Department of Pediatric Pneumonology and Allergy, Medical University of Warsaw, Warsaw, Poland.
Department of Medical Genetics, Medical University of Warsaw, Warsaw, Poland.
Clin Genet. 2019 Nov;96(5):468-472. doi: 10.1111/cge.13614. Epub 2019 Aug 6.
Pathogenic variants in genes encoding aminoacyl-tRNA synthetases cause numerous disorders characterized by involvement of neurons, muscles, lungs and liver. Recently, biallelic FARSB defects have been shown to cause severe growth restriction with combined brain, liver and lung involvement (Rajab interstitial lung disease [ILD] with brain calcifications). Herein, for the first time, we present a patient with similar condition associated with biallelic mutations in FARSA (NM_004461.3: c.766T>C:p.Phe256Leu and c.1230C>A:p.Asn410Lys). Both detected FARSA variants are ultrarare and predicted to be damaging by in silico programs. Furthermore, they are both located in the active site of phenylalanyl-tRNA synthetase (PheRS) with Asn410Lys directly affecting a residue forming the wall of the phenylalanine-binding pocket. Clinical features shared between our patient and the FARSB syndrome include ILD with cholesterol pneumonitis, growth delay, hypotonia, brain calcifications with cysts and liver dysfunction. Our findings indicate that a disease similar to a syndrome associated with FARSB defects can also be caused by biallelic FARSA mutations. These findings are consistent with molecular structure of PheRS which is a tetramer including both FARSA and FARSB proteins.
编码氨酰-tRNA 合成酶的基因中的致病性变异导致许多以神经元、肌肉、肺和肝受累为特征的疾病。最近,已证明双等位基因 FARSB 缺陷可导致严重的生长受限,伴有脑、肝和肺受累(Rajab 间质性肺病 [ILD] 伴脑钙化)。在此,我们首次报道了一例与 FARSA 双等位基因突变相关的具有相似表型的患者(NM_004461.3:c.766T>C:p.Phe256Leu 和 c.1230C>A:p.Asn410Lys)。两种检测到的 FARSA 变异均为超罕见,且预测程序提示其具有致病性。此外,它们均位于苯丙氨酰-tRNA 合成酶(PheRS)的活性部位,Asn410Lys 直接影响构成苯丙氨酸结合口袋壁的残基。我们的患者与 FARSB 综合征之间的临床特征包括伴有胆固醇性肺炎的 ILD、生长迟缓、张力减退、脑钙化伴囊肿和肝功能障碍。我们的研究结果表明,与 FARSB 缺陷相关的综合征类似的疾病也可能由 FARSA 双等位基因突变引起。这些发现与 PheRS 的分子结构一致,该酶为包括 FARSA 和 FARSB 蛋白在内的四聚体。
