| Literature DB >> 32045262 |
Maria Ibars1, Matthew T Maier1, Ernie Yulyaningsih1, Luz Perez1, Rachel Cheang1, Anna Vilhelmsson1, Sharon M Louie2, Scott A Wegner3, Xiaoyi Yuan4, Holger K Eltzschig4, Frederic W Hopf3, Daniel K Nomura2, Suneil K Koliwad1,5, Allison W Xu1,6.
Abstract
Excessive alcohol consumption, including binge drinking, is a common cause of fatty liver disease. Binge drinking rapidly induces hepatic steatosis, an early step in the pathogenesis of chronic liver injury. Despite its prevalence, the process by which excessive alcohol consumption promotes hepatic lipid accumulation remains unclear. Alcohol exerts potent effects on the brain, including hypothalamic neurons crucial for metabolic regulation. However, whether or not the brain plays a role in alcohol-induced hepatic steatosis is unknown. In the brain, alcohol increases extracellular levels of adenosine, a potent neuromodulator, and previous work implicates adenosine signaling as being important for the development of alcoholic fatty liver disease. Acute alcohol exposure also increases both the activity of agouti-related protein (AgRP)-expressing neurons and AgRP immunoreactivity. Here, we show that adenosine receptor A2B signaling in the brain modulates the extent of alcohol-induced fatty liver in mice and that both the AgRP neuropeptide and the sympathetic nervous system are indispensable for hepatic steatosis induced by bingelike alcohol consumption. Together, these results indicate that the brain plays an integral role in alcohol-induced hepatic lipid accumulation and that central adenosine signaling, hypothalamic AgRP, and the sympathetic nervous system are crucial mediators of this process.Entities:
Keywords: AgRP; adenosine signaling; alcohol; binge drinking; hepatic steatosis
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Year: 2020 PMID: 32045262 PMCID: PMC7272724 DOI: 10.1152/ajpendo.00218.2019
Source DB: PubMed Journal: Am J Physiol Endocrinol Metab ISSN: 0193-1849 Impact factor: 5.900