GDNF gene therapy for alcohol use disorder in male non-human primates

被引:0
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作者
Matthew M. Ford
Brianna E. George
Victor S. Van Laar
Katherine M. Holleran
Jerusha Naidoo
Piotr Hadaczek
Lauren E. Vanderhooft
Emily G. Peck
Monica H. Dawes
Kousaku Ohno
John Bringas
Jodi L. McBride
Lluis Samaranch
John R. Forsayeth
Sara R. Jones
Kathleen A. Grant
Krystof S. Bankiewicz
机构
[1] Oregon Health & Science University,Division of Neuroscience, Oregon National Primate Research Center
[2] Lewis & Clark College,Department of Psychology
[3] Wake Forest School of Medicine,Department of Physiology and Pharmacology
[4] The Ohio State University,Department of Neurological Surgery
[5] University of California,Department of Neurological Surgery
来源
Nature Medicine | 2023年 / 29卷
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摘要
Alcohol use disorder (AUD) exacts enormous personal, social and economic costs globally. Return to alcohol use in treatment-seeking patients with AUD is common, engendered by a cycle of repeated abstinence-relapse episodes even with use of currently available pharmacotherapies. Repeated ethanol use induces dopaminergic signaling neuroadaptations in ventral tegmental area (VTA) neurons of the mesolimbic reward pathway, and sustained dysfunction of reward circuitry is associated with return to drinking behavior. We tested this hypothesis by infusing adeno-associated virus serotype 2 vector encoding human glial-derived neurotrophic factor (AAV2-hGDNF), a growth factor that enhances dopaminergic neuron function, into the VTA of four male rhesus monkeys, with another four receiving vehicle, following induction of chronic alcohol drinking. GDNF expression ablated the return to alcohol drinking behavior over a 12-month period of repeated abstinence–alcohol reintroduction challenges. This behavioral change was accompanied by neurophysiological modulations to dopamine signaling in the nucleus accumbens that countered the hypodopaminergic signaling state associated with chronic alcohol use, indicative of a therapeutic modulation of limbic circuits countering the effects of alcohol. These preclinical findings suggest gene therapy targeting relapse prevention may be a potential therapeutic strategy for AUD.
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页码:2030 / 2040
页数:10
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