Jost Wolfgang H, Gluth Ivonne, Lück Jennifer C, Lopes Olga I Fonseca da Cruz
Parkinson-Klinik Ortenau, Wolfach, Germany.
Medical Department, Zambon GmbH, Berlin, Germany.
Curr Med Res Opin. 2023 Dec;39(12):1621-1628. doi: 10.1080/03007995.2023.2234728. Epub 2023 Jul 17.
Parkinson's Disease (PD) is a common progressive neurodegenerative disorder that leads to an imbalance of various neurotransmitters and affects cognitive, motor and non-motor function. Safinamide inhibits monoamine oxidase B in a highly selective and reversible manner and beyond that has anti-glutamatergic properties, with positive effects on motor and non-motor symptoms. The aim of the study was to obtain data about the effectiveness and tolerability of safinamide under routine clinical practice conditions in unselected patients with Parkinson's disease (PD).
A post-hoc analysis of the German cohort of the European SYNAPSES study (a non-interventional cohort study). Patients were treated with safinamide as an add-on to levodopa and followed-up for 12 months. Analyses were done in the total cohort and in clinically relevant subgroups (patients older than 75 years; with relevant comorbidities; with psychiatric conditions).
181 PD patients were eligible for analysis. Motor symptoms included bradykinesia (76.8%), rigidity (77.3%), tremor (58.6%), and postural instability (27.1%). Non-motor symptoms were reported in 161 patients (89.0%), mainly psychiatric symptoms (43.1%), sleep disorders (35.9%), fatigue (30.9%), and pain (27.6%). 28.7% of patients were aged 75 years or older, 84.5% had relevant comorbidities, and 38.1% had psychiatric conditions. During treatment, the rate of motor complications decreased from 100.0% to 71.1%. UPDRS scores improved under safinamide, with a clinically important effect in 50% in the total score and 45% in the motor score. The positive effect on motor complications occurred already at the 4-month visit and was maintained over 12 months. At least one adverse event (AE)/adverse drug reaction (ADR) was reported by 62.4%/25.4% of patients, AEs were generally mild or moderate, and completely resolved. Only 5 (1.5%) AEs had a definite relationship to safinamide.
The benefit-risk profile of safinamide was favourable and consistent with the total cohort of the SYNAPSES study. In the subgroups, findings were congruent with the total population, which allows the clinical utilisation of safinamide also in more vulnerable patient groups.
帕金森病(PD)是一种常见的进行性神经退行性疾病,会导致多种神经递质失衡,影响认知、运动和非运动功能。沙芬酰胺以高度选择性和可逆的方式抑制单胺氧化酶B,此外还具有抗谷氨酸能特性,对运动和非运动症状有积极影响。本研究的目的是获取在常规临床实践条件下,未选择的帕金森病(PD)患者使用沙芬酰胺的有效性和耐受性数据。
对欧洲SYNAPSES研究的德国队列进行事后分析(一项非干预性队列研究)。患者接受沙芬酰胺作为左旋多巴的附加治疗,并随访12个月。在整个队列以及临床相关亚组(年龄大于75岁的患者;有相关合并症的患者;有精神疾病的患者)中进行分析。
181例PD患者符合分析条件。运动症状包括运动迟缓(76.8%)、僵硬(77.3%)、震颤(58.6%)和姿势不稳(27.1%)。161例患者(89.0%)报告有非运动症状,主要是精神症状(43.1%)、睡眠障碍(35.9%)、疲劳(30.9%)和疼痛(27.6%)。28.7%的患者年龄在75岁及以上,84.5%有相关合并症,38.1%有精神疾病。治疗期间,运动并发症发生率从100.0%降至71.1%。沙芬酰胺治疗下UPDRS评分有所改善,总分改善具有临床重要意义的患者占50%,运动评分改善具有临床重要意义的患者占45%。对运动并发症的积极影响在4个月随访时就已出现,并持续12个月。62.4%/25.4%的患者报告了至少一种不良事件(AE)/药物不良反应(ADR),AE一般为轻度或中度,且完全缓解。只有5例(1.5%)AE与沙芬酰胺有明确关联。
沙芬酰胺的获益风险比良好,与SYNAPSES研究的整个队列一致。在亚组中,研究结果与总体人群一致,这使得沙芬酰胺也可在更脆弱的患者群体中临床应用。
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