Literature DB >> 28877969

Overdominant Effect of a CHRNA4 Polymorphism on Cingulo-Opercular Network Activity and Cognitive Control.

Sepideh Sadaghiani1,2,3, Bernard Ng4,5, Andre Altmann4,6, Jean-Baptiste Poline7, Tobias Banaschewski8, Arun L W Bokde9, Uli Bromberg10, Christian Büchel10, Erin Burke Quinlan11, Patricia Conrod11, Sylvane Desrivières11, Herta Flor12,13, Vincent Frouin14, Hugh Garavan15, Penny Gowland16, Jürgen Gallinat17, Andreas Heinz17, Bernd Ittermann18, Jean-Luc Martinot19,20,21,22, Marie-Laure Paillère Martinot20,23, Hervé Lemaitre19, Frauke Nees8,12, Dimitri Papadopoulos Orfanos14, Tomáš Paus24, Luise Poustka25,26, Sabina Millenet8, Juliane H Fröhner27, Michael N Smolka27, Henrik Walter17, Robert Whelan28, Gunter Schumann11, Valerio Napolioni4, Michael Greicius4.   

Abstract

The nicotinic system plays an important role in cognitive control and is implicated in several neuropsychiatric conditions. However, the contributions of genetic variability in this system to individuals' cognitive control abilities are poorly understood and the brain processes that mediate such genetic contributions remain largely unidentified. In this first large-scale neuroimaging genetics study of the human nicotinic receptor system (two cohorts, males and females, fMRI total N = 1586, behavioral total N = 3650), we investigated a common polymorphism of the high-affinity nicotinic receptor α4β2 (rs1044396 on the CHRNA4 gene) previously implicated in behavioral and nicotine-related studies (albeit with inconsistent major/minor allele impacts). Based on our prior neuroimaging findings, we expected this polymorphism to affect neural activity in the cingulo-opercular (CO) network involved in core cognitive control processes including maintenance of alertness. Consistent across the cohorts, all cortical areas of the CO network showed higher activity in heterozygotes compared with both types of homozygotes during cognitive engagement. This inverted U-shaped relation reflects an overdominant effect; that is, allelic interaction (cumulative evidence p = 1.33 * 10-5). Furthermore, heterozygotes performed more accurately in behavioral tasks that primarily depend on sustained alertness. No effects were observed for haplotypes of the surrounding CHRNA4 region, supporting a true overdominant effect at rs1044396. As a possible mechanism, we observed that this polymorphism is an expression quantitative trait locus modulating CHRNA4 expression levels. This is the first report of overdominance in the nicotinic system. These findings connect CHRNA4 genotype, CO network activation, and sustained alertness, providing insights into how genetics shapes individuals' cognitive control abilities.SIGNIFICANCE STATEMENT The nicotinic acetylcholine system plays a central role in neuromodulatory regulation of cognitive control processes and is dysregulated in several neuropsychiatric disorders. Despite this functional importance, no large-scale neuroimaging genetics studies have targeted the contributions of genetic variability in this system to human brain activity. Here, we show the impact of a common polymorphism of the high-affinity nicotinic receptor α4β2 that is consistent across brain activity and behavior in two large human cohorts. We report a hitherto unknown overdominant effect (allelic interaction) at this locus, where the heterozygotes show higher activity in the cingulo-opercular network underlying alertness maintenance and higher behavioral alertness performance than both homozygous groups. This gene-brain-behavior relationship informs about the biological basis of interindividual differences in cognitive control.
Copyright © 2017 the authors 0270-6474/17/379658-10$15.00/0.

Entities:  

Keywords:  alertness; cingulo-opercular network; fMRI; genetics; nicotinic acetylcholine receptor; polymorphism

Mesh:

Substances:

Year:  2017        PMID: 28877969      PMCID: PMC6596609          DOI: 10.1523/JNEUROSCI.0991-17.2017

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


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