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NuGO week 2016 Role of the gut microbiota in overand undernutrition Laure Bindels, PhD Copenhagen September 7, 2016 Adapted from Delzenne et al., Nat Rev Endocrinol 2011 Outline 1. 2. 3. 4. Gut microbiota as a nutritional target Metabolic disorders associated with obesity Metabolic disorders associated with cancer Gut microbiota in alcohol-dependent patients The gut microbiota 40 000 000 000 000 microbes 30 000 000 000 000 human cells for a 'reference man' (70 kilograms, 20–30 years old and 1.7 meters tall) Numbers from Sender et al, preprint on bioRxiv, 2016. Neish, Gastroenterology 2009 Gut microbiota-host crosstalk Delzenne et al., Nat Rev Endocrinol 2011 Prebiotics i.e. inulin-type fructans Probiotics i.e. lactobacilli Bacteriocins Antibiotics FMT Gut microbiota Experimental tools to study our microbial partners Adapted from Bindels & Delzenne, Int J Biochem Cell Biol 2013 Prebiotics Beneficial physiological effects Gibson & Roberfroid, J Nutr 1995 Future research on prebiotics Figure 1 Current and proposed definitions for the concept of prebiotics Bindels et al, Nat Rev Gastroenterol Hepatol 2015 Resistant starches Resistant starches (RS) include all starch and starch degradation products not absorbed in the small intestine of healthy individuals. Asp, Trends Food Sci Technol, 1992; Birt et al., Adv Nutr 2013; Martinez et al, Plos ONE 2010. Outline 1. 2. 3. 4. Gut microbiota as a nutritional target Metabolic disorders associated with obesity Metabolic disorders associated with cancer Gut microbiota in alcohol-dependent patients Cancer cachexia Bindels & Thissen, Clin Nutr Exp 2015 Cancer cachexia • Up to 80% of cancer patients, depending of the tumor site • Reduces quality and length of life • May be a cause of cancer therapy discontinuation • No valid treatment Giacometti, Walking man Fearon et al., Cell Metab 2012; Fearon et al., Nat Rev Oncol 2013; Argiles et al, Nat Rev Cancer 2014. A microbial signature in cancer cachexia Community-wide approach to characterize the gut microbiota in two mouse models of cancer cachexia C26 BaF BaF3 cells with Bcr-Abl Bindels et al, The ISME J 2016 A microbial signature in cancer cachexia BaF 16S rRNA genes from the caecal microbiota analysed by Illumina MiSeq. Logarythmic LDA score. ↑ Enterobacteriaceae ↑ Parabacteroides goldsteinii ↓ Lactobacilli With Inès Martinez and Jens Walter Bindels et al, The ISME J 2016 C26 … independent of the food intake Enterobacteriaceae (log10 [cells/g]) Daily food intake (% initial food intake) * 11 125 100 75 # CT (BaF) BaF CT (DR) DR 50 25 # * 0 10 *** *** ** 9 8 7 6 0 2 4 6 8 10 12 14 CT(BaF) BaF CT(DR) DR CT(BaF) BaF CT(DR) DR Days after BAF injection Lactobacillus spp. (log10 [cells/g]) *** *** *** Parabacteroides goldsteinii ASF519 (log10 [AU/g]) * 10 9 8 CT(BaF) BaF CT(DR) Bindels et al, The ISME J 2016 DR 11 10 9 8 7 1 .0 5.0 10 6 § * * 0 0 24 48 Acetate 72 mRNAlevels (relativeexpression) Number of intact BaF3/w ell BaF B c r-A b l control propionate 2mM 1.0 10 7 Propionate Butyrate 0 .5 0 .0 N D CT BBaF3-ITF aF3 ITF Acetate P r o p i o n a t e Propionate §Butyrate 6 0 µM 4 0 2 0 Acetate Propionate Butyrate 0 BaF3-ITF BaF3 CT Bindels et al, Br J Cancer 2012; Bindels*, Neyrinck* et al, Plos ONE 2015. Selected synbiotic approach D0 D1 D13 L. reuteri 100-23 