TY - JOUR
T1 - Genome-Wide Association Study of Chronic Dizziness in the Elderly Identifies Loci Implicating MLLT10, BPTF, LINC01224, and ROS1
AU - Million Veteran Program
AU - Clifford, Royce
AU - Munro, Daniel
AU - Dochtermann, Daniel
AU - Devineni, Poornima
AU - Pyarajan, Saiju
AU - Muralidhar, Sumitra
AU - Moser, Jennifer
AU - Deen, Jennifer E.
AU - Tsao, Philip S.
AU - Gaziano, J. Michael
AU - Hauser, Elizabeth
AU - Kilbourne, Amy
AU - Luoh, Shiuh Wen
AU - Matheny, Michael
AU - Oslin, Dave
AU - Churby, Lori
AU - Whitbourne, Stacey B.
AU - Brewer, Jessica V.
AU - Shayan, Shahpoor (Alex)
AU - Selva, Luis E.
AU - Pyarajan, Saiju
AU - Cho, Kelly
AU - DuVall, Scott L.
AU - Brophy, Mary T.
AU - Stephens, Brady
AU - Connor, Todd
AU - Argyres, Dean P.
AU - Assimes, Tim
AU - Hung, Adriana
AU - Kranzler, Henry
AU - Aguayo, Samuel
AU - Ahuja, Sunil
AU - Alexander, Kathrina
AU - Androulakis, Xiao M.
AU - Balasubramanian, Prakash
AU - Ballas, Zuhair
AU - Beckham, Jean
AU - Bhushan, Sujata
AU - Boyko, Edward
AU - Cohen, David
AU - Dellitalia, Louis
AU - Faulk, L. Christine
AU - Fayad, Joseph
AU - Fujii, Daryl
AU - Gappy, Saib
AU - Gesek, Frank
AU - Greco, Jennifer
AU - Godschalk, Michael
AU - Gress, Todd W.
AU - Gupta, Samir
N1 - Publisher Copyright:
© 2023, This is a U.S. Government work and not under copyright protection in the US; foreign copyright protection may apply.
PY - 2023/12
Y1 - 2023/12
N2 - Purpose: Chronic age-related imbalance is a common cause of falls and subsequent death in the elderly and can arise from dysfunction of the vestibular system, an elegant neuroanatomical group of pathways that mediates human perception of acceleration, gravity, and angular head motion. Studies indicate that 27–46% of the risk of age-related chronic imbalance is genetic; nevertheless, the underlying genes remain unknown. Methods: The cohort consisted of 50,339 cases and 366,900 controls in the Million Veteran Program. The phenotype comprised cases with two ICD diagnoses of vertigo or dizziness at least 6 months apart, excluding acute or recurrent vertiginous syndromes and other non-vestibular disorders. Genome-wide association studies were performed as individual logistic regressions on European, African American, and Hispanic ancestries followed by trans-ancestry meta-analysis. Downstream analysis included case-case-GWAS, fine mapping, probabilistic colocalization of significant variants and genes with eQTLs, and functional analysis of significant hits. Results: Two significant loci were identified in Europeans, another in the Hispanic population, and two additional in trans-ancestry meta-analysis, including three novel loci. Fine mapping revealed credible sets of intronic single nucleotide polymorphisms (SNPs) in MLLT10 - a histone methyl transferase cofactor, BPTF - a subunit of a nucleosome remodeling complex implicated in neurodevelopment, and LINC01224 - a proto-oncogene receptor tyrosine kinase. Conclusion: Despite the difficulties of phenotyping the nature of chronic imbalance, we replicated two loci from previous vertigo GWAS studies and identified three novel loci. Findings suggest candidates for further study and ultimate treatment of this common elderly disorder.
AB - Purpose: Chronic age-related imbalance is a common cause of falls and subsequent death in the elderly and can arise from dysfunction of the vestibular system, an elegant neuroanatomical group of pathways that mediates human perception of acceleration, gravity, and angular head motion. Studies indicate that 27–46% of the risk of age-related chronic imbalance is genetic; nevertheless, the underlying genes remain unknown. Methods: The cohort consisted of 50,339 cases and 366,900 controls in the Million Veteran Program. The phenotype comprised cases with two ICD diagnoses of vertigo or dizziness at least 6 months apart, excluding acute or recurrent vertiginous syndromes and other non-vestibular disorders. Genome-wide association studies were performed as individual logistic regressions on European, African American, and Hispanic ancestries followed by trans-ancestry meta-analysis. Downstream analysis included case-case-GWAS, fine mapping, probabilistic colocalization of significant variants and genes with eQTLs, and functional analysis of significant hits. Results: Two significant loci were identified in Europeans, another in the Hispanic population, and two additional in trans-ancestry meta-analysis, including three novel loci. Fine mapping revealed credible sets of intronic single nucleotide polymorphisms (SNPs) in MLLT10 - a histone methyl transferase cofactor, BPTF - a subunit of a nucleosome remodeling complex implicated in neurodevelopment, and LINC01224 - a proto-oncogene receptor tyrosine kinase. Conclusion: Despite the difficulties of phenotyping the nature of chronic imbalance, we replicated two loci from previous vertigo GWAS studies and identified three novel loci. Findings suggest candidates for further study and ultimate treatment of this common elderly disorder.
KW - Dizziness
KW - Genome-wide association studies
KW - Human
KW - Imbalance
KW - Vertigo
UR - http://www.scopus.com/inward/record.url?scp=85180714061&partnerID=8YFLogxK
U2 - 10.1007/s10162-023-00917-y
DO - 10.1007/s10162-023-00917-y
M3 - Article
C2 - 38036714
AN - SCOPUS:85180714061
SN - 1525-3961
VL - 24
SP - 575
EP - 591
JO - JARO - Journal of the Association for Research in Otolaryngology
JF - JARO - Journal of the Association for Research in Otolaryngology
IS - 6
ER -