PLoS ONE (Jan 2015)

Adult Moyamoya Disease: A Burden of Intracranial Stenosis in East Asians?

  • Oh Young Bang,
  • Sookyung Ryoo,
  • Suk Jae Kim,
  • Chang Hyo Yoon,
  • Jihoon Cha,
  • Je Young Yeon,
  • Keon Ha Kim,
  • Gyeong-Moon Kim,
  • Chin-Sang Chung,
  • Kwang Ho Lee,
  • Hyung Jin Shin,
  • Chang-Seok Ki,
  • Pyoung Jeon,
  • Jong-Soo Kim,
  • Seung Chyul Hong

DOI
https://doi.org/10.1371/journal.pone.0130663
Journal volume & issue
Vol. 10, no. 6
p. e0130663

Abstract

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Both Moyamoya disease (MMD) and intracranial atherosclerotic stenosis (ICAS) are more prevalent in Asians than in Westerners. We hypothesized that a substantial proportion of patients with adult-onset MMD were misclassified as having ICAS, which may in part explain the high prevalence of intracranial atherosclerotic stroke in Asians.We analyzed 352 consecutive patients with ischemic events within the MCA distribution and relevant intracranial arterial stenosis, but no demonstrable carotid or cardiac embolism sources. Conventional angiography was performed in 249 (70.7%) patients, and the remains underwent MRA. The occurrence of the c.14429G>A (p.Arg4810Lys) variant in ring finger protein 213 (RNF213) was analyzed. This gene was recently identified as a susceptibility gene for MMD in East Asians.The p.Arg4810Lys variant was observed in half of patients with intracranial stenosis (176 of 352, 50.0%), in no healthy control subjects (n = 51), and in 3.2% of stroke control subjects (4 of 124 patients with other etiologies). The presence of basal collaterals, bilateral involvement on angiography, and absence of diabetes were independently associated with the presence of the RNF213 variant. Among 131 patients who met all three diagnostic criteria and were diagnosed with MMD, three-fourths (75.6%) had this variant. However, a significant proportion of patients who met two criteria (57.7%), one criterion (28.6%), or no criteria (20.0%) also had this variant. Some of them developed typical angiographic findings of MMD on follow-up angiography.Careful consideration of MMD is needed when diagnosing ICAS because differential therapeutic strategies are required for these diseases and due to the limitations of the current diagnostic criteria for MMD.