Mild Phenotype of Wolfram Syndrome Associated With a Common Pathogenic Variant Is Predicted by a Structural Model of Wolframin.

Adi Wilf-YarkoniOded ShorAvi FellnerMark Andrew HellmannElon PrasHagit YonathShiri Shkedi-RafidLina Basel-SalmonLili BazakRuth EliahouLior GreenbaumHadas Stiebel-KalishFelix BenningerYael Goldberg

Published in: Neurology. Genetics (2021)

The p.R558C variant causes a milder, late-onset phenotype of WS. We report a structural model of wolframin protein based on empirical functional studies and use NMA modeling to show a genotype-phenotype correlation across all homozygotes. Clinicians should be alert to this condition in patients with juvenile diabetes and patients of any age with a combination of diabetes and optic atrophy. Computational NMA has potential benefit for prediction of the genotype-phenotype relationship.

Keyphrases

late onset
type diabetes
end stage renal disease
cardiovascular disease
early onset
newly diagnosed
chronic kidney disease
ejection fraction
peritoneal dialysis
palliative care
optical coherence tomography
case report
skeletal muscle