Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome

BACKGROUND: Gut‐brain axis is widely implicated in the pathophysiology of Parkinson's disease (PD). We take an integrated approach to considering the gut as a target for disease‐modifying intervention, using continuous measurements of disease facets irrespective of diagnostic divide. METHODS: W...

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Autores principales: Augustin, Aisha, Guennec, Adrien Le, Umamahesan, Chianna, Kendler‐Rhodes, Aidan, Tucker, Rosalind M., Chekmeneva, Elena, Takis, Panteleimon, Lewis, Matthew, Balasubramanian, Karthik, DeSouza, Neville, Mullish, Benjamin H, Taylor, David, Ryan, Suzanne, Whelan, Kevin, Ma, Yun, Ibrahim, Mohammad A. A., Bjarnason, Ingvar, Hayee, Bu’ Hussain, Charlett, André, Dobbs, Sylvia M., Dobbs, R. John, Weller, Clive
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9806009/
https://www.ncbi.nlm.nih.gov/pubmed/36588088
http://dx.doi.org/10.1002/ctm2.1152
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author Augustin, Aisha
Guennec, Adrien Le
Umamahesan, Chianna
Kendler‐Rhodes, Aidan
Tucker, Rosalind M.
Chekmeneva, Elena
Takis, Panteleimon
Lewis, Matthew
Balasubramanian, Karthik
DeSouza, Neville
Mullish, Benjamin H
Taylor, David
Ryan, Suzanne
Whelan, Kevin
Ma, Yun
Ibrahim, Mohammad A. A.
Bjarnason, Ingvar
Hayee, Bu’ Hussain
Charlett, André
Dobbs, Sylvia M.
Dobbs, R. John
Weller, Clive
author_facet Augustin, Aisha
Guennec, Adrien Le
Umamahesan, Chianna
Kendler‐Rhodes, Aidan
Tucker, Rosalind M.
Chekmeneva, Elena
Takis, Panteleimon
Lewis, Matthew
Balasubramanian, Karthik
DeSouza, Neville
Mullish, Benjamin H
Taylor, David
Ryan, Suzanne
Whelan, Kevin
Ma, Yun
Ibrahim, Mohammad A. A.
Bjarnason, Ingvar
Hayee, Bu’ Hussain
Charlett, André
Dobbs, Sylvia M.
Dobbs, R. John
Weller, Clive
author_sort Augustin, Aisha
collection PubMed
description BACKGROUND: Gut‐brain axis is widely implicated in the pathophysiology of Parkinson's disease (PD). We take an integrated approach to considering the gut as a target for disease‐modifying intervention, using continuous measurements of disease facets irrespective of diagnostic divide. METHODS: We characterised 77 participants with diagnosed‐PD, 113 without, by dietary/exogenous substance intake, faecal metabolome, intestinal inflammation, serum cytokines/chemokines, clinical phenotype including colonic transit time. Complete‐linkage hierarchical cluster analysis of metabolites discriminant for PD‐status was performed. RESULTS: Longer colonic transit was linked to deficits in faecal short‐chain‐fatty acids outside PD, to a ‘tryptophan‐containing metabolite cluster’ overall. Phenotypic cluster analysis aggregated colonic transit with brady/hypokinesia, tremor, sleep disorder and dysosmia, each individually associated with tryptophan‐cluster deficit. Overall, a faster pulse was associated with deficits in a metabolite cluster including benzoic acid and an imidazole‐ring compound (anti‐fungals) and vitamin B3 (anti‐inflammatory) and with higher serum CCL20 (chemotactic for lymphocytes/dendritic cells towards mucosal epithelium). The faster pulse in PD was irrespective of postural hypotension. The benzoic acid‐cluster deficit was linked to (well‐recognised) lower caffeine and alcohol intakes, tryptophan‐cluster deficit to higher maltose intake. Free‐sugar intake was increased in PD, maltose intake being 63% higher (p = .001). Faecal calprotectin was 44% (95% CI 5%, 98%) greater in PD [p = .001, adjusted for proton‐pump inhibitors (p = .001)], with 16% of PD‐probands exceeding a cut‐point for clinically significant inflammation compatible with inflammatory bowel disease. Higher maltose intake was associated with exceeding this calprotectin cut‐point. CONCLUSIONS: Emerging picture is of (i) clinical phenotype being described by deficits in microbial metabolites essential to gut health; (ii) intestinal inflammation; (iii) a systemic inflammatory response syndrome.
