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Associating CYP2A6 structural variants with ovarian and lung cancer risk in the UK Biobank: replication and extension

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  • Alec W. R. Langlois
  • Jennie G. Pouget
  • Jo Knight
  • Meghan J. Chenoweth
  • Rachel F. Tyndale
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<mark>Journal publication date</mark>1/03/2024
<mark>Journal</mark>European Journal of Human Genetics
Issue number3
Volume32
Number of pages4
Pages (from-to)357-360
Publication StatusPublished
Early online date14/12/23
<mark>Original language</mark>English

Abstract

CYP2A6 is a polymorphic enzyme that inactivates nicotine; structural variants (SVs) include gene deletions and hybrids with the neighboring pseudogene CYP2A7. Two studies found that CYP2A7 deletions were associated with ovarian cancer risk. Using their methodology, we aimed to characterize CYP2A6 SVs (which may be misidentified by prediction software as CYP2A7 SVs), then assess CYP2A6 SV-associated risk for ovarian cancer, and extend analyses to lung cancer. An updated reference panel was created to impute CYP2A6 SVs from UK Biobank array data. Logistic regression models analyzed the association between CYP2A6 SVs and cancer risk, adjusting for covariates. Software-predicted CYP2A7 deletions were concordant with known CYP2A6 SVs. Deleterious CYP2A6 SVs were not associated with ovarian cancer (OR = 1.06; 95% CI: 0.80-1.37; p = 0.7) but did reduce the risk of lung cancer (OR = 0.44; 95% CI: 0.29-0.64; p