洛伐他汀和米诺环素联合疗法对脆性X综合征患者神经生理学的影响:LOVAMIX随机临床试验的辅助结果。

IF 5.3 2区 医学 Q1 BEHAVIORAL SCIENCES
Autism Research Pub Date : 2024-09-09 DOI:10.1002/aur.3222
Florence Morin-Parent, Camille Champigny, Samantha Côté, Teddy Mohamad, Seyede Anis Hasani, Artuela Çaku, François Corbin, Jean-François Lepage
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引用次数: 0

摘要

脆性 X 综合征(FXS)是导致智力障碍和自闭症谱系障碍的主要遗传原因。它的特征是神经元兴奋性加剧,其校正被认为是动物模型治疗反应的客观衡量标准,但在临床试验中却很少使用。在此,我们使用了一种广泛的经颅磁刺激(TMS)疗法来评估两种疾病调节药物(洛伐他汀(40 毫克)和米诺环素(100 毫克))联合疗法的神经生理学效果,这两种药物分别单独使用 8 周和联合使用 12 周。TMS 测试包括静息运动阈值、短时段皮层内抑制、长时段皮层内抑制、皮质脊髓沉默期和皮层内促进,分别在单药治疗 8 周后(临床试验第 2 次)和双药治疗 12 周后(临床试验第 4 次)完成。在基线与第 2 次就诊(单一疗法)和第 3 次就诊(双重疗法)之间进行了重复测量方差分析,并对参与者开始临床试验时接受的单一疗法进行了交互作用。结果显示,双重疗法与 20 周后大脑皮层兴奋性降低有关。与基线相比,双重疗法后的静息运动阈值明显提高,这反映了这一点。与基线相比,单药治疗8周后皮质短抑制(GABAa介导的抑制标记)有增强的趋势。这些结果表明,米诺环素和洛伐他汀联合疗法可能会对 FXS 的核心神经生理病理学产生作用。该试验已在 clinicaltrials.gov (NCT02680379) 上注册。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Neurophysiological effects of a combined treatment of lovastatin and minocycline in patients with fragile X syndrome: Ancillary results of the LOVAMIX randomized clinical trial

Neurophysiological effects of a combined treatment of lovastatin and minocycline in patients with fragile X syndrome: Ancillary results of the LOVAMIX randomized clinical trial

Fragile X syndrome (FXS) is the primary hereditary cause of intellectual disability and autism spectrum disorder. It is characterized by exacerbated neuronal excitability, and its correction is considered an objective measure of treatment response in animal models, a marker albeit rarely used in clinical trials. Here, we used an extensive transcranial magnetic stimulation (TMS) battery to assess the neurophysiological effects of a therapy combining two disease-modifying drugs, lovastatin (40 mg) and minocycline (100 mg), administered alone for 8 weeks and in combination for 12 weeks, in 19 patients (mean age of 23.58 ± 1.51) with FXS taking part in the LOVAmix trial. The TMS battery, which included the resting motor threshold, short-interval intracortical inhibition, long-interval intracortical inhibition, corticospinal silent period, and intracortical facilitation, was completed at baseline after 8 weeks of monotherapy (visit 2 of the clinical trial) and after 12 weeks of dual therapy (visit 4 of the clinical trial). Repeated measure ANOVAs were performed between baseline and visit 2 (monotherapy) and visit 3 (dual therapy) with interactions for which monotherapy the participants received when they began the clinical trial. Results showed that dual therapy was associated with reduced cortical excitability after 20 weeks. This was reflected by a significant increase in the resting-motor threshold after dual therapy compared to baseline. There was a tendency for enhanced short-intracortical inhibition, a marker of GABAa-mediated inhibition after 8 weeks of monotherapy compared to baseline. Together, these results suggest that a combined therapy of minocycline and lovastatin might act on the core neurophysiopathology of FXS. This trial was registered at clinicaltrials.gov (NCT02680379).

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来源期刊
Autism Research
Autism Research 医学-行为科学
CiteScore
8.00
自引率
8.50%
发文量
187
审稿时长
>12 weeks
期刊介绍: AUTISM RESEARCH will cover the developmental disorders known as Pervasive Developmental Disorders (or autism spectrum disorders – ASDs). The Journal focuses on basic genetic, neurobiological and psychological mechanisms and how these influence developmental processes in ASDs.
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