Montalván-Suárez Martha, Esperón-Moldes Uxia Saraiva, Rodríguez-Pazos Laura, Ordóñez-Ugalde Andrés, Moscoso Fernanda, Ugalde-Noritz Nora, Santomé Luis, Fachal Laura, Tettamanti-Miranda Daniel, Ruiz Juan Carlos, Ginarte Manuel, Vega Ana
Sistema de Investigación y Desarrollo SINDE, Universidad Católica de Santiago de Guayaquil and Universidad de Guayaquil, Guayaquil, Ecuador.
Fundación Pública Galega de Medicina Xenómica-SERGAS, Grupo de Medicina Xenómica-USC, CIBERER, IDIS, Santiago de Compostela, Spain.
Mol Genet Genomic Med. 2019 May;7(5):e608. doi: 10.1002/mgg3.608. Epub 2019 Mar 27.
Autosomal recessive congenital ichthyoses (ARCI) have been associated with different phenotypes including: harlequin ichthyosis (HI), congenital ichthyosiform erythroderma (CIE), and lamellar ichthyosis (LI). While pathogenic variants in all ARCI genes are associated with LI and CIE phenotypes, the unique gene associated with HI is ABCA12. In HI, the most severe ARCI form, pathogenic variants in both ABCA12 gene alleles usually have a severe impact on protein function. The presence of at least one non-truncating variant frequently causes a less severe congenital ichthyosis phenotype (LI and CIE).
We report the case of a 4-year-old Ecuadorian boy with a severe skin disease. Genetic diagnosis was performed by NGS. In silico predictions were performed using Alamut software v2.11. A review of the literature was carried out to identify all patients carrying ABCA12 splice-site and missense variants, and to explore their genotype-phenotype correlations.
Genetic testing revealed a nonsense substitution, p.(Arg2204*), and a new missense variant, p.(Val1927Leu), in the ABCA12 gene. After performing in silico analysis and a comprehensive review of the literature, we conclude that p.(Val1927Leu) affects a well conserved residue which could either disturb the protein function or alter the splicing process, both alternatives could explain the severe phenotype of our patient.
This case expands the spectrum of ABCA12 reported disease-causing variants which is important to unravel genotype-phenotype correlations and highlights the importance of missense variants in the development of HI.
常染色体隐性先天性鱼鳞病(ARCI)与不同的表型相关,包括丑角样鱼鳞病(HI)、先天性鱼鳞病样红皮病(CIE)和板层状鱼鳞病(LI)。虽然所有ARCI基因中的致病变异都与LI和CIE表型相关,但与HI相关的独特基因是ABCA12。在HI这种最严重的ARCI形式中,ABCA12基因两个等位基因中的致病变异通常会对蛋白质功能产生严重影响。至少存在一个非截短变异常常会导致较不严重的先天性鱼鳞病表型(LI和CIE)。
我们报告了一名患有严重皮肤病的4岁厄瓜多尔男孩的病例。通过二代测序进行基因诊断。使用Alamut软件v2.11进行计算机模拟预测。对文献进行综述以确定所有携带ABCA12剪接位点和错义变异的患者,并探讨其基因型与表型的相关性。
基因检测发现ABCA12基因中有一个无义替代突变p.(Arg2204*)和一个新的错义变异p.(Val1927Leu)。在进行计算机模拟分析和全面的文献综述后,我们得出结论,p.(Val1927Leu)影响一个高度保守的残基,这可能会干扰蛋白质功能或改变剪接过程,这两种情况都可以解释我们患者的严重表型。
该病例扩展了已报道的ABCA12致病变异谱,这对于阐明基因型与表型的相关性很重要,并突出了错义变异在HI发病中的重要性。
