Gene and cell therapy on the acquisition and relapse-like binge drinking in a model of alcoholism: translational options

Yedy Israel; Quintanilla M.E.; Ezquer F.; Morales P.; Rivera-Meza M.; Karahanian E.; Ezquer M.; Herrera-Marschitz M.

dc.contributor.author	Yedy Israel
dc.contributor.author	Quintanilla M.E.
dc.contributor.author	Ezquer F.
dc.contributor.author	Morales P.
dc.contributor.author	Rivera-Meza M.
dc.contributor.author	Karahanian E.
dc.contributor.author	Ezquer M.
dc.contributor.author	Herrera-Marschitz M.
dc.date.accessioned	2020-09-02T22:30:37Z
dc.date.available	2020-09-02T22:30:37Z
dc.date.issued	2019
dc.identifier	10.1038/s41434-019-0064-9
dc.identifier.citation	26, 10-11, 407-417
dc.identifier.issn	09697128
dc.identifier.uri	https://hdl.handle.net/20.500.12728/6650
dc.description	Studies reviewed show that lentiviral gene therapy directed either at inhibiting the synthesis of brain acetaldehyde generated from ethanol or at degrading brain acetaldehyde fully prevent ethanol intake by rats bred for their high alcohol preference. However, after animals have chronically consumed alcohol, the above gene therapy did not inhibit alcohol intake, indicating that in the chronic ethanol intake condition brain acetaldehyde is no longer the compound that generates the continued alcohol reinforcement. Oxidative stress and neuroinflammation generated by chronic ethanol intake are strongly associated with the perpetuation of alcohol consumption and alcohol relapse “binge drinking”. Mesenchymal stem cells, referred to as guardians of inflammation, release anti-inflammatory cytokines and antioxidant products. The intravenous delivery of human mesenchymal stem cells or the intranasal administration of mesenchymal stem cell-generated exosomes reverses both (i) alcohol-induced neuro-inflammation and (ii) oxidative stress, and greatly (iii) inhibits (80–90%) chronic alcohol intake and relapse binge-drinking. The therapeutic effect of mesenchymal stem cells is mediated by increased levels of the brain GLT-1 glutamate transporter, indicating that glutamate signaling is pivotal for alcohol relapse. Human mesenchymal stem cells and the products released by these cells may have translational value in the treatment of alcohol-use disorders. © 2019, Springer Nature Limited.
dc.language.iso	en
dc.publisher	Springer Nature
dc.title	Gene and cell therapy on the acquisition and relapse-like binge drinking in a model of alcoholism: translational options
dc.type	Review

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Gene and cell therapy on the acquisition and relapse-like binge drinking in a model of alcoholism: translational options

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