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神经退行性疾病临床药物研发中的问题

Issues for clinical drug development in neurodegenerative diseases.

作者信息

Dib Michel

机构信息

Service de Neurologie, Hôpital de la Salpêtrière, Paris, France.

出版信息

Drugs. 2005;65(17):2463-79. doi: 10.2165/00003495-200565170-00004.

DOI:10.2165/00003495-200565170-00004
PMID:16296872
Abstract

Neurodegenerative diseases pose specific challenges for drug development. These diseases typically have a slow and variable clinical course, an insidious onset, and symptom expression is only observed when a significant proportion of neurons are already lost. It is important to identify vulnerability factors and other determinants of clinical course in order to be able in the future to select patient populations for clinical trials with a predictable prognosis. The neurodegenerative process itself is not amenable to direct observation and, thus, cannot be monitored in clinical trials. For this reason, surrogate biomarkers are required for use as outcome parameters. In this respect, magnetic resonance imaging has proved valuable for assessing disease activity and progression in multiple sclerosis. Rating scales are of use as outcome measures but, as these generally measure symptom severity, they are most appropriate for use in assessing symptomatic treatments. Survival has been used with success as an outcome measure in trials in amyotrophic lateral sclerosis, where disease progression is rapid. The optimal outcome measure, the sample size required and the treatment duration need to be chosen in relation to the phase of the disease. Potential new treatments can be chosen based upon new knowledge of the genetics and physiopathology of neurodegenerative diseases and, in some cases, screened in transgenic mouse models, although it should be recognised that the validity of these models in terms of treatment response has yet to be established empirically.

摘要

神经退行性疾病给药物研发带来了特殊挑战。这些疾病通常临床病程缓慢且多变,起病隐匿,只有当相当比例的神经元已经丧失时才会观察到症状表现。识别脆弱因素和临床病程的其他决定因素很重要,以便未来能够选择预后可预测的患者群体进行临床试验。神经退行性过程本身无法直接观察,因此在临床试验中无法进行监测。出于这个原因,需要替代生物标志物作为结果参数。在这方面,磁共振成像已被证明对评估多发性硬化症的疾病活动和进展很有价值。评定量表用作结果测量指标,但由于这些量表通常测量症状严重程度,它们最适合用于评估对症治疗。在肌萎缩侧索硬化症的试验中,生存期已成功用作结果测量指标,因为该疾病进展迅速。最佳结果测量指标、所需样本量和治疗持续时间需要根据疾病阶段来选择。潜在的新治疗方法可以根据神经退行性疾病的遗传学和生理病理学新知识来选择,在某些情况下,可在转基因小鼠模型中进行筛选,尽管应该认识到这些模型在治疗反应方面的有效性尚未通过经验得到证实。

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