The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner

Margaret M. Harnett; James Doonan; Anuradha Tarafdar; Miguel A. Pineda; Josephine Duncombe-Moore; Geraldine Buitrago; Piaopiao Pan; Paul A. Hoskisson; Colin Selman; William Harnett

doi:10.3389/fitd.2023.1334705

The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner

Margaret M. Harnett
, James Doonan
, Anuradha Tarafdar
, Miguel A. Pineda
, Josephine Duncombe-Moore
, Geraldine Buitrago
, Piaopiao Pan
, Paul A. Hoskisson
, Colin Selman
, William Harnett

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

3 Citations (Scopus)

Abstract

The parasitic worm-derived immunomodulator, ES-62 rescues defective levels of IL-10-producing regulatory B cells (Bregs) and suppresses chronic Th1/Th17-driven inflammation to protect against joint destruction in the mouse collagen-induced arthritis (CIA) model of rheumatoid arthritis. Such autoimmune arthritis is also associated with dysbiosis of the gut microbiota and disruption of intestinal barrier integrity. We recently further exploited the CIA model to show that ES-62’s prevention of joint destruction is associated with protection of intestinal barrier integrity and normalization of the gut microbiota, thereby suppressing the gut pathology that precedes the onset of autoimmunity and joint damage in CIA-mice. As the status of the gut microbiota impacts on immune responses by influencing haematopoiesis, we have therefore investigated whether ES-62 harnesses the homeostatic mechanisms regulating this gut-bone marrow (BM) axis to resolve the chronic inflammation promoting autoimmunity and joint destruction in CIA. Reflecting this, ES-62 was found to counteract the BM myeloid/lymphoid bias typically associated with chronic inflammation and infection. This was achieved primarily by ES-62 acting to maintain the levels of lymphoid lineages (B220⁺ and CD3⁺ cells) observed in naïve, healthy mice but lost from the BM of CIA-mice. Moreover, ES-62’s ability to prevent bone-destroying osteoclastogenesis was found to be associated with its suppression of CIA-induced upregulation of osteoclast progenitors (OCPs) in the BM. Critically, and supporting ES-62’s targeting of the gut-BM axis, this rewiring of inflammatory haematopoiesis was lost in mice with a depleted microbiome. Underlining the importance of ES-62’s actions in restoring steady-state haematopoiesis, the BM levels of B and T lymphoid cells were shown to be inversely correlated, whilst the levels of OCPs positively correlated, with the severity of joint damage in CIA-mice.

Original language	English
Article number	1334705
Journal	Frontiers in Tropical Diseases
Volume	4
DOIs	https://doi.org/10.3389/fitd.2023.1334705
Publication status	Published - 31 Jan 2024
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

arthritis
ES-62
gut
haematopoiesis
helminth
inflammation
osteoimmunology

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10.3389/fitd.2023.1334705

Cite this

Harnett, M. M., Doonan, J., Tarafdar, A., Pineda, M. A., Duncombe-Moore, J., Buitrago, G., Pan, P., Hoskisson, P. A., Selman, C., & Harnett, W. (2024). The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner. Frontiers in Tropical Diseases, 4, Article 1334705. https://doi.org/10.3389/fitd.2023.1334705

@article{c59d3ce99dd34c80bcce63420902352b,

title = "The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner",

abstract = "The parasitic worm-derived immunomodulator, ES-62 rescues defective levels of IL-10-producing regulatory B cells (Bregs) and suppresses chronic Th1/Th17-driven inflammation to protect against joint destruction in the mouse collagen-induced arthritis (CIA) model of rheumatoid arthritis. Such autoimmune arthritis is also associated with dysbiosis of the gut microbiota and disruption of intestinal barrier integrity. We recently further exploited the CIA model to show that ES-62{\textquoteright}s prevention of joint destruction is associated with protection of intestinal barrier integrity and normalization of the gut microbiota, thereby suppressing the gut pathology that precedes the onset of autoimmunity and joint damage in CIA-mice. As the status of the gut microbiota impacts on immune responses by influencing haematopoiesis, we have therefore investigated whether ES-62 harnesses the homeostatic mechanisms regulating this gut-bone marrow (BM) axis to resolve the chronic inflammation promoting autoimmunity and joint destruction in CIA. Reflecting this, ES-62 was found to counteract the BM myeloid/lymphoid bias typically associated with chronic inflammation and infection. This was achieved primarily by ES-62 acting to maintain the levels of lymphoid lineages (B220+ and CD3+ cells) observed in na{\"i}ve, healthy mice but lost from the BM of CIA-mice. Moreover, ES-62{\textquoteright}s ability to prevent bone-destroying osteoclastogenesis was found to be associated with its suppression of CIA-induced upregulation of osteoclast progenitors (OCPs) in the BM. Critically, and supporting ES-62{\textquoteright}s targeting of the gut-BM axis, this rewiring of inflammatory haematopoiesis was lost in mice with a depleted microbiome. Underlining the importance of ES-62{\textquoteright}s actions in restoring steady-state haematopoiesis, the BM levels of B and T lymphoid cells were shown to be inversely correlated, whilst the levels of OCPs positively correlated, with the severity of joint damage in CIA-mice.",

keywords = "arthritis, ES-62, gut, haematopoiesis, helminth, inflammation, osteoimmunology",

author = "Harnett, \{Margaret M.\} and James Doonan and Anuradha Tarafdar and Pineda, \{Miguel A.\} and Josephine Duncombe-Moore and Geraldine Buitrago and Piaopiao Pan and Hoskisson, \{Paul A.\} and Colin Selman and William Harnett",

note = "Publisher Copyright: Copyright {\textcopyright} 2024 Harnett, Doonan, Tarafdar, Pineda, Duncombe-Moore, Buitrago, Pan, Hoskisson, Selman and Harnett.",

year = "2024",

month = jan,

day = "31",

doi = "10.3389/fitd.2023.1334705",

language = "English",

volume = "4",

journal = "Frontiers in Tropical Diseases",

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Harnett, MM, Doonan, J, Tarafdar, A, Pineda, MA, Duncombe-Moore, J, Buitrago, G, Pan, P, Hoskisson, PA, Selman, C & Harnett, W 2024, 'The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner', Frontiers in Tropical Diseases, vol. 4, 1334705. https://doi.org/10.3389/fitd.2023.1334705

