Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction

Torsten P. M. Scheithauer; Hilde Herrema; Hongbing Yu; Guido J. Bakker; Maaike Winkelmeijer; Galina Soukhatcheva; Derek Dai; Caixia Ma; Stefan R. Havik; Manon Balvers; Mark Davids; Abraham S. Meijnikman; Ömrüm Aydin; Bert-Jan H. van den Born; Marc G. Besselink; Olivier R. Busch; Maurits de Brauw; Arnold van de Laar; Clara Belzer; Martin Stahl; Willem M. de Vos; Bruce A. Vallance; Max Nieuwdorp; C. Bruce Verchere; Daniël H. van Raalte

doi:https://doi.org/10.1080/19490976.2022.2111951

Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction

Torsten P. M. Scheithauer, Hilde Herrema, Hongbing Yu, Guido J. Bakker, Maaike Winkelmeijer, Galina Soukhatcheva, Derek Dai, Caixia Ma, Stefan R. Havik, Manon Balvers, Mark Davids, Abraham S. Meijnikman, Ömrüm Aydin, Bert-Jan H. van den Born, Marc G. Besselink, Olivier R. Busch, Maurits de Brauw, Arnold van de Laar, Clara Belzer, Martin StahlWillem M. de Vos, Bruce A. Vallance, Max Nieuwdorp, C. Bruce Verchere, Daniël H. van Raalte

Research output: Contribution to journal › Article › Academic › peer-review

5 Citations (Scopus)

Abstract

Hyperglycemia and type 2 diabetes (T2D) are caused by failure of pancreatic beta cells. The role of the gut microbiota in T2D has been studied, but causal links remain enigmatic. Obese individuals with or without T2D were included from two independent Dutch cohorts. Human data were translated in vitro and in vivo by using pancreatic islets from C57BL6/J mice and by injecting flagellin into obese mice. Flagellin is part of the bacterial locomotor appendage flagellum, present in gut bacteria including Enterobacteriaceae, which we show to be more abundant in the gut of individuals with T2D. Subsequently, flagellin induces a pro-inflammatory response in pancreatic islets mediated by the Toll-like receptor (TLR)-5 expressed on resident islet macrophages. This inflammatory response is associated with beta-cell dysfunction, characterized by reduced insulin gene expression, impaired proinsulin processing and stress-induced insulin hypersecretion in vitro and in vivo in mice. We postulate that increased systemically disseminated flagellin in T2D is a contributing factor to beta-cell failure in time and represents a novel therapeutic target.

Original language	English
Article number	2111951
Journal	Gut Microbes
Volume	14
Issue number	1
DOIs	https://doi.org/10.1080/19490976.2022.2111951
Publication status	Published - 19 Aug 2022

Keywords

Gut microbiota
beta-cell function
flagellin
inflammation
type 2 diabetes

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https://doi.org/10.1080/19490976.2022.2111951

Cite this

Scheithauer, T. P. M., Herrema, H., Yu, H., Bakker, G. J., Winkelmeijer, M., Soukhatcheva, G., Dai, D., Ma, C., Havik, S. R., Balvers, M., Davids, M., Meijnikman, A. S., Aydin, Ö., van den Born, B.-J. H., Besselink, M. G., Busch, O. R., de Brauw, M., van de Laar, A., Belzer, C., ... van Raalte, D. H. (2022). Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction. Gut Microbes, 14(1), Article 2111951. https://doi.org/10.1080/19490976.2022.2111951

@article{3a7c4e8bd7154c4a9c9926f3440f1218,

title = "Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction",

abstract = "Hyperglycemia and type 2 diabetes (T2D) are caused by failure of pancreatic beta cells. The role of the gut microbiota in T2D has been studied, but causal links remain enigmatic. Obese individuals with or without T2D were included from two independent Dutch cohorts. Human data were translated in vitro and in vivo by using pancreatic islets from C57BL6/J mice and by injecting flagellin into obese mice. Flagellin is part of the bacterial locomotor appendage flagellum, present in gut bacteria including Enterobacteriaceae, which we show to be more abundant in the gut of individuals with T2D. Subsequently, flagellin induces a pro-inflammatory response in pancreatic islets mediated by the Toll-like receptor (TLR)-5 expressed on resident islet macrophages. This inflammatory response is associated with beta-cell dysfunction, characterized by reduced insulin gene expression, impaired proinsulin processing and stress-induced insulin hypersecretion in vitro and in vivo in mice. We postulate that increased systemically disseminated flagellin in T2D is a contributing factor to beta-cell failure in time and represents a novel therapeutic target.",

