Institute of Human Genetics, Friedrich-Alexander-Universität Erlangen-Nürnberg (FAU), Erlangen, Germany.
Am J Med Genet A. 2019 Jan;179(1):50-56. doi: 10.1002/ajmg.a.60679. Epub 2018 Dec 11.
Biallelic variants in the AEBP1 gene cause a novel autosomal-recessive connective tissue disorder (CTD) reminiscent of Ehlers-Danlos Syndrome (EDS). The four previously reported individuals show considerable clinical variability. Unbiased high-throughput sequencing enables the rapid identification of additional cases for such rare entities. We identified the homozygous nonsense variant c.917dup, p.Tyr306* in AEBP1 using clinical exome sequencing in a female individual with previously unsolved CTD. Segregation testing confirmed homozygosity in the clinically affected brother and heterozygous carrier status in the healthy mother. Chromosomal microarray showed that the variant lies in a run of homozygosity, suggesting a common origin of this genomic segment. RT-PCR analysis in the mother revealed a monoallelic expression of the normal transcript supporting a nonsense-mediated mRNA decay and functional nullizygosity as disease mechanism. We describe two individuals from a fourth family with AEBP1-associated CTD. Our results further verify that autosomal-recessive inherited LOF variants in the AEBP1 gene cause clinical features of different EDS subtypes, but also of the marfanoid spectrum. As identification of further individuals is necessary to inform the clinical characterization, we stress the added value of exome sequencing for such rare diseases.
AEBP1 基因中的双等位基因变异导致一种新型常染色体隐性结缔组织疾病(CTD),类似于埃勒斯-当洛斯综合征(EDS)。之前报道的 4 名患者表现出相当大的临床变异性。无偏倚的高通量测序能够快速识别此类罕见疾病的其他病例。我们使用临床外显子组测序在一名患有先前未解决的 CTD 的女性个体中发现了 AEBP1 基因的纯合无义变异 c.917dup,p.Tyr306*。 连锁分析证实了临床受累兄弟的纯合性和健康母亲的杂合子携带状态。染色体微阵列显示该变异位于一段纯合性区域内,提示该基因组片段具有共同的起源。母亲的 RT-PCR 分析显示正常转录本的单等位基因表达,支持无义介导的 mRNA 降解和功能纯合性作为疾病机制。我们描述了来自第四个家族的两名 AEBP1 相关 CTD 患者。我们的结果进一步证实,AEBP1 基因中的常染色体隐性遗传 LOF 变异导致不同 EDS 亚型的临床特征,但也导致马凡综合征样谱。由于需要进一步识别个体以告知临床特征,我们强调外显子组测序对于此类罕见疾病的附加价值。
