论文信息 - Unraveling the pectinolytic function of Bacteroides xylanisolvens using a RNA-seq approach and mutagenesis - 字舞流文

Unraveling the pectinolytic function of Bacteroides xylanisolvens using a RNA-seq approach and mutagenesis

BackgroundDiet and particularly dietary fibres have an impact on the gut microbiome and play an important role in human health and disease. Pectin is a highly consumed dietary fibre found in fruits and vegetables and is also a widely used additive in the food industry. Yet there is no information on the effect of pectin on the human gut microbiome. Likewise, little is known on gut pectinolytic bacteria and their enzyme systems. This study was undertaken to investigate the mechanisms of pectin degradation by the prominent human gut symbiont Bacteroides xylanisolvens.ResultsTranscriptomic analyses of B. xylanisolvens XB1A grown on citrus and apple pectins at mid- and late-log phases highlighted six polysaccharide utilization loci (PUL) that were overexpressed on pectin relative to glucose. The PUL numbers used in this report are those given by Terrapon et al. (Bioinformatics 31(5):647-55, 2015) and found in the PUL database: http://www.cazy.org/PULDB/. Based on their CAZyme composition, we propose that PUL 49 and 50, the most overexpressed PULs on both pectins and at both growth phases, are involved in homogalacturonan (HG) and type I rhamnogalacturonan (RGI) degradation, respectively. PUL 13 and PUL 2 could be involved in the degradation of arabinose-containing side chains and of type II rhamnogalacturonan (RGII), respectively. Considering that HG is the most abundant moiety (>70 %) within pectin, the importance of PUL 49 was further investigated by insertion mutagenesis into the susC-like gene. The insertion blocked transcription of the susC-like and the two downstream genes (susD-like/FnIII). The mutant showed strong growth reduction, thus confirming that PUL 49 plays a major role in pectin degradation.ConclusionThis study shows the existence of six PULs devoted to pectin degradation by B. xylanisolvens, one of them being particularly important in this function. Hence, this species deploys a very complex enzymatic machinery that probably reflects the structural complexity of pectin. Our findings also highlight the metabolic plasticity of B. xylanisolvens towards dietary fibres that contributes to its competitive fitness within the human gut ecosystem. Wider functional and ecological studies are needed to understand how dietary fibers and especially plant cell wall polysaccharides drive the composition and metabolism of the fibrolytic and non-fibrolytic community within the gut microbial ecosystem.

Bernard Henrissat | Nicolas Terrapon | Christopher J. Fields | Catherine M.G.C. Renard | Bryan A. White | Carl J. Yeoman | Margret E. Berg Miller | Pascale Lepercq | Carine Le Bourvellec | B. Henrissat | B. White | C. Yeoman | C. Fields | P. Mosoni | N. Terrapon | E. Forano | P. Lepercq | Grégory Jubelin | Jordane Despres | Evelyne Forano | Sophie Comtet-Marre | Grégory Jubelin | Pascale Mosoni | C. Le Bourvellec | S. Comtet-Marre | C. Renard | M. B. Miller | Jordane Despres

[1] Wei Shi,et al. featureCounts: an efficient general purpose program for assigning sequence reads to genomic features , 2013, Bioinform..

[2] A. Imberty,et al. Interactions between pectic compounds and procyanidins are influenced by methylation degree and chain length. , 2013, Biomacromolecules.

[3] B. Tjaden,et al. Computational analysis of bacterial RNA-Seq data , 2013, Nucleic acids research.

[4] J. Gordon,et al. Starch catabolism by a prominent human gut symbiont is directed by the recognition of amylose helices. , 2008, Structure.

[5] Bernard Henrissat,et al. The abundance and variety of carbohydrate-active enzymes in the human gut microbiota , 2013, Nature Reviews Microbiology.

[6] M. Morell,et al. Resistant Starches Protect against Colonic DNA Damage and Alter Microbiota and Gene Expression in Rats Fed a Western Diet123 , 2012, The Journal of nutrition.

[7] Leandro Martínez,et al. Medium Chain Fatty Acids Are Selective Peroxisome Proliferator Activated Receptor (PPAR) γ Activators and Pan-PPAR Partial Agonists , 2012, PloS one.

[8] P. Lerouge,et al. Pectins from citrus peel cell walls contain homogalacturonans homogenous with respect to molar mass, rhamnogalacturonan I and rhamnogalacturonan II , 2007 .

[9] H. Flint,et al. The influence of diet on the gut microbiota. , 2013, Pharmacological research.

[10] H. Englyst,et al. Determination of the non-starch polysaccharides in plant foods by gas-liquid chromatography of constituent sugars as alditol acetates. , 1982, The Analyst.

[11] J. Mikkelsen,et al. Pectin: new insights into an old polymer are starting to gel , 2006 .

[12] G. Frost,et al. Propionate. Anti-obesity and satiety enhancing factor? , 2011, Appetite.

[13] W. Verstraete,et al. Propionate as a health-promoting microbial metabolite in the human gut. , 2011, Nutrition reviews.

