BMC Medical Genetics (Nov 2012)

Adult siblings with homozygous <it>G6PC3</it> mutations expand our understanding of the severe congenital neutropenia type 4 (SCN4) phenotype

  • Fernandez Bridget A,
  • Green Jane S,
  • Bursey Ford,
  • Barrett Brendan,
  • MacMillan Andrée,
  • McColl Sarah,
  • Fernandez Sara,
  • Rahman Proton,
  • Mahoney Krista,
  • Pereira Sergio L,
  • Scherer Stephen W,
  • Boycott Kym M,
  • Woods Michael O

DOI
https://doi.org/10.1186/1471-2350-13-111
Journal volume & issue
Vol. 13, no. 1
p. 111

Abstract

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Abstract Background Severe congenital neutropenia type 4 (SCN4) is an autosomal recessive disorder caused by mutations in the third subunit of the enzyme glucose-6-phosphatase (G6PC3). Its core features are congenital neutropenia and a prominent venous skin pattern, and affected individuals have variable birth defects. Oculocutaneous albinism type 4 (OCA4) is caused by autosomal recessive mutations in SLC45A2. Methods We report a sister and brother from Newfoundland, Canada with complex phenotypes. The sister was previously reported by Cullinane et al., 2011. We performed homozygosity mapping, next generation sequencing and conventional Sanger sequencing to identify mutations that cause the phenotype in this family. We have also summarized clinical data from 49 previously reported SCN4 cases with overlapping phenotypes and interpret the medical histories of these siblings in the context of the literature. Results The siblings’ phenotype is due in part to a homozygous mutation in G6PC3, [c.829C > T, p.Gln277X]. Their ages are 38 and 37 years respectively and they are the oldest SCN4 patients published to date. Both presented with congenital neutropenia and later developed Crohn disease. We suggest that the latter is a previously unrecognized SCN4 manifestation and that not all affected individuals have an intellectual disability. The sister also has a homozygous mutation in SLC45A2, which explains her severe oculocutaneous hypopigmentation. Her brother carried one SLC45A2 mutation and was diagnosed with “partial OCA” in childhood. Conclusions This family highlights that apparently novel syndromes can in fact be caused by two known autosomal recessive disorders.

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