Bone loss and aggravated autoimmune arthritis in HLA-DRβ1-bearing humanized mice following oral challenge with Porphyromonas gingivalis

Sandal, Indra; Karydis, Anastasios; Luo, Jiwen; Prislovsky, Amanda; Whittington, Karen B.; Rosloniec, Edward F.; Dong, Chen; Novack, Deborah V.; Mydel, Piotr; Zheng, Song Guo; Radic, Marko; Brand, David

doi:10.1186/s13075-016-1143-6

Cited by 50 publications

(50 citation statements)

References 35 publications

(36 reference statements)

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“…A recent study demonstrated that the exacerbation of autoimmune arthritis in human leukocyte antigen-DR1 humanized C57Bl/6 mice under P. gingivalis infection was shown to be followed by a transitory increase of systemic Th17 population and in cervical lymph nodes. This same study also suggested a complementary mechanism because they detected the production of anti-citrullinated protein antibodies (ACPAs) - (Sandal et al, 2016); importantly, the generation of ACPAs was not detected in P. gingivalis-infected wild type C57Bl/6 mice. In this context of controversies, the present study showed that PD-induced arthritis aggravation in an AIA model is dependent on IL-17RA activation.…”

Section: Discussionmentioning

confidence: 87%

The aggravation of arthritis by periodontitis is dependent of IL‐17 receptor A activation

Aquino

Talbot

Sônego

et al. 2017

J Clinic Periodontology

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Section: Discussionmentioning

confidence: 87%

The aggravation of arthritis by periodontitis is dependent of IL‐17 receptor A activation

Aquino

Talbot

Sônego

et al. 2017

J Clinic Periodontology

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“…This is an important differentiation from human PAD genes (which endocitrullinate) as one of the proposed mechanisms in which P. gingivalis induces arthritis is via the release of the virulence factor arginine-gingipanis (RpgB) which cleaves host proteins exposing the terminal arginine residue which is then free to undergo citrullination via PPAD with the creation of neo-epitopes and subsequent ACPA positivity ( Wegner et al, 2010 ). This hypothesis is supported by murine models which demonstrated that mice with laboratory induced arthritis had higher autoantibody production and joint destruction in those infected with wild type PPAD compared to those with mutated deficient PPAD genes ( Maresz et al, 2013 ; Gully et al, 2014 ; Sandal et al, 2016 ; Courbon et al, 2019 ). Sandel et al demonstrated this pathway was restricted via HLA-DRB1 positive mice suggesting that in addition to the presence of P. gingivalis and its associated expressed virulence factors, a genetic predisposition was also required.…”

Section: Periodontal Microbiome and Acpamentioning

confidence: 85%

The Role of the Microbiome in Driving RA-Related Autoimmunity

Rooney

Mankia

Emery

2020

Front. Cell Dev. Biol.

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Once referred to as “normal commensal flora” the human microbiome plays an integral role between health and disease. The host mucosal surface replete with a multitude of immune cells is a vast arena constantly sensing and responding to antigen presentation and microbial by-products. It is this key role that may allow the microbiome to prime or protect the host from autoimmune disease. Rheumatoid arthritis (RA) is a chronic, disabling inflammatory condition characterized by a complex multifactorial etiology. The presence of certain genetic markers has been proven to increase susceptibility to RA however it does not guarantee disease development. Given low concordance rates demonstrated in monozygotic twin studies there is a clear implication for the involvement of external players in RA pathogenesis. Since the historical description of rheumatoid factor, numerous additional autoantibodies have been described in the sera of RA patients. The presence of anti-cyclic citrullinated protein antibody is now a standard test, and is associated with a more severe disease course. Interestingly these antibodies are detectable in patient’s sera long before the clinical signs of RA occur. The production of autoantibodies is driven by the lack of tolerance of the immune system, and how tolerance is broken is a crucial question for understanding RA development. Here we review current literature on the role of the microbiome in RA development including periodontal, gut and lung mucosa, with particular focus on proposed mechanisms of host microbiome interactions. We discuss the use of Mendelian randomization to assign causality to the microbiome and present considerations for future studies.

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“…The precise mechanism by which these microbial changes during the development of CIA modulate host immunity requires further study. However, using a known oral pathogen, Sandal et al demonstrated that oral infection with Porphyromonas gingivalis could transiently expand Th17 cells in the draining cervical lymph nodes and circulation and exacerbated disease in HLA–DRB1–transgenic mice with CIA, even in those that had previously resisted development of disease . Another study showed that treatment by oral gavage with Prevotella histicola attenuates CIA in HLA–DQ8–transgenic mice by increasing IL‐10–producing Treg cells and reducing Th17 cells in the gut .…”

Section: Discussionmentioning

confidence: 99%

Modulation of Inflammatory Arthritis in Mice by Gut Microbiota Through Mucosal Inflammation and Autoantibody Generation

Jubair

Hendrickson

Severs

et al. 2018

Arthritis & Rheumatology

128

125

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Bone loss and aggravated autoimmune arthritis in HLA-DRβ1-bearing humanized mice following oral challenge with Porphyromonas gingivalis

Cited by 50 publications

References 35 publications

The aggravation of arthritis by periodontitis is dependent of IL‐17 receptor A activation

The aggravation of arthritis by periodontitis is dependent of IL‐17 receptor A activation

The Role of the Microbiome in Driving RA-Related Autoimmunity

Modulation of Inflammatory Arthritis in Mice by Gut Microbiota Through Mucosal Inflammation and Autoantibody Generation

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