Department of Internal Medicine, The University of Texas Health Science Center at Houston McGovern Medical School, Houston, USA.
Department of Emergency Medicine, Zhongshan Hospital, Fudan University, Shanghai, China.
Eur J Hum Genet. 2019 Jul;27(7):1054-1060. doi: 10.1038/s41431-019-0357-x. Epub 2019 Feb 26.
SMAD4 pathogenic variants cause juvenile polyposis (JPS) and hereditary hemorrhagic telangiectasia (HHT), and 40% of affected individuals also have thoracic aortic disease. At the same time, SMAD4 pathogenic variants have not been reported in thoracic aortic disease families without JPS-HHT. A SMAD4 heterozygous variant, c.290G>T, p.(Arg97Leu), not present in population databases and predicted to be damaging to protein function, was identified in a family with thoracic aortic disease and no evidence of HHT or JPS. Cellular studies revealed that the SMAD4 p.(Arg97Leu) alteration increased SMAD4 ubiquitination and 26S proteasome-mediated protein degradation. Smooth muscle cells (SMCs) infected with lentivirus expressing the SMAD4 p.(Arg97Leu) variant demonstrated reduced contractile protein gene expression when compared to that of wild-type SMAD4. In addition, two rare variants were identified in individuals with early age of onset of thoracic aortic dissection. These results suggest that SMAD4 rare missense variants can lead to thoracic aortic disease in individuals who do not have JPS or HHT.
SMAD4 致病变体可导致少年型息肉病 (JPS) 和遗传性出血性毛细血管扩张症 (HHT),40%的受影响个体也有胸主动脉疾病。同时,在没有 JPS-HHT 的胸主动脉疾病家族中,尚未报道 SMAD4 致病变体。在一个有胸主动脉疾病且没有 HHT 或 JPS 证据的家族中,发现了一种 SMAD4 杂合变体 c.290G>T,p.(Arg97Leu),该变体不存在于人群数据库中,预测对蛋白质功能有损害。细胞研究表明,SMAD4 p.(Arg97Leu)改变增加了 SMAD4 的泛素化和 26S 蛋白酶体介导的蛋白质降解。与野生型 SMAD4 相比,感染表达 SMAD4 p.(Arg97Leu)变体的慢病毒的平滑肌细胞 (SMCs) 表现出收缩蛋白基因表达降低。此外,在胸主动脉夹层发病年龄较早的个体中还鉴定出两种罕见变异体。这些结果表明,SMAD4 罕见错义变体可导致没有 JPS 或 HHT 的个体发生胸主动脉疾病。
