Servicio de Genética, Hospital Universitario Ramón y Cajal, IRYCIS, 28034 Madrid, Spain.
Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), 28034 Madrid, Spain.
Genes (Basel). 2024 Jul 19;15(7):951. doi: 10.3390/genes15070951.
Dysfunction of some mitochondrial aminoacyl-tRNA synthetases (encoded by the , , and genes) results in a great variety of phenotypes ranging from non-syndromic hearing impairment (NSHI) to very complex syndromes, with a predominance of neurological signs. The diversity of roles that are played by these moonlighting enzymes and the fact that most pathogenic variants are missense and affect different domains of these proteins in diverse compound heterozygous combinations make it difficult to establish genotype-phenotype correlations. We used a targeted gene-sequencing panel to investigate the presence of pathogenic variants in those four genes in cohorts of 175 Spanish and 18 Colombian familial cases with non-DFNB1 autosomal recessive NSHI. Disease-associated variants were found in five cases. Five mutations were novel as follows: c.766C>T in , c.475C>T, c.728A>C and c.1012G>A in , and c.795A>G in . We provide audiograms from patients at different ages to document the evolution of the hearing loss, which is mostly prelingual and progresses from moderate/severe to profound, the middle frequencies being more severely affected. No additional clinical sign was observed in any affected subject. Our results confirm the involvement of in DFNB89 NSHI, for which until now there was limited evidence.
一些线粒体氨酰-tRNA 合成酶(由 、 、 和 基因编码)的功能障碍导致了各种表型,从非综合征性听力损失(NSHI)到非常复杂的综合征,以神经体征为主。这些兼职酶的作用多样性,以及大多数致病性变异是错义的,并影响这些蛋白质的不同结构域,形成不同的复合杂合组合,这使得建立基因型-表型相关性变得困难。我们使用靶向基因测序panel 对 175 名西班牙和 18 名哥伦比亚家族性非 DFNB1 常染色体隐性 NSHI 患者的四个基因中的致病性变异进行了研究。在五个病例中发现了与疾病相关的变异。五个突变是新的,分别为: 中的 c.766C>T, 中的 c.475C>T、c.728A>C 和 c.1012G>A,以及 中的 c.795A>G。我们提供了不同年龄患者的听力图,以记录听力损失的演变,听力损失主要是先天性的,从中度/重度进展到重度,中频受影响更严重。在任何受影响的患者中都没有观察到其他额外的临床症状。我们的结果证实了 参与了 DFNB89 NSHI,而到目前为止,这方面的证据有限。
