FMR1 前突变女性在一个未选择的社区为基础的队列中的轻度神经体征。
Mild Neurological Signs in FMR1 Premutation Women in an Unselected Community-Based Cohort.
机构信息
Waisman Center, University of Wisconsin-Madison, Madison, Wisconsin, USA.
Department of Neurological Sciences, Rush University, Chicago, Illinois, USA.
出版信息
Mov Disord. 2021 Oct;36(10):2378-2386. doi: 10.1002/mds.28683. Epub 2021 Jun 12.
BACKGROUND
Premutation-sized (55-200) CGG repeat expansions in the FMR1 gene cause fragile X-associated tremor/ataxia syndrome (FXTAS). Most studies of premutation carriers utilized reverse ascertainment to identify patients, leading to a selection bias for larger repeats. As shorter CGG premutation repeats are common in the population, understanding their impact on health outcomes has a potentially large public health footprint.
OBJECTIVE
The study's objective was to compare an unselected group of premutation carriers (n = 35, 55-101 CGG repeats) with matched controls (n = 61, 29-39 CGG repeats) with respect to FXTAS-type signs using structured neurological assessments.
METHODS
Three neurologists independently rated signs, using an adapted version of the FXTAS Rating Scale (Leehey MA, Berry-Kravis E, Goetz CG, et al. FMR1 CGG repeat length predicts motor dysfunction in premutation carriers. Neurology. 2008). This was a double-blind study, as genetic status (premutation vs. control) was known neither by the participants nor by any of the neurologists. Analyses controlled potentially confounding comorbid conditions in the electronic health record (eg, osteoarthritis and stroke) and probed the association of age with signs.
RESULTS
Although there was no overall difference between carriers and controls, among individuals without any potentially confounding comorbid diagnoses, there was a statistically significant age-associated elevation in FXTAS-type signs in premutation carriers compared to controls.
CONCLUSIONS
Among those who do not have other comorbid diagnoses, women who have CGG repeats at the lower end of the premutation range may be at greater risk for ataxia and parkinsonism than their age peers, although their overall risk of developing such clinical features is low. This study should provide reassurance to those who share characteristics with the present cohort. © 2021 International Parkinson and Movement Disorder Society.
背景
脆性 X 相关震颤/共济失调综合征(FXTAS)是由 FMR1 基因中 55-200 个 CGG 重复扩增引起的。大多数对前突变携带者的研究利用反向确定法来识别患者,从而导致对较大重复的选择偏差。由于较短的 CGG 前突变重复在人群中很常见,了解它们对健康结果的影响可能具有很大的公共卫生意义。
目的
本研究的目的是使用结构化神经评估,比较未经选择的前突变携带者组(n=35,55-101 CGG 重复)与匹配的对照组(n=61,29-39 CGG 重复)的 FXTAS 型体征。
方法
三位神经病学家使用改良的 FXTAS 评分量表(Leehey MA、Berry-Kravis E、Goetz CG 等人。FMR1 CGG 重复长度预测前突变携带者的运动功能障碍。神经病学。2008)独立评估体征。这是一项双盲研究,因为参与者和任何一位神经病学家都不知道遗传状态(前突变与对照)。分析控制了电子健康记录中潜在的混杂共病(如骨关节炎和中风),并探讨了年龄与体征的关联。
结果
尽管携带者和对照组之间没有总体差异,但在没有任何潜在混杂共病诊断的个体中,与对照组相比,前突变携带者中与 FXTAS 型体征相关的年龄呈统计学显著升高。
结论
在没有其他共病诊断的人中,CGG 重复处于前突变范围较低端的女性可能比同龄人群更容易出现共济失调和帕金森病,但她们出现此类临床特征的总体风险较低。本研究应该为与本队列具有相似特征的人提供安慰。 © 2021 国际帕金森病和运动障碍学会。
Zotero 插件