J05 Legato-hd研究:一项评估拉喹莫德治疗亨廷顿病的有效性和安全性的2期研究

Journal of Neurology, Neurosurgery & Psychiatry Pub Date : 2018-09-01 DOI:10.1136/jnnp-2018-ehdn.265

R. Reilmann, M. Gordon, K. Anderson, A. Feigin, S. Tabrizi, B. Leavitt, J. Stout, P. Piccini, Gail Rynkowski, Rita Volkinshtein, J. Savola

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引用次数: 3

摘要

Laquinimod (Teva Pharmaceuticals)是一种口服活性小分子，可被动进入血脑屏障，已被证明可上调BDNF分泌并调节参与HD病理的中枢神经系统炎症通路。LEGATO-HD研究最初包括三个剂量组，0.5 mg, 1.0 mg和1.5 mg与安慰剂相比，在一项为期12个月的多中心双盲2期研究中，HD患者。在多发性硬化症研究中，使用剂量分别为1.2 mg和1.5 mg的拉喹莫德观察到心血管安全性问题。虽然在LEGATO-HD中没有发现类似的问题，但梯瓦公司于2016年1月停止了1.5毫克的治疗组，作为一项预防性安全措施，并继续评估0.5毫克和1.0毫克剂量的疗效和安全性。目的评价拉喹莫德治疗亨廷顿病(HD)的疗效和安全性。方法疗效评估包括主要终点，12个月时统一亨廷顿病评定量表总运动评分(UHDRS-TMS)从基线的变化，以及次要终点，12个月时尾状核体积的百分比变化。安全措施包括不良事件报告、临床实验室检查、生命体征、心电图、体格检查和自杀(C-SSRS)。LEGATO-HD完全入组了352名随机患者，预计将于2018年6月完成。入组患者的基线平均(SD)汇总统计数据包括女性172人(49.1%)，男性178人(50.9%)，年龄44.4(7.6)岁，UHDRS-TMS 24.3(13.1)， uhdrs -总功能容量(TFC) 11.1(1.7)， uhdrs -功能评估(FA) 22.7(2.4)。主要和次要疗效终点和安全措施的结果将在会议上公布。结论改善HD患者症状进展和神经退行性变的医学需求仍未得到满足。LEGATO-HD为了解拉喹莫德作为HD患者潜在治疗方法的有效性和安全性提供了有价值的信息。LEGATO-HD研究由梯瓦制药有限公司与HSG和EHDN合作赞助，注册号为NCT02215616-clinicaltrials.gov和2014-000418-75-EudraCT。

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J05 Legato-hd study: a phase 2 study assessing the efficacy and safety of laquinimod as a treatment for huntington disease

Introduction Laquinimod (Teva Pharmaceuticals) is an orally active small molecule that passively enters the blood brain barrier and has been shown to upregulate BDNF secretion and modulate CNS-resident inflammatory pathways involved in pathology of HD. The LEGATO-HD study originally included three dose arms, 0.5 mg, 1.0 mg and 1.5 mg versus placebo in a 12-month multicenter double blind phase 2 study in patients with HD. Cardiovascular safety concerns were observed in multiple sclerosis studies with laquinimod doses of 1.2 mg and 1.5 mg. Although no similar concern was identified in LEGATO-HD, Teva discontinued the 1.5 mg arm in January 2016 as a precautionary safety measure and continued to evaluate the efficacy and safety of the 0.5 mg and 1.0 mg doses. Aims Evaluate the efficacy and safety of laquinimod in patients with Huntington Disease (HD). Methods Efficacy assessments include the primary endpoint, change from baseline in Unified Huntington’s Disease Rating Scale Total Motor Score (UHDRS-TMS) at month 12, and the secondary endpoint, percent change in caudate volume at month 12. Safety measures include adverse event reporting, clinical laboratory tests, vital signs, ECGs, physical examinations, and suicidality (C-SSRS). Results LEGATO-HD is fully enrolled with 352 patients randomized and is expected to complete in June 2018. Baseline mean (SD) pooled demographics of enrolled patients include females n=172 (49.1%), males n=178 (50.9%), age 44.4(7.6) years, UHDRS-TMS 24.3(13.1), UHDRS-Total Functional Capacity (TFC) 11.1(1.7), and UHDRS-Functional Assessment (FA) 22.7(2.4). The results of the primary and secondary efficacy endpoints and safety measures will be presented at the conference. Conclusion There is a significant unmet medical need to ameliorate the progression of symptoms and the neurodegeneration in HD. LEGATO-HD provides valuable information towards understanding the efficacy and safety of laquinimod as a potential treatment for patients with HD. The LEGATO-HD Study is sponsored by Teva Pharmaceuticals Ltd in collaboration with HSG and EHDN and is registered as NCT02215616-clinicaltrials.gov and 2014–000418–75-EudraCT.

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Journal of Neurology, Neurosurgery & Psychiatry

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