Laboratorio de Biología Molecular, Instituto Nacional de Pediatría, Secretaría de Salud, Ciudad de México, México.
IDIX SA de CV., Querétaro, México.
Sci Rep. 2020 Apr 20;10(1):6589. doi: 10.1038/s41598-020-62759-5.
The aim of this study was to improve knowledge of the mutational spectrum causing tuberous sclerosis complex (TSC) in a sample of Mexican patients, given the limited information available regarding this disease in Mexico and Latin America. Four different molecular techniques were implemented to identify from single nucleotide variants to large rearrangements in the TSC1 and TSC2 genes of 66 unrelated Mexican-descent patients that clinically fulfilled the criteria for a definitive TSC diagnosis. The mutation detection rate was 94%, TSC2 pathogenic variants (PV) prevailed over TSC1 PV (77% vs. 23%) and a recurrent mutation site (hotspot) was observed in TSC1 exon 15. Interestingly, 40% of the identified mutations had not been previously reported. The wide range of novels PV made it difficult to establish any genotype-phenotype correlation, but most of the PV conditioned neurological involvement (intellectual disability and epilepsy). Our 3D protein modeling of two variants classified as likely pathogenic demonstrated that they could alter the structure and function of the hamartin (TSC1) or tuberin (TSC2) proteins. Molecular analyses of parents and first-degree affected family members of the index cases enabled us to distinguish familial (18%) from sporadic (82%) cases and to identify one case of apparent gonadal mosaicism.
本研究旨在提高对结节性硬化症(TSC)突变谱的认识,为此我们对 66 名无亲缘关系的墨西哥裔患者进行了研究,这些患者的临床表现均符合 TSC 的明确诊断标准。我们采用了四种不同的分子技术,对 TSC1 和 TSC2 基因进行了分析,检测范围包括单核苷酸变异到大片段重排。结果显示,突变检测率为 94%,致病性变异(PV)在 TSC2 中更为常见(77%比 23%),在 TSC1 外显子 15 中还观察到一个反复出现的突变热点。有趣的是,40%的鉴定突变此前尚未报道过。由于所鉴定的 PV 大多为新的变异,因此难以建立任何基因型-表型相关性,但大多数 PV 会导致神经系统受累(智力残疾和癫痫)。我们对两种归类为可能致病性的变异进行了 3D 蛋白建模,结果表明它们可能改变错构瘤蛋白(TSC1)或 tuberin 蛋白(TSC2)的结构和功能。对先证者的父母和一级亲属进行的分子分析,有助于我们区分家族性(18%)和散发性(82%)病例,并鉴定出一例明显的性腺镶嵌现象。
