Exome Sequencing Identified a Splice Site Mutation in FHL1 that Causes Uruguay Syndrome, an X-Linked Disorder With Skeletal Muscle Hypertrophy and Premature Cardiac Death

Yuan Xue, B. Schoser, Aliz R. Rao, R. Quadrelli, A. Vaglio, Verena Rupp, Christine Beichler, S. Nelson, Gudrun Schapacher-Tilp, C. Windpassinger, W. Wilcox
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引用次数: 9

Abstract

Background—Previously, we reported a rare X-linked disorder, Uruguay syndrome in a single family. The main features are pugilistic facies, skeletal deformities, and muscular hypertrophy despite a lack of exercise and cardiac ventricular hypertrophy leading to premature death. Methods and Results—An ≈19 Mb critical region on X chromosome was identified through identity-by-descent analysis of 3 affected males. Exome sequencing was conducted on one affected male to identify the disease-causing gene and variant. A splice site variant (c.502-2A>G) in the FHL1 gene was highly suspicious among other candidate genes and variants. FHL1A is the predominant isoform of FHL1 in cardiac and skeletal muscle. Sequencing cDNA showed the splice site variant led to skipping of exons 6 of the FHL1A isoform, equivalent to the FHL1C isoform. Targeted analysis showed that this splice site variant cosegregated with disease in the family. Western blot and immunohistochemical analysis of muscle from the proband showed a significant decrease in protein expression of FHL1A. Real-time polymerase chain reaction analysis of different isoforms of FHL1 demonstrated that the FHL1C is markedly increased. Conclusions—Mutations in the FHL1 gene have been reported in disorders with skeletal and cardiac myopathy but none has the skeletal or facial phenotype seen in patients with Uruguay syndrome. Our data suggest that a novel FHL1 splice site variant results in the absence of FHL1A and the abundance of FHL1C, which may contribute to the complex and severe phenotype. Mutation screening of the FHL1 gene should be considered for patients with uncharacterized myopathies and cardiomyopathies.
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外显子组测序发现FHL1剪接位点突变导致乌拉圭综合征,一种骨骼肌肥大和心脏性过早死亡的x连锁疾病
背景:以前,我们报道了一个罕见的x连锁疾病,乌拉圭综合征在一个家庭。其主要特征是拳击相、骨骼畸形和肌肉肥大,尽管缺乏运动和心室肥大导致过早死亡。方法与结果:通过遗传鉴定分析,在3个患病雄性的X染色体上鉴定出一个≈19 Mb的关键区域。对一名患病男性进行了外显子组测序,以确定致病基因和变异。FHL1基因的剪接位点变异(c.502-2A>G)在其他候选基因和变异中高度可疑。FHL1A是FHL1在心脏和骨骼肌中的主要亚型。cDNA测序显示,剪接位点变异导致FHL1A异构体外显子6的跳跃,相当于FHL1C异构体。有针对性的分析表明,该剪接位点变异在家族中与疾病共分离。先证者肌肉的Western blot和免疫组化分析显示FHL1A蛋白表达显著降低。不同亚型FHL1的实时聚合酶链反应分析显示,fh1c明显升高。结论:FHL1基因突变在骨骼和心肌病疾病中有报道,但没有一例出现乌拉圭综合征患者的骨骼或面部表型。我们的数据表明,一种新的FHL1剪接位点变异导致了FHL1A的缺失和FHL1C的丰富,这可能导致了复杂和严重的表型。对于非特征性肌病和心肌病患者,应考虑FHL1基因突变筛查。
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来源期刊
Circulation-Cardiovascular Genetics
Circulation-Cardiovascular Genetics CARDIAC & CARDIOVASCULAR SYSTEMS-GENETICS & HEREDITY
CiteScore
3.95
自引率
0.00%
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0
期刊介绍: Circulation: Genomic and Precision Medicine considers all types of original research articles, including studies conducted in human subjects, laboratory animals, in vitro, and in silico. Articles may include investigations of: clinical genetics as applied to the diagnosis and management of monogenic or oligogenic cardiovascular disorders; the molecular basis of complex cardiovascular disorders, including genome-wide association studies, exome and genome sequencing-based association studies, coding variant association studies, genetic linkage studies, epigenomics, transcriptomics, proteomics, metabolomics, and metagenomics; integration of electronic health record data or patient-generated data with any of the aforementioned approaches, including phenome-wide association studies, or with environmental or lifestyle factors; pharmacogenomics; regulation of gene expression; gene therapy and therapeutic genomic editing; systems biology approaches to the diagnosis and management of cardiovascular disorders; novel methods to perform any of the aforementioned studies; and novel applications of precision medicine. Above all, we seek studies with relevance to human cardiovascular biology and disease. Manuscripts are examined by the editorial staff and usually evaluated by expert reviewers assigned by the editors. Both clinical and basic articles will also be subject to statistical review, when appropriate. Provisional or final acceptance is based on originality, scientific content, and topical balance of the journal. Decisions are communicated by email, generally within six weeks. The editors will not discuss a decision about a manuscript over the phone. All rebuttals must be submitted in writing to the editorial office.
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