Genetics and Molecular Biology (Aug 2017)

Exome sequencing identifies a novel mutation of the GDI1 gene in a Chinese non-syndromic X-linked intellectual disability family

  • Yongheng Duan,
  • Sheng Lin,
  • Lichun Xie,
  • Kaifeng Zheng,
  • Shiguo Chen,
  • Hui Song,
  • Xuchun Zeng,
  • Xueying Gu,
  • Heyun Wang,
  • Linghua Zhang,
  • Hao Shao,
  • Wenxu Hong,
  • Lijie Zhang,
  • Shan Duan

DOI
https://doi.org/10.1590/1678-4685-gmb-2016-0249
Journal volume & issue
Vol. 40, no. 3
pp. 591 – 596

Abstract

Read online

Abstract X-linked intellectual disability (XLID) has been associated with various genes. Diagnosis of XLID, especially for non-syndromic ones (NS-XLID), is often hampered by the heterogeneity of this disease. Here we report the case of a Chinese family in which three males suffer from intellectual disability (ID). The three patients shared the same phenotype: no typical clinical manifestation other than IQ score ≤ 70. For a genetic diagnosis for this family we carried out whole exome sequencing on the proband, and validated 16 variants of interest in the genomic DNA of all the family members. A missense mutation (c.710G > T), which mapped to exon 6 of the Rab GDP-Dissociation Inhibitor 1 (GDI1) gene, was found segregating with the ID phenotype, and this mutation changes the 237th position in the guanosine diphosphate dissociation inhibitor (GDI) protein from glycine to valine (p. Gly237Val). Through molecular dynamics simulations we found that this substitution results in a conformational change of GDI, possibly affecting the Rab-binding capacity of this protein. In conclusion, our study identified a novel GDI1 mutation that is possibly NS-XLID causative, and showed that whole exome sequencing provides advantages for detecting novel ID-associated variants and can greatly facilitate the genetic diagnosis of the disease.

Keywords