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IMPORTANCE

Carrying a variation in the gene for β-glucocerebrosidase is a major risk factor for Parkinson disease dementia (PDD), and raising β-glucocerebrosidase levels lowers α-synuclein in cell and animals. Ambroxol is a chaperone for β-glucocerebrosidase, which increases the levels of β-glucocerebrosidase.

OBJECTIVE

To examine the safety and tolerability of ambroxol in PDD, test the efficacy of ambroxol in improving or slowing the progression of cognitive deficits, and acquire pharmacological data.

DESIGN, SETTING, AND PARTICIPANTS: This was a 52-week, phase 2, double-blind, placebo-controlled, randomized clinical trial conducted from February 2015 to June 2023. The study took place at a single center and was referral based. Included were patients with PDD who were older than 50 years, had Parkinson disease for at least 1 year before cognitive impairment, had mild to moderate dementia, were taking stable medications, and had a study partner.

INTERVENTIONS

Ambroxol low dose (525 mg per day), high dose (1050 mg per day), or placebo.

MAIN OUTCOMES AND MEASURES

Safety and tolerability outcomes were adverse events. Primary efficacy outcomes were the Alzheimer Disease Assessment Scale-cognitive subscale, version 13 (ADAS-Cog-13) and Clinician's Global Impression of Change (CGIC).

RESULTS

A total of 75 patients were screened, and 55 were randomized. Thirty-one individuals received ambroxol, with 8 patients (mean [SD] age, 78.8 [3.4] years, all male) in the low-dose group and 22 patients (mean [SD] age, 70.7 [7.6]; 19 male [86.4%]) in the high-dose group. One patient was excluded from the high-dose group due to a diagnosis of progressive supranuclear palsy. A total of 24 patients (mean [SD] age, 72.7 [6.3] years; 19 male [79.2%]) were included in the placebo group. Participants receiving ambroxol (23 of 193 adverse events [12%]) showed more gastrointestinal adverse events than those receiving placebo (9 of 172 adverse events [5%]). Statistical analyses compared ambroxol high dose vs placebo. There was no evidence to suggest differences between groups on primary or secondary outcomes. Mean (SD) ambroxol high-dose concentrations were 7.48μM (3.17μM; 95% CI, 6.08-8.87μM) in plasma and 0.73μM (0.07μM; 95% CI, 0.64-0.81μM) in cerebrospinal fluid at the end of titration. Mean (SD) β-glucocerebrosidase levels were higher at week 26 (ambroxol, 12.45 [1.97] nmol/h/mg; 91% CI, 11.54-13.36 nmol/h/mg); placebo, 8.50 [1.96] nmol/h/mg; 91% CI, 7.65-9.34 nmol/h/mg; P = .05) in the ambroxol group compared with placebo.

CONCLUSIONS AND RELEVANCE

Results of this randomized clinical trial reveal that ambroxol was safe, well-tolerated, and demonstrated target engagement. However, the effect of ambroxol on cognition was not confirmed.

TRIAL REGISTRATION

ClinicalTrials.gov Identifier: NCT02914366.

重要性

携带β-葡萄糖脑苷脂酶基因变异是帕金森病痴呆（PDD）的主要危险因素，提高β-葡萄糖脑苷脂酶水平可降低细胞和动物体内的α-突触核蛋白。氨溴索是β-葡萄糖脑苷脂酶的伴侣蛋白，可提高β-葡萄糖脑苷脂酶水平。

目的

研究氨溴索在PDD中的安全性和耐受性，测试氨溴索改善或延缓认知功能障碍进展的疗效，并获取药理学数据。

设计、地点和参与者：这是一项为期52周的2期双盲、安慰剂对照、随机临床试验，于2015年2月至2023年6月进行。该研究在单一中心进行，基于转诊。纳入的PDD患者年龄超过50岁，在认知障碍前帕金森病至少1年，患有轻度至中度痴呆，正在服用稳定的药物，并有一名研究伙伴。

干预措施

氨溴索低剂量（每天525毫克）、高剂量（每天1050毫克）或安慰剂。

主要结局和测量指标

安全性和耐受性结局为不良事件。主要疗效结局为阿尔茨海默病评估量表认知子量表第13版（ADAS-Cog-13）和临床医师总体印象变化（CGIC）。

结果

共筛查75例患者，55例随机分组。31例接受氨溴索治疗，低剂量组8例患者（平均[标准差]年龄，78.8[3.4]岁，均为男性），高剂量组22例患者（平均[标准差]年龄，70.7[7.6]岁；19例男性[86.4%]）。高剂量组有1例患者因诊断为进行性核上性麻痹而被排除。安慰剂组共纳入24例患者（平均[标准差]年龄，72.7[6.3]岁；19例男性[79.2%]）。接受氨溴索治疗的参与者（193例不良事件中的23例[12%]）比接受安慰剂的参与者（172例不良事件中的9例[5%]）出现更多胃肠道不良事件。统计分析比较了氨溴索高剂量组与安慰剂组。没有证据表明两组在主要或次要结局上存在差异。滴定结束时，血浆中氨溴索高剂量平均（标准差）浓度为7.48μM（3.17μM；95%CI，6.08 - 8.87μM），脑脊液中为0.73μM（0.07μM；95%CI，0.64 - 0.81μM）。氨溴索组在第26周时β-葡萄糖脑苷脂酶平均（标准差）水平较高（氨溴索，12.45[1.97]nmol/h/mg；91%CI，11.54 - 13.36 nmol/h/mg）；安慰剂组为8.50[1.96]nmol/h/mg；91%CI，7.65 - 9.34 nmol/h/mg；P = 0.05）。

结论和相关性

这项随机临床试验结果显示，氨溴索安全、耐受性良好，并显示出靶点作用。然而，氨溴索对认知的影响未得到证实。

试验注册

ClinicalTrials.gov标识符：NCT02914366。

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