速释/缓释金刚烷胺（OS320）治疗左旋多巴诱导的异动症帕金森病：随机对照ALLAY-LID研究分析

Immediate-release/extended-release amantadine (OS320) to treat Parkinson's disease with levodopa-induced dyskinesia: Analysis of the randomized, controlled ALLAY-LID studies.

作者信息

Rascol Olivier, Tönges Lars, deVries Tina, Jaros Mark, Quartel Adrian, Jacobs David

机构信息

University of Toulouse 3, University Hospital of Toulouse, INSERM, Clinical Investigation Center CIC1436, Parkinson Expert Center, Department of Neurology and Department of Clinical Pharmacology, NS- Park/FCRIN Network et Centre of Excellence for Neurodegenerative Disorders (COEN) of Toulouse, Toulouse, France.

Ruhr-University Bochum, St. Josef-Hospital, Department of Neurology, Bochum, Germany; Ruhr-University Bochum, Center for Protein Diagnostics (ProDi), Experimental Neurology, Bochum, Germany.

出版信息

Parkinsonism Relat Disord. 2022 Mar;96:65-73. doi: 10.1016/j.parkreldis.2022.01.022. Epub 2022 Feb 8.

DOI:10.1016/j.parkreldis.2022.01.022

PMID:35227940

Abstract

BACKGROUND

Immediate-release (IR) amantadine has been used for treatment of levodopa induced dyskinesia (LID). The immediate-release/extended-release (IR/ER) amantadine formulation OS320 (OSMOLEX ER®) contains an IR outer layer and ER core for once-daily dosing.

OBJECTIVE

Report individual and pooled results for the similarly designed double-blind, placebo-controlled ALLAY-LID I and II trials, assessing IR/ER-amantadine for LID.

METHODS

PD patients with LID were randomized to IR/ER-amantadine 193 mg, 258 mg, or placebo. Primary endpoint was Unified Dyskinesia Rating Scale (UDysRS) score change from baseline to Day 98. Secondary outcome was ON time without troublesome dyskinesia based on diaries. Exploratory outcomes were other diary states (including OFF), MDS-UPDRS Parts II + III and Fatigue Severity Scale.

RESULTS

Overall, 222 individuals enrolled (N = 87 ALLAY-LID I, N = 135 ALLAY-LID II); both trials terminated early for sponsor's decision. While ALLAY-LID I did not meet its primary endpoint, a significant reduction in UDysRS scores versus placebo was observed in ALLAY-LID II for both 193 mg and 258 mg doses. In the pooled analysis, placebo-adjusted UDysRS score differences were -5.5 [-9.8, -1.2], p = 0.012 and -5.2 [-9.5, -0.9], p = 0.017, respectively. IR/ER-amantadine 258 mg significantly increased time spent ON without troublesome dyskinesia in ALLAY-LID II and pooled analysis. Reductions in ON time with dyskinesia supported the primary outcome. There was no effect on OFF time or other outcomes. Overall, 13.3% (193 mg), 18.7% (258 mg) and 11.1% (placebo) discontinued for adverse events, most commonly hallucinations (4.0%, 10.7%, and 1.4%, respectively).

CONCLUSIONS

IR/ER-amantadine significantly reduced LID in ALLAY-LID II but not in ALLAY-LID I; post-hoc pooled data also indicated a positive treatment effect on LID.

摘要

背景

速释金刚烷胺已用于治疗左旋多巴诱导的异动症（LID）。速释/缓释（IR/ER）金刚烷胺制剂OS320（OSMOLEX ER®）包含速释外层和缓释核心，每日给药一次。

目的

报告设计相似的双盲、安慰剂对照的ALLAY-LID I和II试验的个体及汇总结果，评估IR/ER-金刚烷胺治疗LID的效果。

方法

患有LID的帕金森病患者被随机分为接受193毫克、258毫克的IR/ER-金刚烷胺或安慰剂治疗。主要终点是统一异动症评定量表（UDysRS）从基线到第98天的评分变化。次要结果是根据日记记录的无困扰异动症的“开”期时间。探索性结果是其他日记状态（包括“关”期）、MDS-UPDRS第二部分+第三部分以及疲劳严重程度量表。

结果

总体而言，共有222人入组（ALLAY-LID I中87人，ALLAY-LID II中135人）；两项试验均因申办方的决定提前终止。虽然ALLAY-LID I未达到其主要终点，但在ALLAY-LID II中，193毫克和258毫克剂量的IR/ER-金刚烷胺与安慰剂相比均观察到UDysRS评分显著降低。在汇总分析中，安慰剂调整后的UDysRS评分差异分别为-5.5[-9.8，-1.2]，p = 0.012和-5.2[-9.5，-0.9]，p = 0.017。在ALLAY-LID II和汇总分析中，258毫克的IR/ER-金刚烷胺显著增加了无困扰异动症的“开”期时间。伴有异动症的“开”期时间减少支持了主要结果。对“关”期时间或其他结果无影响。总体而言，13.3%（193毫克）、18.7%（258毫克）和11.1%（安慰剂）因不良事件停药，最常见的是幻觉（分别为4.0%、10.7%和1.4%）。