The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients

Carlos G. Gonzalez; Robert H. Mills; Melissa C. Kordahi; Marvic Carrillo-Terrazas; Henry Secaira-Morocho; Christella E. Widjaja; Matthew S. Tsai; Yash Mittal; Brian A. Yee; Fernando Vargas; Kelly Weldon; Julia M. Gauglitz; Clara Delaroque; Consuelo Sauceda; Leigh Ana Rossitto; Gail Ackermann; Gregory Humphrey; Austin D. Swafford; Corey A. Siegel; Jay C. Buckey; Laura E. Raffals; Charlotte Sadler; Peter Lindholm; Kathleen M. Fisch; Mark Valaseck; Arief Suriawinata; Gene W. Yeo; Pradipta Ghosh; John T. Chang; Hiutung Chu; Pieter Dorrestein; Qiyun Zhu; Benoit Chassaing; Rob Knight; David J. Gonzalez; Parambir S. Dulai

doi:10.1016/j.jcmgh.2022.03.008

The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients

Carlos G. Gonzalez, Robert H. Mills, Melissa C. Kordahi, Marvic Carrillo-Terrazas, Henry Secaira-Morocho, Christella E. Widjaja, Matthew S. Tsai, Yash Mittal, Brian A. Yee, Fernando Vargas, Kelly Weldon, Julia M. Gauglitz, Clara Delaroque, Consuelo Sauceda, Leigh Ana Rossitto, Gail Ackermann, Gregory Humphrey, Austin D. Swafford, Corey A. Siegel, Jay C. BuckeyLaura E. Raffals, Charlotte Sadler, Peter Lindholm, Kathleen M. Fisch, Mark Valaseck, Arief Suriawinata, Gene W. Yeo, Pradipta Ghosh, John T. Chang, Hiutung Chu, Pieter Dorrestein, Qiyun Zhu, Benoit Chassaing, Rob Knight, David J. Gonzalez, Parambir S. Dulai

Life Sciences, School of (SOLS)

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

4 Scopus citations

Abstract

Background & Aims: Hyperbaric oxygen therapy (HBOT) is a promising treatment for moderate-to-severe ulcerative colitis. However, our current understanding of the host and microbial response to HBOT remains unclear. This study examined the molecular mechanisms underpinning HBOT using a multi-omic strategy. Methods: Pre- and post-intervention mucosal biopsies, tissue, and fecal samples were collected from HBOT phase 2 clinical trials. Biopsies and fecal samples were subjected to shotgun metaproteomics, metabolomics, 16s rRNA sequencing, and metagenomics. Tissue was subjected to bulk RNA sequencing and digital spatial profiling (DSP) for single-cell RNA and protein analysis, and immunohistochemistry was performed. Fecal samples were also used for colonization experiments in IL10^-/- germ-free UC mouse models. Results: Proteomics identified negative associations between HBOT response and neutrophil azurophilic granule abundance. DSP identified an HBOT-specific reduction of neutrophil STAT3, which was confirmed by immunohistochemistry. HBOT decreased microbial diversity with a proportional increase in Firmicutes and a secondary bile acid lithocholic acid. A major source of the reduction in diversity was the loss of mucus-adherent taxa, resulting in increased MUC2 levels post-HBOT. Targeted database searching revealed strain-level associations between Akkermansia muciniphila and HBOT response status. Colonization of IL10^-/- with stool obtained from HBOT responders resulted in lower colitis activity compared with non-responders, with no differences in STAT3 expression, suggesting complementary but independent host and microbial responses. Conclusions: HBOT reduces host neutrophil STAT3 and azurophilic granule activity in UC patients and changes in microbial composition and metabolism in ways that improve colitis activity. Intestinal microbiota, especially strain level variations in A muciniphila, may contribute to HBOT non-response.