keywords = "Gut microbiota, beta-cell function, flagellin, inflammation, type 2 diabetes",

author = "Scheithauer, {Torsten P. M.} and Hilde Herrema and Hongbing Yu and Bakker, {Guido J.} and Maaike Winkelmeijer and Galina Soukhatcheva and Derek Dai and Caixia Ma and Havik, {Stefan R.} and Manon Balvers and Mark Davids and Meijnikman, {Abraham S.} and {\"O}mr{\"u}m Aydin and {van den Born}, {Bert-Jan H.} and Besselink, {Marc G.} and Busch, {Olivier R.} and {de Brauw}, Maurits and {van de Laar}, Arnold and Clara Belzer and Martin Stahl and {de Vos}, {Willem M.} and Vallance, {Bruce A.} and Max Nieuwdorp and Verchere, {C. Bruce} and {van Raalte}, {Dani{\"e}l H.}",

note = "Funding Information: This study was funded by Diabetes Fonds (Application number: 2015.81) and Marie Sk{\l}odowska-Curie Actions (Call H2020-MSCA-IF-2015). CBV was supported by CIHR project grant PJT-165943. M.N. is supported by a personal ZONMW VICI grant 2020 [09150182010020]. B.A.V. is the Children with Intestinal and Liver Disorders (CH.I.L.D) Foundation Chair in Pediatric Gastroenterology. The HELIUS study is conducted by the Amsterdam University Medical Centers, location AMC and the Public Health Service of Amsterdam. Both organizations provided core support for HELIUS. The HELIUS study is also funded by the Dutch Heart Foundation, the Netherlands Organization for Health Research and Development (ZonMw), the European Union (FP-7), and the European Fund for the Integration of non-EU immigrants (EIF). We are most grateful to the participants of the HELIUS study and the management team, research nurses, interviewers, research assistants and other staff who have taken part in gathering the data of this study. The study reported here was additionally supported by (an) additional grant(s) from Dutch Heart Foundation: 2010T084 (K Stronks), ZonMw: 200500003 (K Stronks), European Union (FP-7): 278901 (K Stronks), European Fund for the Integration of non-EU immigrants (EIF): 2013EIF013 (K Stronks). HH is supported by a Senior Fellowship of the Dutch Diabetes Research Foundation (2019.82.004). Funding Information: This work was supported by the Diabetes Fonds [2019.82.004]; Diabetes Fonds [2015.81]; Marie Sklodowska-Curie [H2020-MSCA-IF-2015]; Netherlands Organisation for Health Research and Development [09150182010020]. This study was funded by Diabetes Fonds (Application number: 2015.81) and Marie Sk{\l}odowska-Curie Actions (Call H2020-MSCA-IF-2015). CBV was supported by CIHR project grant PJT-165943. M.N. is supported by a personal ZONMW VICI grant 2020 [09150182010020]. B.A.V. is the Children with Intestinal and Liver Disorders (CH.I.L.D) Foundation Chair in Pediatric Gastroenterology. The HELIUS study is conducted by the Amsterdam University Medical Centers, location AMC and the Public Health Service of Amsterdam. Both organizations provided core support for HELIUS. The HELIUS study is also funded by the Dutch Heart Foundation, the Netherlands Organization for Health Research and Development (ZonMw), the European Union (FP-7), and the European Fund for the Integration of non-EU immigrants (EIF). We are most grateful to the participants of the HELIUS study and the management team, research nurses, interviewers, research assistants and other staff who have taken part in gathering the data of this study. The study reported here was additionally supported by (an) additional grant(s) from Dutch Heart Foundation: 2010T084 (K Stronks), ZonMw: 200500003 (K Stronks), European Union (FP-7): 278901 (K Stronks), European Fund for the Integration of non-EU immigrants (EIF): 2013EIF013 (K Stronks). HH is supported by a Senior Fellowship of the Dutch Diabetes Research Foundation (2019.82.004). Publisher Copyright: {\textcopyright} 2022 The Author(s). Published with license by Taylor & Francis Group, LLC.",

