Genome-wide association study reveals multiple loci for nociception and opioid consumption behaviors associated with heroin vulnerability in outbred rats

Author:

Kuhn Brittany N.ORCID,Cannella NazzarenoORCID,Chitre Apurva S.ORCID,Nguyen Khai-Minh H.ORCID,Cohen KatarinaORCID,Chen DenghuiORCID,Peng BeverlyORCID,Ziegler Kendra S.ORCID,Lin Bonnie,Johnson Benjamin B.ORCID,Missfeldt Sanches ThiagoORCID,Crow Ayteria D.ORCID,Lunerti VeronicaORCID,Gupta ArkobratoORCID,Dereschewitz Eric,Soverchia Laura,Hopkins Jordan L.ORCID,Roberts Analyse T.ORCID,Ubaldi MassimoORCID,Abdulmalek SarahORCID,Kinen AnaliaORCID,Hardiman GaryORCID,Chung DongjunORCID,Polesskaya OksanaORCID,Solberg Woods Leah C.ORCID,Ciccocioppo RobertoORCID,Kalivas Peter W.ORCID,Palmer Abraham A.ORCID

Abstract

AbstractThe increased prevalence of opioid use disorder (OUD) makes it imperative to disentangle the biological mechanisms contributing to individual differences in OUD vulnerability. OUD shows strong heritability, however genetic variants contributing toward vulnerability remain poorly defined. We performed a genome-wide association study using over 850 male and female heterogeneous stock (HS) rats to identify genes underlying behaviors associated with OUD such as nociception, as well as heroin-taking, extinction and seeking behaviors. By using an animal model of OUD, we were able to identify genetic variants associated with distinct OUD behaviors while maintaining a uniform environment, an experimental design not easily achieved in humans. Furthermore, we used a novel non-linear network-based clustering approach to characterize rats based on OUD vulnerability to assess genetic variants associated with OUD susceptibility. Our findings confirm the heritability of several OUD-like behaviors, including OUD susceptibility. Additionally, several genetic variants associated with nociceptive threshold prior to heroin experience, heroin consumption, escalation of intake, and motivation to obtain heroin were identified.Tom1, a microglial component, was implicated for nociception. Several genes involved in dopaminergic signaling, neuroplasticity and substance use disorders, includingBrwd1,Pcp4, Phb1l2andMmp15were implicated for the heroin traits. Additionally, an OUD vulnerable phenotype was associated with genetic variants for consumption and break point, suggesting a specific genetic contribution for OUD-like traits contributing to vulnerability. Together, these findings identify novel genetic markers related to the susceptibility to OUD-relevant behaviors in HS rats.

Publisher

Cold Spring Harbor Laboratory

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