From the Department of Neurology (M.W., C.G.H., B.G.v.E., G.W.P., N.C.V.), Donders Institute for Brain, Cognition and Behavior, and Radboud Institute for Health Sciences (M.J.), Radboud University Medical Center, Nijmegen; Department of Neurology (M.W.), ETZ, Tilburg; Department of Human Genetics (R.J.L., S.M.v.d.M.), Leiden University Medical Center; and Department of Neurology (E.v.d.K.), MCL, Leeuwarden, the Netherlands.
Neurology. 2018 Jul 31;91(5):e444-e454. doi: 10.1212/WNL.0000000000005915. Epub 2018 Jul 11.
An observational cross-sectional study was conducted in a national facioscapulohumeral muscular dystrophy (FSHD) expertise center to estimate the penetrance of FSHD1 and to evaluate phenotype-genotype correlations.
Ten FSHD1 probands carrying 4-9 D4Z4 unit alleles and 140 relatives were examined. All 150 participants were genetically characterized, including D4Z4 methylation levels in the mutation carriers. Mutation carriers were classified as (1) symptomatic: with symptoms of muscle weakness on history and muscle FSHD signs on examination; (2) asymptomatic: without symptoms of muscle weakness but with muscle FSHD signs on examination; and (3) nonpenetrant: without symptoms of muscle weakness on history and without muscle FSHD signs on examination. We assessed the relationship between age-corrected clinical severity score and repeat size, sex, and D4Z4 methylation levels.
The maximum likelihood estimates of symptomatic and those of symptomatic plus asymptomatic FSHD showed that penetrance depends on repeat size and increases until late adulthood. We observed many asymptomatic carriers with subtle facial weakness with or without mild shoulder girdle weakness (25% [17/69]). Nonpenetrance was observed less frequently than in recent population studies (17% [12/69]), and most asymptomatic patients reported some shoulder pain. D4Z4 methylation tended to be lower in moderately to severely affected mutation carriers with 7 or 9 repeats.
This family-based study detected a lower overall nonpenetrance than previously observed, probably due to many asymptomatic mutation carriers identified by careful examination of facial and shoulder muscles. The recognition of asymptomatic mutation carriers is essential for selection of participants for future trials, and the likelihood estimates are helpful in counseling.
本研究在全国面肩肱型肌营养不良症(FSHD)专业中心进行了一项观察性横断面研究,旨在估计 FSHD1 的外显率,并评估表型-基因型相关性。
研究纳入了 10 名携带 4-9 个 D4Z4 单位等位基因的 FSHD1 先证者及其 140 名亲属。对所有 150 名参与者进行了基因特征分析,包括突变携带者的 D4Z4 甲基化水平。突变携带者分为以下几类:(1)有症状者:有肌肉无力病史和肌肉 FSHD 体征;(2)无症状者:无肌肉无力病史,但有肌肉 FSHD 体征;(3)未外显者:无肌肉无力病史和肌肉 FSHD 体征。我们评估了年龄校正后的临床严重程度评分与重复大小、性别和 D4Z4 甲基化水平之间的关系。
最大似然估计的有症状和有症状加无症状 FSHD 表明,外显率取决于重复大小,并在成年后期增加。我们观察到许多无症状携带者存在轻微的面部无力,伴有或不伴有轻度肩部无力(25%[17/69])。未外显的情况比最近的人群研究中观察到的要少(17%[12/69]),而且大多数无症状患者报告有一些肩部疼痛。D4Z4 甲基化在重复数为 7 或 9 的中度至重度受累突变携带者中往往较低。
这项基于家庭的研究检测到的总体未外显率低于以往观察到的水平,这可能是由于通过对面部和肩部肌肉的仔细检查,发现了许多无症状的突变携带者。识别无症状的突变携带者对于未来试验的参与者选择至关重要,而可能性估计有助于咨询。
