Scientific Reports (Oct 2022)

Clinical and molecular findings in three Japanese patients with N-acetylneuraminic acid synthetase-congenital disorder of glycosylation (NANS-CDG)

  • Yohei Masunaga,
  • Gen Nishimura,
  • Koji Takahashi,
  • Tomiyuki Hishiyama,
  • Masatoshi Imamura,
  • Kenichi Kashimada,
  • Machiko Kadoya,
  • Yoshinao Wada,
  • Nobuhiko Okamoto,
  • Daiju Oba,
  • Hirofumi Ohashi,
  • Mitsuru Ikeno,
  • Yuko Sakamoto,
  • Maki Fukami,
  • Hirotomo Saitsu,
  • Tsutomu Ogata

DOI
https://doi.org/10.1038/s41598-022-21751-x
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 11

Abstract

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Abstract We report clinical and molecular findings in three Japanese patients with N-acetylneuraminic acid synthetase-congenital disorder of glycosylation (NANS-CDG). Patient 1 exhibited a unique constellation of clinical features including marked hydrocephalus, spondyloepimetaphyseal dysplasia (SEMD), and thrombocytopenia which is comparable to that of an infant reported by Faye-Peterson et al., whereas patients 2 and 3 showed Camera-Genevieve type SMED with intellectual/developmental disability which is currently known as the sole disease name for NANS-CDG. Molecular studies revealed a maternally inherited likely pathogenic c.207del:p.(Arg69Serfs*57) variant and a paternally derived likely pathogenic c.979_981dup:p.(Ile327dup) variant in patient 1, a homozygous likely pathogenic c.979_981dup:p.(Ile327dup) variant caused by maternal segmental isodisomy involving NANS in patient 2, and a paternally inherited pathogenic c.133−12T>A variant leading to aberrant splicing and a maternally inherited likely pathogenic c.607T>C:p.(Tyr203His) variant in patient 3 (reference mRNA: NM_018946.4). The results, together with previously reported data, imply that (1) NANS plays an important role in postnatal growth and fetal brain development; (2) SMED is recognizable at birth and shows remarkable postnatal evolution; (3) NANS-CDG is associated with low-normal serum sialic acid, obviously elevated urine N-acetylmannosamine, and normal N- and O-glycosylation of serum proteins; and (4) NANS-CDG is divided into Camera-Genevieve type and more severe Faye-Peterson type.