Original language	English (US)
Pages (from-to)	35-53
Number of pages	19
Journal	CMGH
Volume	14
Issue number	1
DOIs	https://doi.org/10.1016/j.jcmgh.2022.03.008
State	Published - Jan 2022

ASJC Scopus subject areas

Hepatology
Gastroenterology

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10.1016/j.jcmgh.2022.03.008

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Gonzalez, C. G., Mills, R. H., Kordahi, M. C., Carrillo-Terrazas, M., Secaira-Morocho, H., Widjaja, C. E., Tsai, M. S., Mittal, Y., Yee, B. A., Vargas, F., Weldon, K., Gauglitz, J. M., Delaroque, C., Sauceda, C., Rossitto, L. A., Ackermann, G., Humphrey, G., Swafford, A. D., Siegel, C. A., ... Dulai, P. S. (2022). The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients. CMGH, 14(1), 35-53. https://doi.org/10.1016/j.jcmgh.2022.03.008

Gonzalez, CG, Mills, RH, Kordahi, MC, Carrillo-Terrazas, M, Secaira-Morocho, H, Widjaja, CE, Tsai, MS, Mittal, Y, Yee, BA, Vargas, F, Weldon, K, Gauglitz, JM, Delaroque, C, Sauceda, C, Rossitto, LA, Ackermann, G, Humphrey, G, Swafford, AD, Siegel, CA, Buckey, JC, Raffals, LE, Sadler, C, Lindholm, P, Fisch, KM, Valaseck, M, Suriawinata, A, Yeo, GW, Ghosh, P, Chang, JT, Chu, H, Dorrestein, P, Zhu, Q, Chassaing, B, Knight, R, Gonzalez, DJ & Dulai, PS 2022, 'The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients', CMGH, vol. 14, no. 1, pp. 35-53. https://doi.org/10.1016/j.jcmgh.2022.03.008

@article{8e8429a850c54234ac0fb7ede117ed8a,

title = "The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients",

abstract = "Background & Aims: Hyperbaric oxygen therapy (HBOT) is a promising treatment for moderate-to-severe ulcerative colitis. However, our current understanding of the host and microbial response to HBOT remains unclear. This study examined the molecular mechanisms underpinning HBOT using a multi-omic strategy. Methods: Pre- and post-intervention mucosal biopsies, tissue, and fecal samples were collected from HBOT phase 2 clinical trials. Biopsies and fecal samples were subjected to shotgun metaproteomics, metabolomics, 16s rRNA sequencing, and metagenomics. Tissue was subjected to bulk RNA sequencing and digital spatial profiling (DSP) for single-cell RNA and protein analysis, and immunohistochemistry was performed. Fecal samples were also used for colonization experiments in IL10-/- germ-free UC mouse models. Results: Proteomics identified negative associations between HBOT response and neutrophil azurophilic granule abundance. DSP identified an HBOT-specific reduction of neutrophil STAT3, which was confirmed by immunohistochemistry. HBOT decreased microbial diversity with a proportional increase in Firmicutes and a secondary bile acid lithocholic acid. A major source of the reduction in diversity was the loss of mucus-adherent taxa, resulting in increased MUC2 levels post-HBOT. Targeted database searching revealed strain-level associations between Akkermansia muciniphila and HBOT response status. Colonization of IL10-/- with stool obtained from HBOT responders resulted in lower colitis activity compared with non-responders, with no differences in STAT3 expression, suggesting complementary but independent host and microbial responses. Conclusions: HBOT reduces host neutrophil STAT3 and azurophilic granule activity in UC patients and changes in microbial composition and metabolism in ways that improve colitis activity. Intestinal microbiota, especially strain level variations in A muciniphila, may contribute to HBOT non-response.",

author = "Gonzalez, {Carlos G.} and Mills, {Robert H.} and Kordahi, {Melissa C.} and Marvic Carrillo-Terrazas and Henry Secaira-Morocho and Widjaja, {Christella E.} and Tsai, {Matthew S.} and Yash Mittal and Yee, {Brian A.} and Fernando Vargas and Kelly Weldon and Gauglitz, {Julia M.} and Clara Delaroque and Consuelo Sauceda and Rossitto, {Leigh Ana} and Gail Ackermann and Gregory Humphrey and Swafford, {Austin D.} and Siegel, {Corey A.} and Buckey, {Jay C.} and Raffals, {Laura E.} and Charlotte Sadler and Peter Lindholm and Fisch, {Kathleen M.} and Mark Valaseck and Arief Suriawinata and Yeo, {Gene W.} and Pradipta Ghosh and Chang, {John T.} and Hiutung Chu and Pieter Dorrestein and Qiyun Zhu and Benoit Chassaing and Rob Knight and Gonzalez, {David J.} and Dulai, {Parambir S.}",

