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Penetrance of marked cognitive impairment in older male carriers of the FMR1 gene premutation.脆性 X 智力低下 1 基因前突变男性携带者老年时明显认知障碍的外显率。
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No evidence for a difference in neuropsychological profile among carriers and noncarriers of the FMR1 premutation in adults under the age of 50.在50岁以下的成年人中,没有证据表明FMR1前突变携带者和非携带者在神经心理学特征上存在差异。
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The primary cognitive deficit among males with fragile X-associated tremor/ataxia syndrome (FXTAS) is a dysexecutive syndrome.脆性 X 相关震颤/共济失调综合征(FXTAS)男性患者的主要认知缺陷是执行功能障碍综合征。
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Age-dependent cognitive changes in carriers of the fragile X syndrome.脆性X综合征携带者的年龄依赖性认知变化。
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Detection of early FXTAS motor symptoms using the CATSYS computerised neuromotor test battery.使用CATSYS计算机化神经运动测试组合检测脆性X震颤共济失调综合征(FXTAS)早期运动症状
J Med Genet. 2008 May;45(5):290-7. doi: 10.1136/jmg.2007.054676. Epub 2008 Jan 30.
8
Cognitive profile of fragile X premutation carriers with and without fragile X-associated tremor/ataxia syndrome.伴有和不伴有脆性X相关震颤/共济失调综合征的脆性X前突变携带者的认知特征。
Neuropsychology. 2008 Jan;22(1):48-60. doi: 10.1037/0894-4105.22.1.48.
9
Cognitive, anxiety and mood disorders in the fragile X-associated tremor/ataxia syndrome.脆性X相关震颤/共济失调综合征中的认知、焦虑和情绪障碍。
Gen Hosp Psychiatry. 2007 Jul-Aug;29(4):349-56. doi: 10.1016/j.genhosppsych.2007.03.003.
10
Examination of reproductive aging milestones among women who carry the FMR1 premutation.对携带FMR1前突变的女性生殖衰老里程碑的研究。
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脆性 X 综合征家系中携带前突变的老年男性及其非携带者兄弟姊妹的神经心理学研究结果。

Neuropsychological findings from older premutation carrier males and their noncarrier siblings from families with fragile X syndrome.

机构信息

Department of Human Genetics, Emory University.

Department of Rehabilitation Medicine, Emory University.

出版信息

Neuropsychology. 2011 May;25(3):404-411. doi: 10.1037/a0021879.

DOI:10.1037/a0021879
PMID:21443343
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3086936/
Abstract

OBJECTIVE

Carriers of the FMR1 premutation allele are at a significantly increased risk for a late-onset neurodegenerative disorder, fragile X-associated tremor/ataxia syndrome (FXTAS). The primary features of FXTAS are late-onset intention tremor and gait ataxia. Previous reports have shown global deficits in neuropsychological measures among males with FXTAS, particularly those related to executive functioning. The purpose of this study was to investigate the neuropsychological profile among older males with the premutation who are at risk for FXTAS.

METHOD

Premutation carriers, 66 with motor symptoms and 23 without, and 18 noncarrier siblings were recruited from pedigrees diagnosed with fragile X syndrome, all over age 50. Subjects were examined with a neurological test battery to identify symptoms of FXTAS and a neuropsychological test battery to investigate cognitive and behavioral profiles. Linear regression and ANCOVA were used to determine the effect of the premutation on outcome measures adjusting for age and education.

RESULTS

We identified a significant decrease in scores of general intelligence and a marginally significant decrease in scores of logical memory among premutation carrier males with motor symptoms compared to the noncarrier male siblings. We did not identify deficits in executive functioning in our sample of premutation carrier males with motor symptoms.

CONCLUSIONS

Similar to other reports, we found that the FMR1 premutation is associated with deficits in general intelligence and memory among older males with symptoms of FXTAS. However, our results differed in that we found no evidence of premutation-associated executive dysfunction. We provide possible explanations for this difference.

摘要

目的

FMR1 前突变携带者发生迟发性神经退行性疾病——脆性 X 相关震颤共济失调综合征(FXTAS)的风险显著增加。FXTAS 的主要特征是迟发性意向性震颤和步态共济失调。先前的报告显示,FXTAS 男性存在神经心理学测量的整体缺陷,尤其是与执行功能相关的缺陷。本研究的目的是调查有前突变且有发生 FXTAS 风险的老年男性的神经心理学特征。

方法

我们从被诊断为脆性 X 综合征的家系中招募了前突变携带者(66 名有运动症状,23 名无症状,18 名非携带者兄弟姐妹),所有受试者年龄均超过 50 岁。采用神经学测试组合评估症状,采用神经心理学测试组合评估认知和行为特征,以确定 FXTAS 的神经心理学特征。线性回归和协方差分析用于确定前突变对调整年龄和教育后的结果测量的影响。

结果

我们发现,与非携带者男性兄弟姐妹相比,有运动症状的前突变携带者男性的一般智力评分显著降低,逻辑记忆评分略有降低。我们没有发现运动症状前突变携带者男性在执行功能方面存在缺陷。

结论

与其他报告类似,我们发现 FMR1 前突变与有 FXTAS 症状的老年男性在一般智力和记忆方面的缺陷有关。然而,我们的结果不同,我们没有发现前突变相关的执行功能障碍的证据。我们为这种差异提供了可能的解释。