Bcr-Abl-expressing BaF3 cells Bindels et al, The ISME J 2016 † ITF With Bruno Pot & Corinne Grangette BaF 16S rRNA genes from the caecal microbiota analysed by Illumina MiSeq. LEfSe cladogram. Bindels et al, The ISME J 2016 Benefits of the synbiotic approach Bcr-Abl BaF 0.45 1.0 # 0.5 Organ weight (% body weight) mRNA levels (relative expression) 0.50 * 0.40 0.35 0.20 * 0.15 *$ 0.10 0.05 ND 0.0 0.00 CT CT BaF BaF-LrI BaF BaF-LrI CT tibialis Morbidity score 5 1.2 4 1.0 3 ## 2 1 0 BaF BaF-LrI gastrocnemius Survival Fraction survival Score *# BaF BaF-LrI p = 0.007 median survival + 2 days 0.8 0.6 0.4 0.2 0.0 BaF BaF-LrI 0 5 10 15 Days after BaF injection Bindels et al, The ISME J 2016 20 Hypothetical role of the gut barrier Bindels & Thissen, Clin Nutr Exp 2015 Hypothetical role of the gut barrier Gut permeability BaF mRNA levels (relative expression) ↘ Gut permeability ↗ 1.5 # # 1.0 * * CT BaF BaF-LrI # * 0.5 0.0 occludin ZO-1 Muc2 proglucagon Paneth cell differentiation and antimicrobials ↘ Antimicrobial peptides ↗ ↘ Immune system ↗ mRNA levels (relative expression) 1.5 # # 1.0 * *# * * 0.5 * 0.0 Lysozyme -defensins Reg3 TCF4 Pla2g2 ↘ Decreased in leukemic mice ↗ Increased by synbiotics mRNA levels (relative expression) 2.0 *# # 1.5 0.5 * $ * * * 0.0 CD3 Bindels et al, The ISME J 2016 # # # 1.0 Tbet IL-17A Foxp3 lymphocytes IL-10 Ebi3 Current working model Gut barrier function Cancer cachexia Probiotics ? Propionate Prebiotics New metabolites ? Outline 1. 2. 3. 4. Gut microbiota as a nutritional target Metabolic disorders associated with obesity Metabolic disorders associated with cancer Gut microbiota in alcohol-dependent patients A role for the gut permeability? Leclercq et al, Brain Behav Immun 2012; Leclercq et al, Biol Psychiatry 2014. A role for the gut permeability ? Leclercq et al, PNAS 2014 Dysbiosis Leclercq et al, PNAS 2014 Altered fecal metabolite profil Analysis of Volatile organic compounds by gas-chromatography-mass spectrometry (K. Verbeke, Kuleuven B) Bi-plot analysis reveals ADT1 HP- versus LP are differentiated (14 metabolites) Leclercq et al, PNAS 2014 Conclusions • Importance of the prebiotic concept. • Microbiota-dependent and independent effects of functional foods: strategies to demonstrate causality exist. • Underexplored areas could benefit from targeted prebiotic or synbiotic approaches. Carlos Gomes Neto Hatem Kittana Rafael Segura Munoz UNL Gnotobiotic Mouse Facility Robert Schmaltz Brandon White Prof. Amanda Ramer-Tait Liz Cody Prof. Jens Walter Dr. Inés Martínez FSR Fellowship Maria Isabel Quintero Junyi Yang Maria Ximena Maldonado-Gomez Post-doc position in July 2017 : [email protected] Prof N. Delzenne Dr A. Neyrinck Prof P. Cani UCL (BE) Prof G. Muccioli Prof P. Buc Calderon Prof J.P. Thissen Prof O. Feron Prof P. Sonveaux Dr P. Porporato Dr J. Verrax Dr R. Beck UCL (BE) Prof E. Hermans Dr B. Koener Dr O. Schakman Prof J. Mahillon Prof J.B. Demoulin Dr V. Havelange Dr Fl. Bindels ULG (BE) Dr B. Taminiau Prof G. Daube E. François Prof C. Blecker Prof A. Richel Katholieke Universiteit Leuven (BE) Dr H. Schoemans Prof J. Maertens University of Alberta (CA) Prof J. Walter Dr I. Martinez Rowett Institute, Aberdeen (UK) Dr K.P. Scott and J.C. Martin University of Reading (UK) Prof S. P. Claus and C. Leroy Institut Pasteur, Lille (FR) Prof B. Pot and Dr C. Grangette