year = "2022",

month = aug,

day = "19",

doi = "https://doi.org/10.1080/19490976.2022.2111951",

language = "English",

volume = "14",

journal = "Gut Microbes",

issn = "1949-0976",

publisher = "Landes Bioscience",

number = "1",

}

Scheithauer, TPM , Herrema, H, Yu, H, Bakker, GJ, Winkelmeijer, M, Soukhatcheva, G, Dai, D, Ma, C, Havik, SR , Balvers, M , Davids, M , Meijnikman, AS, Aydin, Ö, van den Born, B-JH , Besselink, MG , Busch, OR, de Brauw, M, van de Laar, A, Belzer, C, Stahl, M, de Vos, WM, Vallance, BA, Nieuwdorp, M, Verchere, CB & van Raalte, DH 2022, 'Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction', Gut Microbes, vol. 14, no. 1, 2111951. https://doi.org/10.1080/19490976.2022.2111951

TY - JOUR

T1 - Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction

AU - Scheithauer, Torsten P. M.

AU - Herrema, Hilde

AU - Yu, Hongbing

AU - Bakker, Guido J.

AU - Winkelmeijer, Maaike

AU - Soukhatcheva, Galina

AU - Dai, Derek

AU - Ma, Caixia

AU - Havik, Stefan R.

AU - Balvers, Manon

AU - Davids, Mark

AU - Meijnikman, Abraham S.

AU - Aydin, Ömrüm

AU - van den Born, Bert-Jan H.

AU - Besselink, Marc G.

AU - Busch, Olivier R.

AU - de Brauw, Maurits

AU - van de Laar, Arnold

AU - Belzer, Clara

AU - Stahl, Martin

AU - de Vos, Willem M.

AU - Vallance, Bruce A.

AU - Nieuwdorp, Max

AU - Verchere, C. Bruce

AU - van Raalte, Daniël H.

N1 - Funding Information: This study was funded by Diabetes Fonds (Application number: 2015.81) and Marie Skłodowska-Curie Actions (Call H2020-MSCA-IF-2015). CBV was supported by CIHR project grant PJT-165943. M.N. is supported by a personal ZONMW VICI grant 2020 [09150182010020]. B.A.V. is the Children with Intestinal and Liver Disorders (CH.I.L.D) Foundation Chair in Pediatric Gastroenterology. The HELIUS study is conducted by the Amsterdam University Medical Centers, location AMC and the Public Health Service of Amsterdam. Both organizations provided core support for HELIUS. The HELIUS study is also funded by the Dutch Heart Foundation, the Netherlands Organization for Health Research and Development (ZonMw), the European Union (FP-7), and the European Fund for the Integration of non-EU immigrants (EIF). We are most grateful to the participants of the HELIUS study and the management team, research nurses, interviewers, research assistants and other staff who have taken part in gathering the data of this study. The study reported here was additionally supported by (an) additional grant(s) from Dutch Heart Foundation: 2010T084 (K Stronks), ZonMw: 200500003 (K Stronks), European Union (FP-7): 278901 (K Stronks), European Fund for the Integration of non-EU immigrants (EIF): 2013EIF013 (K Stronks). HH is supported by a Senior Fellowship of the Dutch Diabetes Research Foundation (2019.82.004). Funding Information: This work was supported by the Diabetes Fonds [2019.82.004]; Diabetes Fonds [2015.81]; Marie Sklodowska-Curie [H2020-MSCA-IF-2015]; Netherlands Organisation for Health Research and Development [09150182010020]. This study was funded by Diabetes Fonds (Application number: 2015.81) and Marie Skłodowska-Curie Actions (Call H2020-MSCA-IF-2015). CBV was supported by CIHR project grant PJT-165943. M.N. is supported by a personal ZONMW VICI grant 2020 [09150182010020]. B.A.V. is the Children with Intestinal and Liver Disorders (CH.I.L.D) Foundation Chair in Pediatric Gastroenterology. The HELIUS study is conducted by the Amsterdam University Medical Centers, location AMC and the Public Health Service of Amsterdam. Both organizations provided core support for HELIUS. The HELIUS study is also funded by the Dutch Heart Foundation, the Netherlands Organization for Health Research and Development (ZonMw), the European Union (FP-7), and the European Fund for the Integration of non-EU immigrants (EIF). We are most grateful to the participants of the HELIUS study and the management team, research nurses, interviewers, research assistants and other staff who have taken part in gathering the data of this study. The study reported here was additionally supported by (an) additional grant(s) from Dutch Heart Foundation: 2010T084 (K Stronks), ZonMw: 200500003 (K Stronks), European Union (FP-7): 278901 (K Stronks), European Fund for the Integration of non-EU immigrants (EIF): 2013EIF013 (K Stronks). HH is supported by a Senior Fellowship of the Dutch Diabetes Research Foundation (2019.82.004). Publisher Copyright: © 2022 The Author(s). Published with license by Taylor & Francis Group, LLC.

