格列醇治疗对早婴儿尼曼-匹克病 C 型神经障碍和生存的影响:一项全国性的法国回顾性研究。
Effects of miglustat therapy on neurological disorder and survival in early-infantile Niemann-Pick disease type C: a national French retrospective study.
机构信息
Department of Paediatric Neurology, Reference Centre for Lysosomal Diseases, Armand Trousseau-La Roche Guyon Hospital and Hospital-University I2-D2 Federation, Sorbonne-Université, Paris, France.
Department of Paediatrics, Jean Verdier University Hospital, Bondy, France.
出版信息
Orphanet J Rare Dis. 2023 Jul 21;18(1):204. doi: 10.1186/s13023-023-02804-4.
BACKGROUND
Niemann-Pick disease type C (NP-C) is a rare neurovisceral lysosomal lipid storage disease characterized by progressive neurodegeneration and premature death. While miglustat can stabilize neurological manifestations in later onset forms of NP-C, its efficacy in the early-infantile neurological form has not been demonstrated. In this observational retrospective study, we compared long-term neurodevelopmental outcome and survival between an untreated and a treated group of early infantile NP-C patients.
METHODS
Data available on all NP-C patients with early infantile neurological onset diagnosed in France between 1990 and 2013 were compiled. Patients with incomplete data or who had died from a systemic perinatal, rapidly fatal form were excluded.
RESULTS
Ten patients were included in the treated group (year of birth: 2006-2012), and 16 patients in the untreated group [born 1987-2005 (n = 15), 2012 (n = 1)]. The median age at neurological onset was 9 months (5-18) in the treated group, and 12 months (3-18) in the untreated group (p = 0.22). Miglustat therapy was started at a median age of 24.5 months (9-29) and median duration was 30 months (11-56). Gastrointestinal adverse events were reported in 7/10 patients on miglustat. All patients developed loss of psychomotor acquisitions or additional neurological symptoms despite miglustat therapy. The ages of developmental milestones and neurological involvement did not significantly differ between the two groups. Four patients in the untreated group were lost to follow up. The 22 remaining patients had died by the end of the study and no patient survived beyond the age of 7.4 years. The median survival age was 4.42 years in the untreated group and 5.56 years in the treated group; the Kaplan-Meier survival curves were not significantly different (log-rank test: p = 0.11).
CONCLUSIONS
Miglustat allowed no significant long-term neurodevelopmental improvement nor significant increase of survival in patients with early infantile NP-C.
背景
尼曼-匹克病 C 型(NP-C)是一种罕见的神经内脏溶酶体脂质贮积病,其特征为进行性神经退行性变和过早死亡。虽然米格列奈特可稳定 NP-C 晚发型的神经表现,但尚未证明其在早发型神经型中的疗效。在这项观察性回顾性研究中,我们比较了未经治疗和治疗的早发型 NP-C 患者的长期神经发育结局和存活率。
方法
收集了 1990 年至 2013 年间在法国诊断为早发型神经发病的所有 NP-C 患者的数据。排除数据不完整或死于全身围产期、迅速致命型的患者。
结果
10 例患者纳入治疗组(出生年份:2006-2012 年),16 例患者纳入未治疗组[1987-2005 年出生(n=15),2012 年出生(n=1)]。治疗组的神经发病中位年龄为 9 个月(5-18 个月),未治疗组为 12 个月(3-18 个月)(p=0.22)。米格列奈特治疗中位年龄为 24.5 个月(9-29 个月),中位持续时间为 30 个月(11-56 个月)。7/10 例米格列奈特治疗患者出现胃肠道不良事件。尽管接受米格列奈特治疗,所有患者仍出现精神运动发育丧失或其他神经症状。两组的发育里程碑和神经受累年龄无显著差异。未治疗组有 4 例失访。其余 22 例患者在研究结束时死亡,无患者存活至 7.4 岁以上。未治疗组的中位生存年龄为 4.42 岁,治疗组为 5.56 岁;Kaplan-Meier 生存曲线无显著差异(对数秩检验:p=0.11)。
结论
米格列奈特不能显著改善早发型 NP-C 患者的长期神经发育,也不能显著提高生存率。
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