note = "Funding Information: Funding This work was directly supported by an American Gastroenterology Association Research Scholar Award and NIDDK U34 Planning Grant (DK126626) to Parambir S. Dulai. This work was also supported by the Crohn's and Colitis Foundation through a Litwin IBD Pioneers Program Grant, the UCSD Collaborative Center for Multiplexed Proteomics, the San Diego Digestive Disease Center (P30 DK120515), UCSD Gastroenterology T32 training grant (DK 0070202; P.S.D., M.T., R.H.M, C.S., and Y.M.), and UCSD Graduate Training Program in Cellular and Molecular Pharmacology (T32 GM007752; L.R.). Y.M. was also supported by an NIH CTSA-funded career-development award (1TL1TR001443). P.G. is supported by the NIH (UG3TR003355, AI155696, and AI141630). J.T.C. is supported by the NIH (AI123202, AI129973, AI132122, and DK119724). C.G.G. is funded by Institutional Research and Academic Career Development Awards (K12GM068524). C.S. is supported by NIH Training grant (T32, DK007202). K.F. is supported by the NIH (2UL1TR001442-06). B.C. is supported by a Starting Grant from the European Research Council (ERC) under the European Union{\textquoteright}s Horizon 2020 research and innovation program (grant agreement no. ERC-2018-StG- 804135), a Chaire d{\textquoteright}Excellence from IdEx Universit{\'e} de Paris - ANR-18-IDEX-0001, an Innovator Award from the Kenneth Rainin Foundation, an ANR grant EMULBIONT ANR-21-CE15-0042-01, and the national program “Microbiote” from INSERM. P.C.D. is supported by the Crohn's and Colitis Foundation (grant #675191). Funding Information: Funding This work was directly supported by an American Gastroenterology Association Research Scholar Award and NIDDK U34 Planning Grant (DK126626) to Parambir S. Dulai. This work was also supported by the Crohn's and Colitis Foundation through a Litwin IBD Pioneers Program Grant, the UCSD Collaborative Center for Multiplexed Proteomics, the San Diego Digestive Disease Center (P30 DK120515), UCSD Gastroenterology T32 training grant (DK 0070202; P.S.D., M.T., R.H.M, C.S., and Y.M.), and UCSD Graduate Training Program in Cellular and Molecular Pharmacology (T32 GM007752; L.R.). Y.M. was also supported by an NIH CTSA-funded career-development award (1TL1TR001443). P.G. is supported by the NIH (UG3TR003355, AI155696, and AI141630). J.T.C. is supported by the NIH (AI123202, AI129973, AI132122, and DK119724). C.G.G. is funded by Institutional Research and Academic Career Development Awards (K12GM068524). C.S. is supported by NIH Training grant (T32, DK007202). K.F. is supported by the NIH (2UL1TR001442-06). B.C. is supported by a Starting Grant from the European Research Council (ERC) under the European Union's Horizon 2020 research and innovation program (grant agreement no. ERC-2018-StG- 804135), a Chaire d'Excellence from IdEx Universit{\'e} de Paris - ANR-18-IDEX-0001, an Innovator Award from the Kenneth Rainin Foundation, an ANR grant EMULBIONT ANR-21-CE15-0042-01, and the national program “Microbiote” from INSERM. P.C.D. is supported by the Crohn's and Colitis Foundation (grant #675191). Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2022",

month = jan,

doi = "10.1016/j.jcmgh.2022.03.008",

language = "English (US)",

volume = "14",

pages = "35--53",

journal = "CMGH",

issn = "2352-345X",

publisher = "Elsevier Inc.",

number = "1",

}

TY - JOUR

T1 - The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients

AU - Gonzalez, Carlos G.

AU - Mills, Robert H.

AU - Kordahi, Melissa C.

