摘要
Mutations of the genes encoding aminoacyl-tRNA synthetases are highly associated with various central nervous system disorders.Recurrent mutations,including c.5A>G,p.D2G;c.1367C>T,p.S456L;c.1535G>A,p.R512Q and c.1846_1847del,p.Y616Lfs*6 of RARS1 gene,which encodes two forms of human cytoplasmic arginyl-tRNA synthetase(hArgRS),are linked to Pelizaeus-Merzbacher-like disease(PMLD)with unclear pathogenesis.Among these mutations,c.5A>G is the most extensively reported mutation,leading to a p.D2G mutation in the N-terminal extension of the long-form hArgRS.Here,we showed the detrimental effects of R512Q substitution andΔC mutations on the structure and function of hArgRS,while the most frequent mutation c.5A>G,p.D2G acted in a different manner without impairing hArgRS activity.The nucleotide substitution c.5A>G reduced translation of hArgRS mRNA,and an upstream open reading frame contributed to the suppressed translation of the downstream main ORF.Taken together,our results elucidated distinct pathogenic mechanisms of various RARS1 mutations in PMLD.
基金
supported by the National Key Research and Development Program of China(2017YFA0504000)
the Natural Science Foundation of China(91940302,31500644,31570792,31822015,81870896,31670801,31870811)
the Strategic Priority Research Program of the Chinese Academy of Sciences(XDB19010203)
Key Laboratory of Reproductive Genetics(Zhejiang University),Ministry of Education,P.R.China(ZDFY2020-RG-0003)
Shanghai Key Laboratory of Embryo Original Diseases(Shelab201904).
