National Institute of Nursing Research, NIH, Bethesda, MD, USA.
Rehabilitation Medicine, NIH, Bethesda, MD, USA.
Orphanet J Rare Dis. 2018 Jul 3;13(1):105. doi: 10.1186/s13023-018-0848-9.
RYR1-related Myopathies (RYR1-RM) comprise a group of rare neuromuscular diseases (NMDs) occurring in approximately 1/90000 people in the US pediatric population. RYR1-RM result from pathogenic mutations in the ryanodine receptor isoform-1 (RYR1) gene where consequent RyR1 protein calcium dysregulation leads to impaired excitation-contraction coupling, oxidative and nitrosative stress, and mitochondrial depletion. These physiological deficits perpetuate RyR1 dysfunction causing further muscle injury, muscle weakness, and muscle fatigue. Muscle weakness and fatigue are two primary complaints in patients with RYR1-RM and are major symptoms that limit the ability of individuals to perform activities of daily living. The six-minute walk test (6MWT) is an endurance test with high reliability and validity used to measure walking capacity, disease progression, and more recently, fatigability in NMDs with limited results in RYR1-RM. Therefore, the purpose of our study is to objectively assess disease progression and fatigability in RYR1-RM affected individuals using the 6MWT. We hypothesized that 6MWT distance and fatigability would not change significantly between 0 and 6-month visits in RYR1-RM patients, given the clinically reported stable or slowly progressive nature of the disease. We also hypothesized participants would show fatigability during the 6MWT, given muscle weakness and fatigue are the two primary complaints of affected individuals.
As expected, paired t-test analyses revealed no significant difference between total distance traveled (p = .608) or percent change in speed (p = .141) at 0-months compared with the 6-month visit. Fatigability was observed given the decline in speed between the first and last minute of the 6MWT at the 6-month time point (p ≤ .0005,). Although this decline was not significant at baseline, a significant decline in speed from the 1st minute did occur at minutes 2, 3, and 4 during the baseline visit.
In this RYR1-RM cohort, the 6MWT showed disease stability over a 6-month period but revealed fatigability during the test. Given these results, the 6MWT may be a promising endpoint for evaluating fatigability and therapeutic efficacy in the 6-month treatment phase of our current n-acetylcysteine trial in this population. Improvement post intervention could be attributed to the intervention rather than variability in disease progression.
Clinical Trials.gov, NCT02362425 , Registered 13 February 2015-Prospectively registered.
RYR1 相关肌病(RYR1-RM)是一组罕见的神经肌肉疾病(NMD),在美国儿科人群中,每 90000 人中约有 1 人患病。RYR1-RM 是由于兰尼碱受体 1 型(RYR1)基因的致病性突变引起的,由此导致的 RyR1 蛋白钙调节异常导致兴奋-收缩偶联受损、氧化和硝化应激以及线粒体耗竭。这些生理缺陷使 RyR1 功能障碍持续存在,导致进一步的肌肉损伤、肌肉无力和肌肉疲劳。肌肉无力和疲劳是 RYR1-RM 患者的两个主要主诉,也是限制个体进行日常生活活动能力的主要症状。6 分钟步行试验(6MWT)是一种耐力测试,具有高度的可靠性和有效性,用于测量步行能力、疾病进展,最近还用于 RYR1-RM 中疲劳性的测量,但在 RYR1-RM 中的结果有限。因此,我们的研究目的是使用 6MWT 客观评估 RYR1-RM 受影响个体的疾病进展和疲劳性。我们假设,鉴于该疾病的临床报告为稳定或缓慢进展,在 RYR1-RM 患者的 0 至 6 个月就诊期间,6MWT 的距离和疲劳性不会发生显著变化。我们还假设参与者在 6MWT 期间会表现出疲劳性,因为肌肉无力和疲劳是受影响个体的两个主要主诉。
正如预期的那样,配对 t 检验分析显示,与 6 个月就诊时相比,总行进距离(p=0.608)或速度百分比变化(p=0.141)在 0 个月时无显著差异。在 6 个月时观察到疲劳性,因为在 6MWT 的最后一分钟与第一分钟之间速度下降(p≤0.0005)。尽管在基线时这一下降不显著,但在基线就诊期间,速度确实从第 1 分钟开始显著下降,在第 2、3 和 4 分钟时也下降了。
在这个 RYR1-RM 队列中,6MWT 在 6 个月的时间内显示出疾病稳定,但在测试过程中显示出疲劳性。鉴于这些结果,6MWT 可能是评估该人群中当前 N-乙酰半胱氨酸试验 6 个月治疗阶段疲劳性和治疗效果的有前途的终点。干预后的改善可能归因于干预,而不是疾病进展的变异性。
ClinicalTrials.gov,NCT02362425,2015 年 2 月 13 日注册-前瞻性注册。
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