McCance Center for Brain Health and Department of Neurology, Massachusetts General Hospital, Boston, MA, 02114, USA.
Stanley Center for Psychiatric Research, Broad Institute, Cambridge, MA, 02142, USA.
Sci Rep. 2022 Oct 21;12(1):17708. doi: 10.1038/s41598-022-21820-1.
Neurodegenerative disease is increasingly prevalent and remains without disease-modifying therapies. Engaging the right target, at the right disease stage, could be an important determinant of success. We annotated targets and eligibility criteria for 3238 neurodegenerative disease trials registered at ClinicalTrials.gov from 2000 to 2020. Trials became more selective as the mean number of inclusion and exclusion criteria increased and eligible score ranges shrank. Despite a shift towards less impaired participants, only 2.7% of trials included pre-symptomatic individuals; these were depleted for drug trials and enriched for behavioral interventions. Sixteen novel, genetically supported therapeutic hypotheses tested in drug trials represent a small, non-increasing fraction of trials, and the mean lag from genetic association to first trial was 13 years. Though often linked to disease initiation, not progression, these targets were tested mostly at symptomatic disease stages. The potential for disease modification through early intervention against root molecular causes of disease remains largely unexplored.
神经退行性疾病的发病率日益增高,但目前仍缺乏可改变疾病进程的疗法。能否针对正确的靶点、在疾病的恰当阶段开展治疗,可能是决定成败的关键因素。我们对 2000 年至 2020 年期间在 ClinicalTrials.gov 注册的 3238 项神经退行性疾病临床试验的靶点和纳入标准进行了标注。随着纳入和排除标准数量的增加,以及合格评分范围的缩小,临床试验的选择性逐渐增强。尽管研究对象的认知障碍程度有所降低,但只有 2.7%的试验纳入了无症状个体;这些试验主要针对药物试验,而行为干预试验则倾向于纳入有症状的个体。在药物试验中,有 16 个新的、有遗传学依据的治疗假设得到了检验,但从遗传关联到首次试验的平均时间滞后为 13 年。这些靶点虽然通常与疾病的起始而非进展有关,但大多在有症状的疾病阶段进行了检测。通过早期干预针对疾病根本的分子病因来实现疾病改善的潜力在很大程度上仍未得到探索。
Zotero 插件
