Molecular Genetics & Genomic Medicine (Jan 2014)

Two novel mutations identified in familial cases with Donohue syndrome

  • Tzipora C. Falik Zaccai,
  • Limor Kalfon,
  • Aharon Klar,
  • Mordechai Ben Elisha,
  • Haggit Hurvitz,
  • Galina Weingarten,
  • Emelia Chechik,
  • Vered Fleisher Sheffer,
  • Raid Haj Yahya,
  • Gal Meidan,
  • Eva Gross‐Kieselstein,
  • Dvora Bauman,
  • Sylvia Hershkovitz,
  • Yuval Yaron,
  • Avi Orr‐Urtreger,
  • Efrat Wertheimer

DOI
https://doi.org/10.1002/mgg3.43
Journal volume & issue
Vol. 2, no. 1
pp. 64 – 72

Abstract

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Abstract Donohue syndrome (DS) is a rare and lethal autosomal recessive disease caused by mutations in the insulin receptor (INSR) gene, manifesting marked insulin resistance, severe growth retardation, hypertrichosis, and characteristic dysmorphic features. We report the clinical, molecular, and biochemical characterization of three new patients with DS, and address genotype–phenotype issues playing a role in the pathophysiology of DS. A female infant born to first‐degree cousins Muslim Arab parents and two brothers born to first‐degree cousins Druze parents presented classical features of DS with hypertrophic cardiomyopathy and died in infancy. Each patient was found homozygous for one missense mutation within the extracellular domain of the INSR gene. Western blot analysis identified the proreceptor of INSR, but not its mature subunits alpha and beta. Of 95 healthy Muslims, no heterozygous was found and of 52 healthy Druze from the same village, one was heterozygous. This study presents two novel familial mutations in the alpha subunit of the INSR which appear to impair post‐translational processing of the INSR, resulting loss of its function. Both mutations cause DS with hypertrophic cardiomyopathy and early death. Identification of the causative mutation enables prevention of this devastating disease.

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