Systemic antibody responses against gut microbiota flagellins implicate shared and divergent immune reactivity in Crohn’s disease and chronic fatigue syndrome

Arno R. Bourgonje; Nicolai V. Hörstke; Michaela Fehringer; Gabriel Innocenti; Thomas Vogl

doi:10.1186/s40168-024-01858-1

Microbiome (Jul 2024)

Systemic antibody responses against gut microbiota flagellins implicate shared and divergent immune reactivity in Crohn’s disease and chronic fatigue syndrome

Arno R. Bourgonje,
Nicolai V. Hörstke,
Michaela Fehringer,
Gabriel Innocenti,
Thomas Vogl

Affiliations

Arno R. Bourgonje: The Henry D. Janowitz Division of Gastroenterology, Department of Medicine, Icahn School of Medicine at Mount Sinai
Nicolai V. Hörstke: Center for Cancer Research, Medical University of Vienna
Michaela Fehringer: Center for Cancer Research, Medical University of Vienna
Gabriel Innocenti: Center for Cancer Research, Medical University of Vienna
Thomas Vogl: Center for Cancer Research, Medical University of Vienna

DOI: https://doi.org/10.1186/s40168-024-01858-1
Journal volume & issue: Vol. 12, no. 1
pp. 1 – 17

Abstract

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Abstract Background Elevated systemic antibody responses against gut microbiota flagellins are observed in both Crohn’s disease (CD) and myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS), suggesting potential serological biomarkers for diagnosis. However, flagellin-specific antibody repertoires and functional roles in the diseases remain incompletely understood. Bacterial flagellins can be categorized into three types depending on their interaction with toll-like receptor 5 (TLR5): (1) “stimulator” and (2) “silent” flagellins, which bind TLR5 through a conserved N-terminal motif, with only stimulators activating TLR5 (involving a C-terminal domain); (3) “evader” flagellins of pathogens, which entirely circumvent TLR5 activation via mutations in the N-terminal TLR5 binding motif. Results Here, we show that both CD and ME/CFS patients exhibit elevated antibody responses against distinct regions of flagellins compared to healthy individuals. N-terminal binding to Lachnospiraceae flagellins was comparable in both diseases, while C-terminal binding was more prevalent in CD. N-terminal antibody-bound flagellin sequences were similar across CD and ME/CFS, resembling “stimulator” and “silent” flagellins more than evaders. However, C-terminal antibody-bound flagellins showed a higher resemblance to the stimulator than to silent flagellins in CD, which was not observed in ME/CFS. Conclusions These findings suggest that antibody binding to the N-terminal domain of stimulator and silent flagellins may impact TLR5 activation in both CD and ME/CFS patients. Blocking this interaction could lead commensal bacteria to be recognized as pathogenic evaders, potentially contributing to dysregulation in both diseases. Furthermore, elevated antibody binding to the C-terminal domain of stimulator flagellins in CD may explain pathophysiological differences between the diseases. Overall, these results highlight the diagnostic potential of these antibody responses and lay a foundation for deeper mechanistic studies of flagellin/TLR5 interactions and their impact on innate/adaptive immunity balance. Graphical Abstract Video Abstract

Published in Microbiome

ISSN: 2049-2618 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Microbiology: Microbial ecology
Website: https://microbiomejournal.biomedcentral.com

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