[14] Eric C. Martens,et al. Complex Glycan Catabolism by the Human Gut Microbiota: The Bacteroidetes Sus-like Paradigm , 2009, The Journal of Biological Chemistry.

[15] E. Bonnin,et al. Microbial Utilization and Selectivity of Pectin Fractions with Various Structures , 2011, Applied and Environmental Microbiology.

[16] P. Bork,et al. A human gut microbial gene catalogue established by metagenomic sequencing , 2010, Nature.

[17] F. Révillion,et al. Intestinal colonization with bifidobacteria affects the expression of galectins in extraintestinal organs. , 2009, FEMS immunology and medical microbiology.

[18] M. Leclerc,et al. Characterization of the xylan-degrading microbial community from human faeces. , 2007, FEMS microbiology ecology.

[19] Krakowie,et al. Health-promoting properties of pectin , 2014 .

[20] Matthew E. Ritchie,et al. limma powers differential expression analyses for RNA-sequencing and microarray studies , 2015, Nucleic acids research.

[21] Bernard Henrissat,et al. Recognition and Degradation of Plant Cell Wall Polysaccharides by Two Human Gut Symbionts , 2011, PLoS biology.

[22] Björn Usadel,et al. Trimmomatic: a flexible trimmer for Illumina sequence data , 2014, Bioinform..

[23] G. Bonheyo,et al. Starting a new genetic system: lessons from bacteroides. , 2000, Methods.

[24] E. Bonnin,et al. Pectin-modifying enzymes and pectin-derived materials: applications and impacts , 2013, Applied Microbiology and Biotechnology.

[25] Michel Paquot,et al. Effect of extraction conditions on the yield and purity of apple pomace pectin precipitated but not washed by alcohol. , 2007, Journal of food science.

[26] Vincent Lombard,et al. Automatic prediction of polysaccharide utilization loci in Bacteroidetes species , 2015, Bioinform..

[27] N. Blumenkrantz,et al. New method for quantitative determination of uronic acids. , 1973, Analytical biochemistry.

[28] Brandi L. Cantarel,et al. Complex Carbohydrate Utilization by the Healthy Human Microbiome , 2012, PloS one.

[29] C. Renard,et al. Comparison of the cell wall composition for flesh and skin from five different plums , 2009 .

[30] H. Brumer,et al. A discrete genetic locus confers xyloglucan metabolism in select human gut Bacteroidetes , 2014, Nature.

[31] Mark D. Robinson,et al. edgeR: a Bioconductor package for differential expression analysis of digital gene expression data , 2009, Bioinform..

[32] C. Renard,et al. Studies of the length of homogalacturonic regions in pectins by acid hydrolysis , 1993 .

[33] Pedro M. Coutinho,et al. The carbohydrate-active enzymes database (CAZy) in 2013 , 2013, Nucleic Acids Res..

[34] P. Mosoni,et al. Development of a RT-qPCR method for the quantification of Fibrobacter succinogenes S85 glycoside hydrolase transcripts in the rumen content of gnotobiotic and conventional sheep. , 2009, Journal of microbiological methods.

[35] S. Nakaji,et al. Comparison of the amount of pectin in the human terminal ileum with the amount of orally administered pectin. , 2005, Nutrition.

[36] T. R. Licht,et al. Intake of whole apples or clear apple juice has contrasting effects on plasma lipids in healthy volunteers , 2013, European Journal of Nutrition.

[37] R. Meli,et al. Potential beneficial effects of butyrate in intestinal and extraintestinal diseases , 2011 .

[38] B. Hamaker,et al. A perspective on the complexity of dietary fiber structures and their potential effect on the gut microbiota. , 2014, Journal of Molecular Biology.

[39] M. A. Millett,et al. Techniques for the determination of pulp constituents by quantitiative paper chromatography , 1954 .

[40] Thomas D. Schmittgen,et al. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method. , 2001, Methods.

[41] H. Flint,et al. Role of the gut microbiota in nutrition and health , 2018, British Medical Journal.

[42] Yookyung Kim,et al. Pectin as a bioactive polysaccharide – Extracting tailored function from less , 2014 .

[43] H. Harmsen,et al. Cultured Representatives of Two Major Phylogroups of Human Colonic Faecalibacterium prausnitzii Can Utilize Pectin, Uronic Acids, and Host-Derived Substrates for Growth , 2011, Applied and Environmental Microbiology.

[44] J. Pérez-Álvarez,et al. Resistant starch as functional ingredient: A review , 2010 .

[45] C. Mora,et al. Global Human Footprint on the Linkage between Biodiversity and Ecosystem Functioning in Reef Fishes , 2011, PLoS biology.

[46] B. Henrissat,et al. Glycan complexity dictates microbial resource allocation in the large intestine , 2015, Nature Communications.

[47] P. Chomczyński,et al. Single-step method of RNA isolation by acid guanidinium thiocyanate-phenol-chloroform extraction. , 1987, Analytical biochemistry.

[48] E. Bonnin,et al. Characterisation of pectin subunits released by an optimised combination of enzymes. , 2002, Carbohydrate research.