Biomedicines (Sep 2022)

Does the c.-14C>T Mutation in the <i>IFITM5</i> Gene Provide Identical Phenotypes for Osteogenesis Imperfecta Type V? Data from Russia and a Literature Review

  • Anton Tyurin,
  • Elena Merkuryeva,
  • Aliya Zaripova,
  • Tatyana Markova,
  • Tatyana Nagornova,
  • Ilya Dantsev,
  • Dina Nadyrshina,
  • Ekaterina Zakharova,
  • Rita Khusainova

DOI
https://doi.org/10.3390/biomedicines10102363
Journal volume & issue
Vol. 10, no. 10
p. 2363

Abstract

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Osteogenesis imperfecta (OI) is a large group of genetically heterogeneous diseases resulting from decreased bone density and an abnormal microarchitecture, which are clinically manifested by abnormal bone fractures. A distinctive clinical feature of this group of diseases is the presence of spontaneous fractures and skeletal deformities. However, the clinical manifestations of different types of OI are characterized by marked polymorphism with variable severity of skeletal and extra-skeletal features. Previous studies have shown that a mutation (c.-14C>T) in the IFITM5 gene is responsible for autosomal dominant OI type V. However, the mutation has a variable expression pattern and marked clinical heterogeneity. In this study, a clinical and genetic analysis of 12 cases with molecularly confirmed OI type V from 12 unrelated families was performed. Significant clinical heterogeneity of the disease with the same molecular defect was detected. In six subjects (50%), there were no classic signs of OI type V (formation of a hyperplastic bone callus, calcification of the interosseous membrane and dislocation of the radial head). In all cases, the mutation occurred de novo.

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