A.1 Repurposing Ambroxol as a disease-modifying treatment for Parkinson’s disease dementia: A phase 2, randomized, double blind placebo-controlled trial

SH Pasternak, C. Silveira, K. Coleman, M. Borrie, J. Wells, E. Finger, R. Bartha, M. Jog, M. Jenkins, P. MacDonald, G. Zou, S. Stukas, C. Wellington, R. Tirona, T. Rupar
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Abstract

Background: Currently there are no disease modifying treatment for Synucleinopathies including Parkinson’s disease Dementia (PDD). Carrying a mutation in the GBA gene (beta-glucocerebrosidase/ GCAse) is a leading risk factor for synucleinopathies. Raising activity GCAse lowers α-synuclein levels in cells and animal models. Ambroxol is a pharmacological chaperone for GCAse and can raise GCAse levels. Our goal is to test Ambroxol as a disease-modifying treatment in PDD. Methods: We randomized fifty-five individuals with PDD to Ambroxol 1050mg/day, 525mg/day, or placebo for 52 weeks. Primary outcome measures included safety, Alzheimer’s disease Assessment Scale-cognitive (ADAS-Cog) subscale and the Clinician’s Global Impression of Change (CGIC). Secondary outcomes included pharmacokinetics, cognitive and motor outcomes and and plasma and CSF biomarkers. Results: Ambroxol was well tolerated. There were 7 serious adverse events (SAEs) none deemed related to Ambroxol. GCase activity was increased in white blood cells by ~1.5 fold. There were no differences between groups on primary outcome measures. Patients receiving high dose Ambroxol appeared better on the Neuropsychiatric Inventory. GBA carriers appeared to improve on some cognitive tests. pTau 181 was reduced in CSF. Conclusions: Ambroxol was safe and well-tolerated in PDD. Ambroxol may improve biomarkers and cognitive outcomes in GBA1 mutation carrie.rs Ambroxol improved some biomarkerss. ClinicalTrials.gov NCT02914366
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A.1 将氨溴索重新用作帕金森病痴呆症的疾病调节疗法:2期随机双盲安慰剂对照试验
背景:目前还没有针对包括帕金森病痴呆症(PDD)在内的突触核蛋白病的治疗方法。携带 GBA 基因(β-葡糖脑苷脂/GCAse)突变是突触核蛋白病的主要风险因素。提高 GCAse 的活性可降低细胞和动物模型中的α-突触核蛋白水平。氨溴索是 GCAse 的药理伴侣,可以提高 GCAse 的水平。我们的目标是测试氨溴索是否可作为治疗 PDD 的疾病调节剂。方法:我们将 55 名 PDD 患者随机分配到氨溴索 1050 毫克/天、525 毫克/天或安慰剂中,为期 52 周。主要结果指标包括安全性、阿尔茨海默病评估量表-认知(ADAS-Cog)分量表和临床医生总体变化印象(CGIC)。次要结果包括药代动力学、认知和运动结果以及血浆和脑脊液生物标志物。研究结果氨溴索耐受性良好。共发生了 7 起严重不良事件 (SAE),均与氨溴索无关。白细胞中的 GCase 活性增加了约 1.5 倍。各组在主要结果指标上没有差异。接受大剂量氨溴索治疗的患者在神经精神量表方面表现较好。脑脊液中的 pTau 181 有所降低。结论氨溴索对PDD患者安全且耐受性良好。氨溴索可改善GBA1突变携带者的生物标志物和认知结果。ClinicalTrials.gov NCT02914366
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