Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease (Dec 2023)

Chromosome 10q24.32 Variants Associate With Brain Arterial Diameters in Diverse Populations: A Genome‐Wide Association Study

  • Minghua Liu,
  • Farid Khasiyev,
  • Sanjeev Sariya,
  • Antonio Spagnolo‐Allende,
  • Danurys L Sanchez,
  • Howard Andrews,
  • Qiong Yang,
  • Alexa Beiser,
  • Ye Qiao,
  • Emy A Thomas,
  • Jose Rafael Romero,
  • Tatjana Rundek,
  • Adam M Brickman,
  • Jennifer J Manly,
  • Mitchell SV Elkind,
  • Sudha Seshadri,
  • Christopher Chen,
  • Saima Hilal,
  • Bruce A Wasserman,
  • Giuseppe Tosto,
  • Myriam Fornage,
  • Jose Gutierrez

DOI
https://doi.org/10.1161/JAHA.123.030935
Journal volume & issue
Vol. 12, no. 23

Abstract

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Background Brain arterial diameters (BADs) are novel imaging biomarkers of cerebrovascular disease, cognitive decline, and dementia. Traditional vascular risk factors have been associated with BADs, but whether there may be genetic determinants of BADs is unknown. Methods and Results The authors studied 4150 participants from 6 geographically diverse population‐based cohorts (40% European, 14% African, 22% Hispanic, 24% Asian ancestries). Brain arterial diameters for 13 segments were measured and averaged to obtain a global measure of BADs as well as the posterior and anterior circulations. A genome‐wide association study revealed 14 variants at one locus associated with global BAD at genome‐wide significance (P<5×10−8) (top single‐nucleotide polymorphism, rs7921574; β=0.06 [P=1.54×10−8]). This locus mapped to an intron of CNNM2. A trans‐ancestry genome‐wide association study meta‐analysis identified 2 more loci at NT5C2 (rs10748839; P=2.54×10−8) and AS3MT (rs10786721; P=4.97×10−8), associated with global BAD. In addition, 2 single‐nucleotide polymorphisms colocalized with expression of CNNM2 (rs7897654; β=0.12 [P=6.17×10−7]) and AL356608.1 (rs10786719; β=−0.17 [P=6.60×10−6]) in brain tissue. For the posterior BAD, 2 variants at one locus mapped to an intron of TCF25 were identified (top single‐nucleotide polymorphism, rs35994878; β=0.11 [P=2.94×10−8]). For the anterior BAD, one locus at ADAP1 was identified in trans‐ancestry genome‐wide association analysis (rs34217249; P=3.11×10−8). Conclusions The current study reveals 3 novel risk loci (CNNM2, NT5C2, and AS3MT) associated with BADs. These findings may help elucidate the mechanism by which BADs may influence cerebrovascular health.

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