4.3 Article

tRNA methyltransferase homologue gene TRMT10A mutation in young adult-onset diabetes with intellectual disability, microcephaly and epilepsy

Journal

DIABETIC MEDICINE
Volume 33, Issue 9, Pages E21-E25

Publisher

WILEY-BLACKWELL
DOI: 10.1111/dme.13024

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Funding

  1. Health Innovation Challenge Fund (HICF)
  2. Wellcome Trust
  3. Department of Health [091985/HICF 1009-041]
  4. Academic Medicine Development Award from National University Health System, Singapore
  5. Wellcome Trust New Investigator award

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BackgroundA syndrome of young-onset diabetes mellitus associated with microcephaly, epilepsy and intellectual disability caused by mutations in the tRNA methyltransferase 10 homologue A (TRMT10A) gene has recently been described. Case reportWe report two siblings from the fourth family reported to have diabetes mellitus as a result of a TRMT10A mutation. A homozygous nonsense mutation p.Glu27Ter in TRMT10A was identified using targeted next-generation sequencing and confirmed by PCR/Sanger sequencing. Diabetes was diagnosed while the subjects were in their 20s and was characterized by insulin resistance. Epilepsy and intellectual disability were features in common. Mild microcephaly was present at birth but their final head circumferences were normal. ConclusionOur report provides independent confirmation of the role of TRMT10A mutations in this syndrome and expands its phenotypic description. TRMT10A sequencing should be considered in children or adults with young-onset diabetes who have a history of intellectual disability, microcephaly and epilepsy. This report also shows the advantages of using a targeted panel to identify previously unsuspected monogenic diabetes among young-onset non-insulin-dependent diabetes in the absence of obesity and autoimmunity.

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