A Model Organism Pipeline Provides Insight into the Clinical Heterogeneity of TARS1 Loss-of-function Variants

Overview

Journal HGG Adv

Specialty Genetics

Date 2024 Jul 3

PMID 38956874

Authors

Rebecca Meyer-Schuman

Allison R Cale

Jennifer A Pierluissi

Kira E Jonatzke

Young N Park

Guy M Lenk

Stephanie N Oprescu

Marina A Grachtchouk

Andrzej A Dlugosz

Asim A Beg

Miriam H Meisler

Anthony Antonellis

Affiliations

Soon will be listed here.

Abstract

Aminoacyl-tRNA synthetases (ARSs) are ubiquitously expressed, essential enzymes that complete the first step of protein translation: ligation of amino acids to cognate tRNAs. Genes encoding ARSs have been implicated in myriad dominant and recessive phenotypes, the latter often affecting multiple tissues but with frequent involvement of the central and peripheral nervous systems, liver, and lungs. Threonyl-tRNA synthetase (TARS1) encodes the enzyme that ligates threonine to tRNA in the cytoplasm. To date, TARS1 variants have been implicated in a recessive brittle hair phenotype. To better understand TARS1-related recessive phenotypes, we engineered three TARS1 missense variants at conserved residues and studied these variants in Saccharomyces cerevisiae and Caenorhabditis elegans models. This revealed two loss-of-function variants, including one hypomorphic allele (R433H). We next used R433H to study the effects of partial loss of TARS1 function in a compound heterozygous mouse model (R432H/null). This model presents with phenotypes reminiscent of patients with TARS1 variants and with distinct lung and skin defects. This study expands the potential clinical heterogeneity of TARS1-related recessive disease, which should guide future clinical and genetic evaluations of patient populations.

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