Article

Microbiome Changes Linked to Childhood Spondyloarthritis

(ACR Pediatrics 2014) More links between the gut and arthritis: Children with spondyloarthritis have different enteric bacteria than healthy kids, adding to a growing body of evidence linking microbes to autoimmune disorders.

To the increasing hints that disturbances in the human-bacterial ecosystem may be at the root of rheumatic disease, add this: Children with spondyloarthritis (SpA) have the same low levels of a microbe called Faecalibacterium prausnitzii that occur in children with inflammatory bowel disease.

This brings a microbiome connection to two autoimmune disorders that also have "strong clinical and pathological links," observed Matthew Stoll MD, an assistant professor of rheumatology in the division of pediatric rheumatology at the University of Alabama-Birmingham. At the ACR pediatric rheumatology meeting in Orlando, Stoll described studies that used DNA sequening to characterize all species of enteric bacteria in 28 children with enthesitis-related arthritis and 13 controls who were either healthy or had non-inflammatory joint pain.

Levels of Faecalibacterium were significantly lower in the children with SpA than in controls. (Some subsets of SpA patients also had non-significantly higher levels of Bacterioides.)

F. prausnitzii  appears to have anti-inflammatory effects, Stoll told Rheumatology Network, although "it is not known yet exactly what the effect is." A next step will to be repeat the studies in a larger cohort of patients with other subtypes of juvenile arthritis.

"The number of diseases associated with changes in microbial diversity continues to grow by the day," said microbiologist David Artis PhD of the University of Pennsylvania Perelman School of Medicine at a separate session on the microbiome.

In germ-free mice, he added, it appears that permanent shifts in microbiota after antibiotic treatment can influence the development of the immune system, and influence pro-inflammatory or regulatory immune responses. He mentioned a study by Daniel Littman of the New York University School of Medicine and coworkers showing that a single species of bacterium introduced into the gut of germ-free mice could drive the development of autoimmune arthritis. A widely cited paper by the same team, published last November, linked the presence of the gut bacterium Prevotella copri to susceptibility to arthritis.

"This organism is difficult to work with and culture," said Artis, "so there has been no followup to date. But certainly the associations in this paper were very strong."

Growing attention to the "barrier cells" in skin and mucosa has revealed a unique set of innate immune cells that are neither T nor B cells, are not myeloid or granulocytic, and have no receptors for pathogens, but are increased in inflammatory conditions, he added. Apparently important regulators of barrier function, they are the only cells to express receptors for interleukin-22.

"We're just beginning to understand the role of these cells in innate immunity and infection," Artis said. The "real challenge," he added, is to identify the ligands responsible for these newfound immune phenomena, and to identify small molecules to control them.

Related Videos
John Tesser, MD, Adjunct Assistant Professor of Medicine, Midwestern University, and Arizona College of Osteopathic Medicine, and Lecturer, University of Arizona Health Sciences Center, and Arizona Arthritis & Rheumatology Associates
Gaith Noaiseh, MD: Nipocalimab Improves Disease Measures, Reduces Autoantibodies in Sjogren’s
Laure Gossec, MD, PhD: Informing Physician Treatment Choices for Psoriatic Arthritis
Søren Andreas Just, MD, PhD: Developing AI to Mitigate Rheumatologist Shortages for Disease Assessment
Shreena K. Gandhi, MBBS: Recognizing Fibromyalgia as a Continuous Variable, Trait Diagnosis
Reducing Treatment Burden of Pegloticase for Uncontrolled Gout, with Orrin Troum, MD
Exploring CAR T-cell Therapy for Rheumatic/Autoimmune Diseases With Georg Schett, MD
John Stone, MD, MPH: Inebilizumab Efficacious for IgG4-Related Disease in MITIGATE Study
Uncovering the Role of COVID-19 in Rheumatic Disease, with Leonard Calabrese, DO
Related Content
Orrin Troum, MD, clinical professor of medicine, Keck School of Medicine, University of Southern California, and director, clinical rheumatology research, Providence St John's Hospital, Santa Monica, California
November 22nd 2024

Shortened Pegloticase Infusions Feasible for Uncontrolled Gout, Reduces Treatment Burden

Victoria Johnson
Emerging Agents in the Treatment of Rheumatic Diseases
October 2nd 2023

Emerging Agents in the Treatment of Rheumatic Diseases

Nehad Soloman, MD, FACR Andrew Sharobeem, DO, FACR Philip J. Mease, MD
Søren Andrea Just, MD, PhD, associate professor, University of Southern Denmark, and Odense University Hospital – Svendborg.
November 21st 2024

AI Assessments, Robotics Perform to Rheumatologist Levels in Joint Assessment

Victoria Johnson
Challenges with Step Therapy Protocols in Treating Rheumatoid Arthritis
August 31st 2023

Challenges with Step Therapy Protocols in Treating Rheumatoid Arthritis

Nehad Soloman, MD, FACR Andrew Sharobeem, DO, FACR John B. Boone, MD, FACR Madelaine Feldman MD, FACR
Megan Clowse, MD, MPH, Associate Professor of Medicine, Associate Professor in Obstetrics and Gynecology, and Associate Professor in Population Health Sciences, and Chief of the Division of Rheumatology and Immunology, Duke University School of Medicine
November 19th 2024

DZP Improves Disease Activity and Reduces Corticosteroid Use in SLE

Victoria Johnson
John Tesser, MD, Adjunct Assistant Professor of Medicine, Midwestern University, and Arizona College of Osteopathic Medicine, and Lecturer, University of Arizona Health Sciences Center, and Arizona Arthritis & Rheumatology Associates
November 19th 2024

Vagus Nerve Stimulation Yields Responses in Refractory Rheumatoid Arthritis

Victoria Johnson
© 2024 MJH Life Sciences

All rights reserved.