Novel biallelic variants in MSTO1 associated with mitochondrial myopathy

Laura Schultz-Rogers; Alejandro Ferrer; Nikita R Dsouza; Michael T Zimmermann; Benn E Smith; Eric W Klee; Radhika Dhamija

doi:10.1101/mcs.a004309

Novel biallelic variants in MSTO1 associated with mitochondrial myopathy

Cold Spring Harb Mol Case Stud. 2019 Dec 13;5(6):a004309. doi: 10.1101/mcs.a004309. Print 2019 Dec.

Authors

Laura Schultz-Rogers¹, Alejandro Ferrer¹, Nikita R Dsouza², Michael T Zimmermann^{2

3}, Benn E Smith⁴, Eric W Klee^{1

5}, Radhika Dhamija⁶

Affiliations

¹ Center for Individualized Medicine, Mayo Clinic, Rochester, Minnesota 55905, USA.
² Bioinformatics Research and Development Laboratory, Genomics Sciences and Precision Medicine Center, Medical College of Wisconsin, Milwaukee, Wisconsin 53226, USA.
³ Clinical and Translational Sciences Institute, Medical College of Wisconsin, Milwaukee, Wisconsin 53226, USA.
⁴ Department of Neurology, Mayo Clinic, Scottsdale, Arizona 85259, USA.
⁵ Department of Clinical Genomics, Mayo Clinic, Rochester, Minnesota 55905, USA.
⁶ Department of Medical Genetics, Mayo Clinic, Phoenix, Arizona 85054, USA.

Abstract

Mitochondrial disorders are caused by nuclear and mitochondrial pathogenic variants leading to defects in mitochondrial function and cellular respiration. Recently, the nuclear-encoded mitochondrial fusion gene MSTO1 (Misato 1) has been implicated in mitochondrial myopathy and ataxia. Here we report on a 30-yr-old man presenting with a maternally inherited NM_018116.3:c.651C>G, p.F217L missense variant as well as a paternally inherited arr[GRCh37] 1q22(155581773_155706887) × 1 deletion encompassing exons 7-14 of MSTO1 His phenotype included muscle weakness, hypotonia, early motor developmental delay, pectus excavatum, and scoliosis. Testing revealed elevated plasma creatine kinase, and electromyogram results were consistent with longstanding generalized myopathy. These phenotypic features overlap well with previously reported patients harboring biallelic MSTO1 variants. Additionally, our patient presents with dysphagia and restrictive lung disease, not previously reported for MSTO1-associated disorders. The majority of patients with disease-associated variants in MSTO1 present with biallelic variants suggesting autosomal recessive inheritance; however, one family has been reported with a single variant and presumed autosomal dominant inheritance. The pattern of inheritance we observed is consistent with the majority of previous reports suggesting an autosomal recessive disorder. We add to our knowledge of the syndrome caused by variants in MSTO1 and provide additional evidence supporting autosomal recessive inheritance. We also describe phenotypic features not reported in previous cases, although further research is needed to confirm they are associated with defects in MSTO1.

Keywords: EMG: myopathic abnormalities; delayed gross motor development; dysphagia; episodic generalized hypotonia; lumbar kyphoscoliosis; mildly elevated creatine phosphokinase; pectus excavatum of inferior sternum; restrictive respiratory insufficiency; speech articulation difficulties; waddling gait.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Alleles
Ataxia / genetics
Cell Cycle Proteins / genetics*
Cell Cycle Proteins / metabolism
Cytoskeletal Proteins / genetics*
Cytoskeletal Proteins / metabolism
Family
Humans
Male
Mitochondria / genetics
Mitochondrial Diseases / genetics
Mitochondrial Diseases / metabolism
Mitochondrial Myopathies / genetics*
Mitochondrial Myopathies / metabolism
Muscular Diseases / genetics
Mutation
Pedigree
Phenotype

Substances

Cell Cycle Proteins
Cytoskeletal Proteins
MSTO1 protein, human