R E Reyes1, L Gao1, Z Zhang1, D L Davies1, L Asatryan2. 1. Titus Family Department of Clinical Pharmacy, School of Pharmacy, University of Southern California, 1985 Zonal Avenue, Los Angeles, CA 90033, United States. 2. Titus Family Department of Clinical Pharmacy, School of Pharmacy, University of Southern California, 1985 Zonal Avenue, Los Angeles, CA 90033, United States. Electronic address: asatryan@usc.edu.
Abstract
BACKGROUND: We have recently reported that oral treatment of adult male C57BL/6J mice with a non-absorbable antibiotic cocktail resulted in an increase in ethanol intake and in significant reductions in butyrate-producing gut microbiota populations. This work led us to hypothesize that reduction in butyrate levels within the gut is linked to antibiotic-induced increases in voluntary ethanol consumption. OBJECTIVE: This study tested whether ad libitum sodium butyrate supplementation can prevent antibiotic-induced ethanol consumption in mice. METHODS: Sodium butyrate was provided to adult male C57BL/6J mice in drinking water alone or in combination with antibiotic cocktail. Effects on ethanol (20%) intake were measured using drinking in the dark and modified 2-bottle choice paradigms. Body parameters, food and liquid intake, cecum, and adipose tissues were measured during and/or at the conclusion of the drinking in the dark study. Cecal 16s rRNA was analyzed for microbiota diversity and changes in specific bacterial phyla/species. RESULTS: In drinking in the dark, sodium butyrate supplementation prevented antibiotic-induced increases in ethanol intake without altering basal ethanol consumption. Furthermore, sodium butyrate supplementation lowered ethanol preference in the 2-bottle choice study. Ethanol intake was correlated to specific bacterial phyla/species. Sodium butyrate did not affect the changes in microbiota diversity and composition induced by antibiotic cocktail. CONCLUSIONS: The findings support a role of gut microbiota-derived butyrate in regulating alcohol-induced behaviors. Additionally, the work contributes to efforts in development of novel microbiome-based strategies as novel preventative and intervention-based therapeutics to address alcohol use disorder.
BACKGROUND: We have recently reported that oral treatment of adult male C57BL/6J mice with a non-absorbable antibiotic cocktail resulted in an increase in ethanol intake and in significant reductions in butyrate-producing gut microbiota populations. This work led us to hypothesize that reduction in butyrate levels within the gut is linked to antibiotic-induced increases in voluntary ethanol consumption. OBJECTIVE: This study tested whether ad libitum sodium butyrate supplementation can prevent antibiotic-induced ethanol consumption in mice. METHODS: Sodium butyrate was provided to adult male C57BL/6J mice in drinking water alone or in combination with antibiotic cocktail. Effects on ethanol (20%) intake were measured using drinking in the dark and modified 2-bottle choice paradigms. Body parameters, food and liquid intake, cecum, and adipose tissues were measured during and/or at the conclusion of the drinking in the dark study. Cecal 16s rRNA was analyzed for microbiota diversity and changes in specific bacterial phyla/species. RESULTS: In drinking in the dark, sodium butyrate supplementation prevented antibiotic-induced increases in ethanol intake without altering basal ethanol consumption. Furthermore, sodium butyrate supplementation lowered ethanol preference in the 2-bottle choice study. Ethanol intake was correlated to specific bacterial phyla/species. Sodium butyrate did not affect the changes in microbiota diversity and composition induced by antibiotic cocktail. CONCLUSIONS: The findings support a role of gut microbiota-derived butyrate in regulating alcohol-induced behaviors. Additionally, the work contributes to efforts in development of novel microbiome-based strategies as novel preventative and intervention-based therapeutics to address alcohol use disorder.