AU - Carrillo-Terrazas, Marvic

AU - Secaira-Morocho, Henry

AU - Widjaja, Christella E.

AU - Tsai, Matthew S.

AU - Mittal, Yash

AU - Yee, Brian A.

AU - Vargas, Fernando

AU - Weldon, Kelly

AU - Gauglitz, Julia M.

AU - Delaroque, Clara

AU - Sauceda, Consuelo

AU - Rossitto, Leigh Ana

AU - Ackermann, Gail

AU - Humphrey, Gregory

AU - Swafford, Austin D.

AU - Siegel, Corey A.

AU - Buckey, Jay C.

AU - Raffals, Laura E.

AU - Sadler, Charlotte

AU - Lindholm, Peter

AU - Fisch, Kathleen M.

AU - Valaseck, Mark

AU - Suriawinata, Arief

AU - Yeo, Gene W.

AU - Ghosh, Pradipta

AU - Chang, John T.

AU - Chu, Hiutung

AU - Dorrestein, Pieter

AU - Zhu, Qiyun

AU - Chassaing, Benoit

AU - Knight, Rob

AU - Gonzalez, David J.

AU - Dulai, Parambir S.

N1 - Funding Information: Funding This work was directly supported by an American Gastroenterology Association Research Scholar Award and NIDDK U34 Planning Grant (DK126626) to Parambir S. Dulai. This work was also supported by the Crohn's and Colitis Foundation through a Litwin IBD Pioneers Program Grant, the UCSD Collaborative Center for Multiplexed Proteomics, the San Diego Digestive Disease Center (P30 DK120515), UCSD Gastroenterology T32 training grant (DK 0070202; P.S.D., M.T., R.H.M, C.S., and Y.M.), and UCSD Graduate Training Program in Cellular and Molecular Pharmacology (T32 GM007752; L.R.). Y.M. was also supported by an NIH CTSA-funded career-development award (1TL1TR001443). P.G. is supported by the NIH (UG3TR003355, AI155696, and AI141630). J.T.C. is supported by the NIH (AI123202, AI129973, AI132122, and DK119724). C.G.G. is funded by Institutional Research and Academic Career Development Awards (K12GM068524). C.S. is supported by NIH Training grant (T32, DK007202). K.F. is supported by the NIH (2UL1TR001442-06). B.C. is supported by a Starting Grant from the European Research Council (ERC) under the European Union’s Horizon 2020 research and innovation program (grant agreement no. ERC-2018-StG- 804135), a Chaire d’Excellence from IdEx Université de Paris - ANR-18-IDEX-0001, an Innovator Award from the Kenneth Rainin Foundation, an ANR grant EMULBIONT ANR-21-CE15-0042-01, and the national program “Microbiote” from INSERM. P.C.D. is supported by the Crohn's and Colitis Foundation (grant #675191). Funding Information: Funding This work was directly supported by an American Gastroenterology Association Research Scholar Award and NIDDK U34 Planning Grant (DK126626) to Parambir S. Dulai. This work was also supported by the Crohn's and Colitis Foundation through a Litwin IBD Pioneers Program Grant, the UCSD Collaborative Center for Multiplexed Proteomics, the San Diego Digestive Disease Center (P30 DK120515), UCSD Gastroenterology T32 training grant (DK 0070202; P.S.D., M.T., R.H.M, C.S., and Y.M.), and UCSD Graduate Training Program in Cellular and Molecular Pharmacology (T32 GM007752; L.R.). Y.M. was also supported by an NIH CTSA-funded career-development award (1TL1TR001443). P.G. is supported by the NIH (UG3TR003355, AI155696, and AI141630). J.T.C. is supported by the NIH (AI123202, AI129973, AI132122, and DK119724). C.G.G. is funded by Institutional Research and Academic Career Development Awards (K12GM068524). C.S. is supported by NIH Training grant (T32, DK007202). K.F. is supported by the NIH (2UL1TR001442-06). B.C. is supported by a Starting Grant from the European Research Council (ERC) under the European Union's Horizon 2020 research and innovation program (grant agreement no. ERC-2018-StG- 804135), a Chaire d'Excellence from IdEx Université de Paris - ANR-18-IDEX-0001, an Innovator Award from the Kenneth Rainin Foundation, an ANR grant EMULBIONT ANR-21-CE15-0042-01, and the national program “Microbiote” from INSERM. P.C.D. is supported by the Crohn's and Colitis Foundation (grant #675191). Publisher Copyright: © 2022 The Authors