TY - JOUR

T1 - The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner

AU - Harnett, Margaret M.

AU - Doonan, James

AU - Tarafdar, Anuradha

AU - Pineda, Miguel A.

AU - Duncombe-Moore, Josephine

AU - Buitrago, Geraldine

AU - Pan, Piaopiao

AU - Hoskisson, Paul A.

AU - Selman, Colin

AU - Harnett, William

PY - 2024/1/31

Y1 - 2024/1/31

N2 - The parasitic worm-derived immunomodulator, ES-62 rescues defective levels of IL-10-producing regulatory B cells (Bregs) and suppresses chronic Th1/Th17-driven inflammation to protect against joint destruction in the mouse collagen-induced arthritis (CIA) model of rheumatoid arthritis. Such autoimmune arthritis is also associated with dysbiosis of the gut microbiota and disruption of intestinal barrier integrity. We recently further exploited the CIA model to show that ES-62’s prevention of joint destruction is associated with protection of intestinal barrier integrity and normalization of the gut microbiota, thereby suppressing the gut pathology that precedes the onset of autoimmunity and joint damage in CIA-mice. As the status of the gut microbiota impacts on immune responses by influencing haematopoiesis, we have therefore investigated whether ES-62 harnesses the homeostatic mechanisms regulating this gut-bone marrow (BM) axis to resolve the chronic inflammation promoting autoimmunity and joint destruction in CIA. Reflecting this, ES-62 was found to counteract the BM myeloid/lymphoid bias typically associated with chronic inflammation and infection. This was achieved primarily by ES-62 acting to maintain the levels of lymphoid lineages (B220+ and CD3+ cells) observed in naïve, healthy mice but lost from the BM of CIA-mice. Moreover, ES-62’s ability to prevent bone-destroying osteoclastogenesis was found to be associated with its suppression of CIA-induced upregulation of osteoclast progenitors (OCPs) in the BM. Critically, and supporting ES-62’s targeting of the gut-BM axis, this rewiring of inflammatory haematopoiesis was lost in mice with a depleted microbiome. Underlining the importance of ES-62’s actions in restoring steady-state haematopoiesis, the BM levels of B and T lymphoid cells were shown to be inversely correlated, whilst the levels of OCPs positively correlated, with the severity of joint damage in CIA-mice.

AB - The parasitic worm-derived immunomodulator, ES-62 rescues defective levels of IL-10-producing regulatory B cells (Bregs) and suppresses chronic Th1/Th17-driven inflammation to protect against joint destruction in the mouse collagen-induced arthritis (CIA) model of rheumatoid arthritis. Such autoimmune arthritis is also associated with dysbiosis of the gut microbiota and disruption of intestinal barrier integrity. We recently further exploited the CIA model to show that ES-62’s prevention of joint destruction is associated with protection of intestinal barrier integrity and normalization of the gut microbiota, thereby suppressing the gut pathology that precedes the onset of autoimmunity and joint damage in CIA-mice. As the status of the gut microbiota impacts on immune responses by influencing haematopoiesis, we have therefore investigated whether ES-62 harnesses the homeostatic mechanisms regulating this gut-bone marrow (BM) axis to resolve the chronic inflammation promoting autoimmunity and joint destruction in CIA. Reflecting this, ES-62 was found to counteract the BM myeloid/lymphoid bias typically associated with chronic inflammation and infection. This was achieved primarily by ES-62 acting to maintain the levels of lymphoid lineages (B220+ and CD3+ cells) observed in naïve, healthy mice but lost from the BM of CIA-mice. Moreover, ES-62’s ability to prevent bone-destroying osteoclastogenesis was found to be associated with its suppression of CIA-induced upregulation of osteoclast progenitors (OCPs) in the BM. Critically, and supporting ES-62’s targeting of the gut-BM axis, this rewiring of inflammatory haematopoiesis was lost in mice with a depleted microbiome. Underlining the importance of ES-62’s actions in restoring steady-state haematopoiesis, the BM levels of B and T lymphoid cells were shown to be inversely correlated, whilst the levels of OCPs positively correlated, with the severity of joint damage in CIA-mice.

KW - arthritis

KW - ES-62

KW - gut

KW - haematopoiesis

KW - helminth

KW - inflammation

KW - osteoimmunology

U2 - 10.3389/fitd.2023.1334705

DO - 10.3389/fitd.2023.1334705

M3 - Article

AN - SCOPUS:85184726449

SN - 2673-7515

VL - 4

JO - Frontiers in Tropical Diseases

JF - Frontiers in Tropical Diseases

M1 - 1334705

ER -

The parasitic worm product ES-62 protects against collagen-induced arthritis by resetting the gut-bone marrow axis in a microbiome-dependent manner

Abstract

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Keywords

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