PLoS ONE (Jan 2012)

The role of VEGF and KDR polymorphisms in moyamoya disease and collateral revascularization.

  • Young Seok Park,
  • Young Joo Jeon,
  • Hyun Seok Kim,
  • Kyu Young Chae,
  • Seung-Hun Oh,
  • In Bo Han,
  • Hyun Sook Kim,
  • Won-Chan Kim,
  • Ok-Joon Kim,
  • Tae Gon Kim,
  • Joong-Uhn Choi,
  • Dong-Seok Kim,
  • Nam Keun Kim

DOI
https://doi.org/10.1371/journal.pone.0047158
Journal volume & issue
Vol. 7, no. 10
p. e47158

Abstract

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We conducted a case-control study to investigate whether vascular endothelial growth factor (VEGF -2578, -1154, -634, and 936) and kinase insert domain containing receptor (KDR -604, 1192, and 1719) polymorphisms are associated with moyamoya disease. Korean patients with moyamoya disease (n = 107, mean age, 20.9±15.9 years; 66.4% female) and 243 healthy control subjects (mean age, 23.0±16.1 years; 56.8% female) were included. The subjects were divided into pediatric and adult groups. Among the 64 surgical patients, we evaluated collateral vessel formation after 2 years and divided patients into good (collateral grade A) or poor (collateral grade B and C) groups. The frequencies and distributions of four VEGF (-2578, -1154, -634, and 936) and KDR (-604, 1192, and 1719) polymorphisms were assessed from patients with moyamoya disease and compared to the control group. No differences were observed in VEGF -2578, -1154, -634, and 936 or KDR -604, 1192, and 1719 polymorphisms between the control group and moyamoya disease group. However, we found the -634CC genotype occurred less frequently in the pediatric moyamoya group (p = 0.040) whereas the KDR -604C/1192A/1719T haplotype increased the risk of pediatric moyamoya (p = 0.024). Patients with the CC genotype of VEGF -634 had better collateral vessel formation after surgery. Our results suggest that the VEGF -634G allele is associated with pediatric moyamoya disease and poor collateral vessel formation.