PY - 2022/1

Y1 - 2022/1

N2 - Background & Aims: Hyperbaric oxygen therapy (HBOT) is a promising treatment for moderate-to-severe ulcerative colitis. However, our current understanding of the host and microbial response to HBOT remains unclear. This study examined the molecular mechanisms underpinning HBOT using a multi-omic strategy. Methods: Pre- and post-intervention mucosal biopsies, tissue, and fecal samples were collected from HBOT phase 2 clinical trials. Biopsies and fecal samples were subjected to shotgun metaproteomics, metabolomics, 16s rRNA sequencing, and metagenomics. Tissue was subjected to bulk RNA sequencing and digital spatial profiling (DSP) for single-cell RNA and protein analysis, and immunohistochemistry was performed. Fecal samples were also used for colonization experiments in IL10-/- germ-free UC mouse models. Results: Proteomics identified negative associations between HBOT response and neutrophil azurophilic granule abundance. DSP identified an HBOT-specific reduction of neutrophil STAT3, which was confirmed by immunohistochemistry. HBOT decreased microbial diversity with a proportional increase in Firmicutes and a secondary bile acid lithocholic acid. A major source of the reduction in diversity was the loss of mucus-adherent taxa, resulting in increased MUC2 levels post-HBOT. Targeted database searching revealed strain-level associations between Akkermansia muciniphila and HBOT response status. Colonization of IL10-/- with stool obtained from HBOT responders resulted in lower colitis activity compared with non-responders, with no differences in STAT3 expression, suggesting complementary but independent host and microbial responses. Conclusions: HBOT reduces host neutrophil STAT3 and azurophilic granule activity in UC patients and changes in microbial composition and metabolism in ways that improve colitis activity. Intestinal microbiota, especially strain level variations in A muciniphila, may contribute to HBOT non-response.

AB - Background & Aims: Hyperbaric oxygen therapy (HBOT) is a promising treatment for moderate-to-severe ulcerative colitis. However, our current understanding of the host and microbial response to HBOT remains unclear. This study examined the molecular mechanisms underpinning HBOT using a multi-omic strategy. Methods: Pre- and post-intervention mucosal biopsies, tissue, and fecal samples were collected from HBOT phase 2 clinical trials. Biopsies and fecal samples were subjected to shotgun metaproteomics, metabolomics, 16s rRNA sequencing, and metagenomics. Tissue was subjected to bulk RNA sequencing and digital spatial profiling (DSP) for single-cell RNA and protein analysis, and immunohistochemistry was performed. Fecal samples were also used for colonization experiments in IL10-/- germ-free UC mouse models. Results: Proteomics identified negative associations between HBOT response and neutrophil azurophilic granule abundance. DSP identified an HBOT-specific reduction of neutrophil STAT3, which was confirmed by immunohistochemistry. HBOT decreased microbial diversity with a proportional increase in Firmicutes and a secondary bile acid lithocholic acid. A major source of the reduction in diversity was the loss of mucus-adherent taxa, resulting in increased MUC2 levels post-HBOT. Targeted database searching revealed strain-level associations between Akkermansia muciniphila and HBOT response status. Colonization of IL10-/- with stool obtained from HBOT responders resulted in lower colitis activity compared with non-responders, with no differences in STAT3 expression, suggesting complementary but independent host and microbial responses. Conclusions: HBOT reduces host neutrophil STAT3 and azurophilic granule activity in UC patients and changes in microbial composition and metabolism in ways that improve colitis activity. Intestinal microbiota, especially strain level variations in A muciniphila, may contribute to HBOT non-response.

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DO - 10.1016/j.jcmgh.2022.03.008

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The Host-Microbiome Response to Hyperbaric Oxygen Therapy in Ulcerative Colitis Patients

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