Frontiers in Pediatrics (Apr 2024)

Case Report: Novel compound heterozygous TPRKB variants cause Galloway-Mowat syndrome

  • Takuya Hiraide,
  • Taiju Hayashi,
  • Taiju Hayashi,
  • Yusuke Ito,
  • Rei Urushibata,
  • Hiroshi Uchida,
  • Ryoichi Kitagata,
  • Hidetoshi Ishigaki,
  • Tsutomu Ogata,
  • Tsutomu Ogata,
  • Tsutomu Ogata,
  • Hirotomo Saitsu,
  • Tokiko Fukuda,
  • Tokiko Fukuda

DOI
https://doi.org/10.3389/fped.2024.1360867
Journal volume & issue
Vol. 12

Abstract

Read online

BackgroundGalloway-Mowat syndrome (GAMOS) is a rare genetic disease characterized by early-onset nephrotic syndrome and microcephaly with central nervous system abnormalities. Pathogenic variants in genes encoding kinase, endopeptidase, and other proteins of small size (KEOPS) complex subunits cause GAMOS. The subunit TPRKB (TP53RK binding protein) has been reported in only two patients with GAMOS with homozygous missense variants.Clinical reportHerein, we described a three-year-old male with GAMOS. He exhibited developmental delay, developmental regression, microcephaly, distinctive facial features, skeletal abnormalities, and epilepsy. Brain magnetic resonance imaging revealed progressive brain atrophy, delayed myelination, T2-hypointense signals in the thalamus, and multiple intracranial abnormal signals on diffusion-weighted imaging. He presented with relapsing nephrotic proteinuria exacerbated by upper respiratory tract infections and progressive renal function decline. Exome sequencing identified compound heterozygous missense and frameshift variants in TPRKB: c.224dup, p.(Ser76IlefsTer3) and c.247C>T, p.(Leu83Phe).ConclusionsOur study supports that pathogenic TPRKB variants cause KEOPS complex-related GAMOS.

Keywords