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spelling pubmed-98060092023-01-04 Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome Augustin, Aisha Guennec, Adrien Le Umamahesan, Chianna Kendler‐Rhodes, Aidan Tucker, Rosalind M. Chekmeneva, Elena Takis, Panteleimon Lewis, Matthew Balasubramanian, Karthik DeSouza, Neville Mullish, Benjamin H Taylor, David Ryan, Suzanne Whelan, Kevin Ma, Yun Ibrahim, Mohammad A. A. Bjarnason, Ingvar Hayee, Bu’ Hussain Charlett, André Dobbs, Sylvia M. Dobbs, R. John Weller, Clive Clin Transl Med Research Articles BACKGROUND: Gut‐brain axis is widely implicated in the pathophysiology of Parkinson's disease (PD). We take an integrated approach to considering the gut as a target for disease‐modifying intervention, using continuous measurements of disease facets irrespective of diagnostic divide. METHODS: We characterised 77 participants with diagnosed‐PD, 113 without, by dietary/exogenous substance intake, faecal metabolome, intestinal inflammation, serum cytokines/chemokines, clinical phenotype including colonic transit time. Complete‐linkage hierarchical cluster analysis of metabolites discriminant for PD‐status was performed. RESULTS: Longer colonic transit was linked to deficits in faecal short‐chain‐fatty acids outside PD, to a ‘tryptophan‐containing metabolite cluster’ overall. Phenotypic cluster analysis aggregated colonic transit with brady/hypokinesia, tremor, sleep disorder and dysosmia, each individually associated with tryptophan‐cluster deficit. Overall, a faster pulse was associated with deficits in a metabolite cluster including benzoic acid and an imidazole‐ring compound (anti‐fungals) and vitamin B3 (anti‐inflammatory) and with higher serum CCL20 (chemotactic for lymphocytes/dendritic cells towards mucosal epithelium). The faster pulse in PD was irrespective of postural hypotension. The benzoic acid‐cluster deficit was linked to (well‐recognised) lower caffeine and alcohol intakes, tryptophan‐cluster deficit to higher maltose intake. Free‐sugar intake was increased in PD, maltose intake being 63% higher (p = .001). Faecal calprotectin was 44% (95% CI 5%, 98%) greater in PD [p = .001, adjusted for proton‐pump inhibitors (p = .001)], with 16% of PD‐probands exceeding a cut‐point for clinically significant inflammation compatible with inflammatory bowel disease. Higher maltose intake was associated with exceeding this calprotectin cut‐point. CONCLUSIONS: Emerging picture is of (i) clinical phenotype being described by deficits in microbial metabolites essential to gut health; (ii) intestinal inflammation; (iii) a systemic inflammatory response syndrome. John Wiley and Sons Inc. 2023-01-01 /pmc/articles/PMC9806009/ /pubmed/36588088 http://dx.doi.org/10.1002/ctm2.1152 Text en © 2022 The Authors. Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Augustin, Aisha
Guennec, Adrien Le
Umamahesan, Chianna
Kendler‐Rhodes, Aidan
Tucker, Rosalind M.
Chekmeneva, Elena
Takis, Panteleimon
Lewis, Matthew
Balasubramanian, Karthik
DeSouza, Neville
Mullish, Benjamin H
Taylor, David
Ryan, Suzanne
Whelan, Kevin
Ma, Yun
Ibrahim, Mohammad A. A.
Bjarnason, Ingvar
Hayee, Bu’ Hussain
Charlett, André
Dobbs, Sylvia M.
Dobbs, R. John
Weller, Clive
Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title_full Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title_fullStr Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title_full_unstemmed Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title_short Faecal metabolite deficit, gut inflammation and diet in Parkinson's disease: Integrative analysis indicates inflammatory response syndrome
title_sort faecal metabolite deficit, gut inflammation and diet in parkinson's disease: integrative analysis indicates inflammatory response syndrome
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9806009/
https://www.ncbi.nlm.nih.gov/pubmed/36588088
http://dx.doi.org/10.1002/ctm2.1152
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