Loss-of-function variants in JPH1 cause congenital myopathy with prominent facial and ocular involvement.

IF 3.5 2区 医学 Q2 GENETICS & HEREDITY
Mridul Johari, Ana Topf, Chiara Folland, Jennifer Duff, Lein Dofash, Pilar Marti, Thomas Robertson, Juan Vilchez, Anita Cairns, Elizabeth Harris, Chiara Marini-Bettolo, Khalid Hundallah, Amal M Alhashem, Mohammed Al-Owain, Reza Maroofian, Gianina Ravenscroft, Volker Straub
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引用次数: 0

Abstract

Background: Weakness of facial, ocular and axial muscles is a common clinical presentation in congenital myopathies caused by pathogenic variants in genes encoding triad proteins. Abnormalities in triad structure and function resulting in disturbed excitation-contraction coupling and Ca2+ homeostasis can contribute to disease pathology.

Methods: We analysed exome and genome sequencing data from four unrelated individuals with congenital myopathy characterised by facial, ocular and bulbar involvement. We collected deep phenotypic data from the affected individuals. We analysed the RNA-sequencing (RNA-seq) data of F3-II.1 and performed gene expression outlier analysis in 129 samples.

Results: The four probands had a remarkably similar clinical presentation with prominent facial, ocular and bulbar features. Disease onset was in the neonatal period with hypotonia, poor feeding, cleft palate and talipes. Muscle weakness was generalised but prominent in the lower limbs with facial weakness also present. All patients had myopathic facies, bilateral ptosis, ophthalmoplegia and fatigability. Muscle biopsy on light microscopy showed type 1 myofiber predominance and ultrastructural analysis revealed slightly reduced triads, and structurally abnormal sarcoplasmic reticulum.DNA sequencing identified four unique homozygous loss-of-function variants in JPH1, encoding junctophilin-1 in the four families; one stop-gain (c.354C>A;p.Tyr118*) and three frameshift (c.373delG;p.Asp125Thrfs*30, c.1738delC;p.Leu580Trpfs*16 and c.1510delG;p. Glu504Serfs*3) variants. Muscle RNA-seq showed strong downregulation of JPH1 in the F3 proband.

Conclusions: Junctophilin-1 is critical for the formation of skeletal muscle triad junctions by connecting the sarcoplasmic reticulum and T-tubules. Our findings suggest that loss of JPH1 results in a congenital myopathy with prominent facial, bulbar and ocular involvement.

JPH1的功能缺失变体会导致先天性肌病,并伴有明显的面部和眼部受累。
背景:面肌、眼肌和轴肌无力是先天性肌病中常见的临床表现,这些先天性肌病是由编码三联蛋白的基因中的致病变异引起的。三联体结构和功能异常导致的兴奋-收缩耦合紊乱和 Ca2+ 平衡紊乱可导致疾病的病理变化:我们分析了四名无亲属关系的先天性肌病患者的外显子组和基因组测序数据,这些患者的面部、眼部和球部受累。我们收集了患者的深度表型数据。我们分析了F3-II.1的RNA测序(RNA-seq)数据,并对129个样本进行了基因表达离群分析:结果:四名患者的临床表现非常相似,面部、眼部和球部特征突出。新生儿期发病,伴有肌张力低下、喂养不良、腭裂和距趾。全身肌肉无力,但下肢突出,面部也有无力症状。所有患者都有肌病面容、双侧上睑下垂、眼肌麻痹和易疲劳。光镜下的肌肉活检显示,1型肌纤维占优势,超微结构分析显示,三联体略有减少,肌质网结构异常。C>A;p.Tyr118*)和三个框移位(c.373delG;p.Asp125Thrfs*30、c.1738delC;p.Leu580Trpfs*16 和 c.1510delG;p.Glu504Serfs*3)变异。肌肉 RNA-seq 分析显示,F3 患儿的 JPH1 有强烈的下调:结论:Junctophilin-1 连接肌浆网和 T 型微管,对骨骼肌三联体连接的形成至关重要。我们的研究结果表明,JPH1的缺失会导致一种先天性肌病,并伴有明显的面部、眼球和眼部受累。
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来源期刊
Journal of Medical Genetics
Journal of Medical Genetics 医学-遗传学
CiteScore
7.60
自引率
2.50%
发文量
92
审稿时长
4-8 weeks
期刊介绍: Journal of Medical Genetics is a leading international peer-reviewed journal covering original research in human genetics, including reviews of and opinion on the latest developments. Articles cover the molecular basis of human disease including germline cancer genetics, clinical manifestations of genetic disorders, applications of molecular genetics to medical practice and the systematic evaluation of such applications worldwide.
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