Genes, Vol. 14, Pages 254: Towards a Cure for HARS Disease

Genes, Vol. 14, Pages 254: Towards a Cure for HARS Disease

Genes doi: 10.3390/genes14020254

Authors: Sarah D. P. Wilhelm Rosan Kenana Yi Qiu Patrick O’Donoghue Ilka U. Heinemann

Histidyl-tRNA synthetase (HARS) ligates histidine to its cognate transfer RNA (tRNAHis). Mutations in HARS cause the human genetic disorders Usher syndrome type 3B (USH3B) and Charcot-Marie-Tooth syndrome type 2W (CMT2W). Treatment for these diseases remains symptomatic, and no disease specific treatments are currently available. Mutations in HARS can lead to destabilization of the enzyme, reduced aminoacylation, and decreased histidine incorporation into the proteome. Other mutations lead to a toxic gain-of-function and mistranslation of non-cognate amino acids in response to histidine codons, which can be rescued by histidine supplementation in vitro. We discuss recent advances in characterizing HARS mutations and potential applications of amino acid and tRNA therapy for future gene and allele specific therapy.