Literature DB >> 25756679

Clostridium difficile heterogeneously impacts intestinal community architecture but drives stable metabolome responses.

David Rojo1, María J Gosalbes2,3, Rafaela Ferrari2,3, Ana E Pérez-Cobas2,3, Ester Hernández4, Rosa Oltra5, Javier Buesa6, Amparo Latorre2,3, Coral Barbas1, Manuel Ferrer4, Andrés Moya2,3.   

Abstract

Clostridium difficile-associated diarrhoea (CDAD) is caused by C. difficile toxins A and B and represents a serious emerging health problem. Yet, its progression and functional consequences are unclear. We hypothesised that C. difficile can drive major measurable metabolic changes in the gut microbiota and that a relationship with the production or absence of toxins may be established. We tested this hypothesis by performing metabolic profiling on the gut microbiota of patients with C. difficile that produced (n=6) or did not produce (n=4) toxins and on non-colonised control patients (n=6), all of whom were experiencing diarrhoea. We report a statistically significant separation (P-value <0.05) among the three groups, regardless of patient characteristics, duration of the disease, antibiotic therapy and medical history. This classification is associated with differences in the production of distinct molecules with presumptive global importance in the gut environment, disease progression and inflammation. Moreover, although severe impaired metabolite production and biological deficits were associated with the carriage of C. difficile that did not produce toxins, only previously unrecognised selective features, namely, choline- and acetylputrescine-deficient gut environments, characterised the carriage of toxin-producing C. difficile. Additional results showed that the changes induced by C. difficile become marked at the highest level of the functional hierarchy, namely the metabolic activity exemplified by the gut microbial metabolome regardless of heterogeneities that commonly appear below the functional level (gut bacterial composition). We discuss possible explanations for this effect and suggest that the changes imposed by CDAD are much more defined and predictable than previously thought.

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Year:  2015        PMID: 25756679      PMCID: PMC4579473          DOI: 10.1038/ismej.2015.32

Source DB:  PubMed          Journal:  ISME J        ISSN: 1751-7362            Impact factor:   10.302


  45 in total

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Journal:  J Nutr Biochem       Date:  2012-03-07       Impact factor: 6.048

2.  Procedures for large-scale metabolic profiling of serum and plasma using gas chromatography and liquid chromatography coupled to mass spectrometry.

Authors:  Warwick B Dunn; David Broadhurst; Paul Begley; Eva Zelena; Sue Francis-McIntyre; Nadine Anderson; Marie Brown; Joshau D Knowles; Antony Halsall; John N Haselden; Andrew W Nicholls; Ian D Wilson; Douglas B Kell; Royston Goodacre
Journal:  Nat Protoc       Date:  2011-06-30       Impact factor: 13.491

3.  Metabolic profiling reveals a contribution of gut microbiota to fatty liver phenotype in insulin-resistant mice.

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5.  Human, rat and chicken small intestinal Na+ - Cl- -creatine transporter: functional, molecular characterization and localization.

Authors:  M J Peral; M García-Delgado; M L Calonge; J M Durán; M C De La Horra; T Wallimann; O Speer; A Ilundáin
Journal:  J Physiol       Date:  2002-11-15       Impact factor: 5.182

6.  Methionine-enkephalin and leucine-enkephalin in human sympathoadrenal system and pheochromocytoma.

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8.  Gut microbiota disturbance during antibiotic therapy: a multi-omic approach.

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Review 9.  Metabolism, physiological role, and clinical implications of sphingolipids in gastrointestinal tract.

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10.  Effects of β-lactam antibiotics and fluoroquinolones on human gut microbiota in relation to Clostridium difficile associated diarrhea.

Authors:  Henrik Knecht; Sven C Neulinger; Femke Anouska Heinsen; Carolin Knecht; Anke Schilhabel; Ruth A Schmitz; Alexandra Zimmermann; Vitor Martins dos Santos; Manuel Ferrer; Philip C Rosenstiel; Stefan Schreiber; Anette K Friedrichs; Stephan J Ott
Journal:  PLoS One       Date:  2014-02-28       Impact factor: 3.240

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  19 in total

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Review 2.  Microbe-microbe interactions during Clostridioides difficile infection.

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Journal:  Curr Opin Microbiol       Date:  2020-02-20       Impact factor: 7.934

3.  Modified Mouse Model of Clostridioides difficile Infection as a Platform for Probiotic Efficacy Studies.

Authors:  T J De Wolfe; A E Kates; L Barko; B J Darien; N Safdar
Journal:  Antimicrob Agents Chemother       Date:  2019-06-24       Impact factor: 5.191

Review 4.  The emerging metabolic view of Clostridium difficile pathogenesis.

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Review 5.  Computational approaches to understanding Clostridioides difficile metabolism and virulence.

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Review 6.  Structural and functional changes within the gut microbiota and susceptibility to Clostridium difficile infection.

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Review 7.  Functional metabolomics: from biomarker discovery to metabolome reprogramming.

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8.  Metabolomics reveals synergy between Ag and g-C3N4 in Ag/g-C3N4 composite photocatalysts: a unique feature among Ag-doped biocidal materials.

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Journal:  Metabolomics       Date:  2021-06-01       Impact factor: 4.290

Review 9.  Colonization Resistance of the Gut Microbiota against Clostridium difficile.

Authors:  Ana Elena Pérez-Cobas; Andrés Moya; María José Gosalbes; Amparo Latorre
Journal:  Antibiotics (Basel)       Date:  2015-08-07

10.  HIV infection results in metabolic alterations in the gut microbiota different from those induced by other diseases.

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