PY - 2022/8/19

Y1 - 2022/8/19

N2 - Hyperglycemia and type 2 diabetes (T2D) are caused by failure of pancreatic beta cells. The role of the gut microbiota in T2D has been studied, but causal links remain enigmatic. Obese individuals with or without T2D were included from two independent Dutch cohorts. Human data were translated in vitro and in vivo by using pancreatic islets from C57BL6/J mice and by injecting flagellin into obese mice. Flagellin is part of the bacterial locomotor appendage flagellum, present in gut bacteria including Enterobacteriaceae, which we show to be more abundant in the gut of individuals with T2D. Subsequently, flagellin induces a pro-inflammatory response in pancreatic islets mediated by the Toll-like receptor (TLR)-5 expressed on resident islet macrophages. This inflammatory response is associated with beta-cell dysfunction, characterized by reduced insulin gene expression, impaired proinsulin processing and stress-induced insulin hypersecretion in vitro and in vivo in mice. We postulate that increased systemically disseminated flagellin in T2D is a contributing factor to beta-cell failure in time and represents a novel therapeutic target.

AB - Hyperglycemia and type 2 diabetes (T2D) are caused by failure of pancreatic beta cells. The role of the gut microbiota in T2D has been studied, but causal links remain enigmatic. Obese individuals with or without T2D were included from two independent Dutch cohorts. Human data were translated in vitro and in vivo by using pancreatic islets from C57BL6/J mice and by injecting flagellin into obese mice. Flagellin is part of the bacterial locomotor appendage flagellum, present in gut bacteria including Enterobacteriaceae, which we show to be more abundant in the gut of individuals with T2D. Subsequently, flagellin induces a pro-inflammatory response in pancreatic islets mediated by the Toll-like receptor (TLR)-5 expressed on resident islet macrophages. This inflammatory response is associated with beta-cell dysfunction, characterized by reduced insulin gene expression, impaired proinsulin processing and stress-induced insulin hypersecretion in vitro and in vivo in mice. We postulate that increased systemically disseminated flagellin in T2D is a contributing factor to beta-cell failure in time and represents a novel therapeutic target.

KW - Gut microbiota

KW - beta-cell function

KW - flagellin

KW - inflammation

KW - type 2 diabetes

UR - http://www.scopus.com/inward/record.url?scp=85136514020&partnerID=8YFLogxK

U2 - https://doi.org/10.1080/19490976.2022.2111951

DO - https://doi.org/10.1080/19490976.2022.2111951

M3 - Article

C2 - 35984746

SN - 1949-0976

VL - 14

JO - Gut Microbes

JF - Gut Microbes

IS - 1

M1 - 2111951

ER -

Gut-derived bacterial flagellin induces beta-cell inflammation and dysfunction

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Keywords

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