Authors: Yuri A Blednov; Pamela Metten; Deborah A Finn; Justin S Rhodes; Susan E Bergeson; R Adron Harris; John C Crabbe Journal: Alcohol Clin Exp Res Date: 2005-11 Impact factor: 3.455
Authors: Sophie Leclercq; Sébastien Matamoros; Patrice D Cani; Audrey M Neyrinck; François Jamar; Peter Stärkel; Karen Windey; Valentina Tremaroli; Fredrik Bäckhed; Kristin Verbeke; Philippe de Timary; Nathalie M Delzenne Journal: Proc Natl Acad Sci U S A Date: 2014-10-06 Impact factor: 11.205
Authors: Raymond K Walters; Renato Polimanti; Emma C Johnson; Jeanette N McClintick; Mark J Adams; Amy E Adkins; Fazil Aliev; Silviu-Alin Bacanu; Anthony Batzler; Sarah Bertelsen; Joanna M Biernacka; Tim B Bigdeli; Li-Shiun Chen; Toni-Kim Clarke; Yi-Ling Chou; Franziska Degenhardt; Anna R Docherty; Alexis C Edwards; Pierre Fontanillas; Jerome C Foo; Louis Fox; Josef Frank; Ina Giegling; Scott Gordon; Laura M Hack; Annette M Hartmann; Sarah M Hartz; Stefanie Heilmann-Heimbach; Stefan Herms; Colin Hodgkinson; Per Hoffmann; Jouke Jan Hottenga; Martin A Kennedy; Mervi Alanne-Kinnunen; Bettina Konte; Jari Lahti; Marius Lahti-Pulkkinen; Dongbing Lai; Lannie Ligthart; Anu Loukola; Brion S Maher; Hamdi Mbarek; Andrew M McIntosh; Matthew B McQueen; Jacquelyn L Meyers; Yuri Milaneschi; Teemu Palviainen; John F Pearson; Roseann E Peterson; Samuli Ripatti; Euijung Ryu; Nancy L Saccone; Jessica E Salvatore; Sandra Sanchez-Roige; Melanie Schwandt; Richard Sherva; Fabian Streit; Jana Strohmaier; Nathaniel Thomas; Jen-Chyong Wang; Bradley T Webb; Robbee Wedow; Leah Wetherill; Amanda G Wills; Jason D Boardman; Danfeng Chen; Doo-Sup Choi; William E Copeland; Robert C Culverhouse; Norbert Dahmen; Louisa Degenhardt; Benjamin W Domingue; Sarah L Elson; Mark A Frye; Wolfgang Gäbel; Caroline Hayward; Marcus Ising; Margaret Keyes; Falk Kiefer; John Kramer; Samuel Kuperman; Susanne Lucae; Michael T Lynskey; Wolfgang Maier; Karl Mann; Satu Männistö; Bertram Müller-Myhsok; Alison D Murray; John I Nurnberger; Aarno Palotie; Ulrich Preuss; Katri Räikkönen; Maureen D Reynolds; Monika Ridinger; Norbert Scherbaum; Marc A Schuckit; Michael Soyka; Jens Treutlein; Stephanie Witt; Norbert Wodarz; Peter Zill; Daniel E Adkins; Joseph M Boden; Dorret I Boomsma; Laura J Bierut; Sandra A Brown; Kathleen K Bucholz; Sven Cichon; E Jane Costello; Harriet de Wit; Nancy Diazgranados; Danielle M Dick; Johan G Eriksson; Lindsay A Farrer; Tatiana M Foroud; Nathan A Gillespie; Alison M Goate; David Goldman; Richard A Grucza; Dana B Hancock; Kathleen Mullan Harris; Andrew C Heath; Victor Hesselbrock; John K Hewitt; Christian J Hopfer; John Horwood; William Iacono; Eric O Johnson; Jaakko A Kaprio; Victor M Karpyak; Kenneth S Kendler; Henry R Kranzler; Kenneth Krauter; Paul Lichtenstein; Penelope A Lind; Matt McGue; James MacKillop; Pamela A F Madden; Hermine H Maes; Patrik Magnusson; Nicholas G Martin; Sarah E Medland; Grant W Montgomery; Elliot C Nelson; Markus M Nöthen; Abraham A Palmer; Nancy L Pedersen; Brenda W J H Penninx; Bernice Porjesz; John P Rice; Marcella Rietschel; Brien P Riley; Richard Rose; Dan Rujescu; Pei-Hong Shen; Judy Silberg; Michael C Stallings; Ralph E Tarter; Michael M Vanyukov; Scott Vrieze; Tamara L Wall; John B Whitfield; Hongyu Zhao; Benjamin M Neale; Joel Gelernter; Howard J Edenberg; Arpana Agrawal Journal: Nat Neurosci Date: 2018-11-26 Impact factor: 24.884