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dc.contributor.authorThorgeirsson, TE
dc.contributor.authorSteinberg, S
dc.contributor.authorReginsson, GW
dc.contributor.authorBjornsdottir, G
dc.contributor.authorRafnar, T
dc.contributor.authorJonsdottir, I
dc.contributor.authorHelgadottir, A
dc.contributor.authorGretarsdottir, S
dc.contributor.authorHelgadottir, H
dc.contributor.authorJonsson, S
dc.contributor.authorMatthiasson, SE
dc.contributor.authorGislason, T
dc.contributor.authorTyrfingsson, T
dc.contributor.authorGudbjartsson, T
dc.contributor.authorIsaksson, HJ
dc.contributor.authorHardardottir, H
dc.contributor.authorSigvaldason, A
dc.contributor.authorKiemeney, LA
dc.contributor.authorHaugen, Aage
dc.contributor.authorZienolddiny, Shanbeh
dc.contributor.authorWolf, HJ
dc.contributor.authorFranklin, WA
dc.contributor.authorPanadero, A
dc.contributor.authorMayordomo, JI
dc.contributor.authorHall, IP
dc.contributor.authorRönmark, E
dc.contributor.authorLundbäck, B
dc.contributor.authorDirksen, A
dc.contributor.authorAshraf, Haseem
dc.contributor.authorPedersen, JH
dc.contributor.authorMasson, G
dc.contributor.authorSulem, P
dc.contributor.authorThorsteinsdottir, U
dc.contributor.authorGudbjartsson, DF
dc.contributor.authorStefansson, K
dc.date.accessioned2024-09-06T06:46:57Z
dc.date.available2024-09-06T06:46:57Z
dc.date.created2016-06-17T10:52:25Z
dc.date.issued2016
dc.identifier.citationMolecular Psychiatry. 2016, 21 (5), 594-600.
dc.identifier.issn1359-4184
dc.identifier.urihttps://hdl.handle.net/11250/3150510
dc.description.abstractUsing Icelandic whole-genome sequence data and an imputation approach we searched for rare sequence variants in CHRNA4 and tested them for association with nicotine dependence. We show that carriers of a rare missense variant (allele frequency=0.24%) within CHRNA4, encoding an R336C substitution, have greater risk of nicotine addiction than non-carriers as assessed by the Fagerstrom Test for Nicotine Dependence (P=1.2 × 10−4). The variant also confers risk of several serious smoking-related diseases previously shown to be associated with the D398N substitution in CHRNA5. We observed odds ratios (ORs) of 1.7–2.3 for lung cancer (LC; P=4.0 × 10−4), chronic obstructive pulmonary disease (COPD; P=9.3 × 10−4), peripheral artery disease (PAD; P=0.090) and abdominal aortic aneurysms (AAAs; P=0.12), and the variant associates strongly with the early-onset forms of LC (OR=4.49, P=2.2 × 10−4), COPD (OR=3.22, P=2.9 × 10−4), PAD (OR=3.47, P=9.2 × 10−3) and AAA (OR=6.44, P=6.3 × 10−3). Joint analysis of the four smoking-related diseases reveals significant association (P=6.8 × 10−5), particularly for early-onset cases (P=2.1 × 10−7). Our results are in agreement with functional studies showing that the human α4β2 isoform of the channel containing R336C has less sensitivity for its agonists than the wild-type form following nicotine incubation.
dc.description.abstractA rare missense mutation in CHRNA4 associates with smoking behavior and its consequences
dc.language.isoeng
dc.titleA rare missense mutation in CHRNA4 associates with smoking behavior and its consequences
dc.title.alternativeA rare missense mutation in CHRNA4 associates with smoking behavior and its consequences
dc.typePeer reviewed
dc.typeJournal article
dc.description.versionpublishedVersion
dc.source.pagenumber594-600
dc.source.volume21
dc.source.journalMolecular Psychiatry
dc.source.issue5
dc.identifier.doi10.1038/mp.2016.13
dc.identifier.cristin1362138
cristin.ispublishedtrue
cristin.fulltextoriginal
cristin.qualitycode2


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