Gut Microbiota: a Player in Chronic Pain in Patients With Rheumatoid Arthritis?

NCT ID: NCT05822856

Last Updated: 2023-09-13

Basic Information

• Recruitment Status: UNKNOWN
• Total Enrollment: 125 participants
• Study Classification: OBSERVATIONAL
• Study Start Date: 2023-07-06
• Study Completion Date: 2024-11-30

Brief Summary

Although rheumatoid arthritis (RA) treatments are very effective in reducing inflammation, chronic pain persists in 20 to 30% of patients.

The intestinal microbiota can participate on the pain pathways and a decrease in Faecalibacterium has been associated with chronic pain and chronic fatigue. RA patients have an altered gut microbiota or dysbiosis. Among the bacteria that are most often differentially represented between RA and control, Faecalibacterium, was also found less abundant in RA patients.

The composition of the gut microbiota has never been evaluated in relation to the clinical phenotype of RA patients and in particular to the presence of a diffuse pain. In this study, investigators will test whether the gut microbiota of RA patients, and in particular the decrease of Faecalibacterium, would promote pain sensitization phenomena, and thus, chronic pain despite the control of joint inflammation.

Detailed Description

There are currently many treatments available for patients with rheumatoid arthritis (RA). Although these treatments are very effective on inflammation, chronic pain persists in 20 to 30% of patients, even though clinical and biological remission seems to have been achieved, greatly reducing their daily quality of life. They are characterized in particular by a global lowering of pain thresholds, with a clinical picture of secondary fibromyalgia. Indeed, it seems that RA patients present central and peripheral hypersensitization of nociceptors, abnormalities in central pain processing and a defect in top-down inhibitory pain control mechanisms. It is also possible that RA patients with these inflammation-dissociated polyalgic pictures have a different pathophysiology of their disease than those with inflammation-only pain. A growing body of work shows that the gut microbiota (GM) affects pain pathways at multiple levels through the gut-brain axis. This axis relies, among others, on the afferent pathways of the vagus nerve. The microbiota modulates the activity of the vagus nerve by releasing neurotransmitters (gamma-aminobutyric acid, dopamine), by modulating immune cells (cytokines), by modulating the secretions of enteroendocrine cells (serotonin, cholecystokinins, glucagon-like peptide-1, peptide XY) or by releasing metabolites such as short-chain fatty acids, including butyrate. The latter is known to bind to several functional receptors present on vagal afferents. A decrease in Faecalibacterium has been associated with chronic pain and chronic fatigue.

RA is associated with dysbiosis of the gut microbiota, i.e. a change in the composition of the gut flora . Among the bacteria that are most often differentially represented between RA and control, Fecal bacteria are also less abundant in RA patients. The research team has conducted several experiments that clearly confirm the hypothesis that the microbiota of RA patients acts differently on the gut-brain axis than that of healthy subjects. Indeed, it is known that these RA patients present a defect in the control of parasympathetic activity and a link between dysbiosis of the GM and alteration of the autonomous nervous system (ANS) has already been shown in several pathologies. Considering that the GM is altered in RA and that alterations in the GM can modulate the ANS, the research team therefore hypothesized that the GM of RA patients is capable of altering cardiovascular function and particularly autonomic function. To demonstrate the role of the GM in ANS alterations, a mouse model with humanized microbiota by fecal microbiota transplantation (FMT) of RA patients or healthy subjects (age- and sex-matched controls) was developed and the research team showed that transfer of gut microbiota from RA patients toof mice previously treated with antibiotics alters the autonomic control of cardiac rhythm. Indeed, a decrease in vagal activity, objectified by the analysis of heart rate variability was observed, unpublished data. This confirms our hypothesis that the microbiota of RA patients acts differently on the gut-brain axis than that of healthy subjects. There is therefore a strong rationale for thinking that the microbiota of these patients could influence the central sensitization and control of pain and that RA patients with a fibromyalgia profile have a different microbiota from others.

Bacterial extracellular vesicles (EVs) are important vectors of communication between the gut microbiota and its host. They are the subject of increasing attention and could participate in the gut-brain axis. Indeed, some pathogenic EVs participate in the alteration of the intestinal barrier, pass into the bloodstream and can therefore act remotely from the intestine. Moreover, it has been shown that some bacteria (e.g. A. muciniphila and Faecalibacterium Prausnitzii) modulate the intestinal serotonin system mainly via their EVs. However, our preliminary experiments with stool transfer from RA patients suggest that serotonin (5-hydroxytryptamine 5 HT) is altered, as the research team showed that its expression is decreased in the intestine of mice transplanted with stool from RA patients (unpublished).

Hypothesis: RA patients have an altered gut microbiota or dysbiosis. Among the bacteria that are most often differentially found between RA and control, Faecalibacterium are less abundant in RA patients and a decrease in Faecalibacterium has also been associated with chronic pain patterns . The research team therefore hypothesizes that the intestinal microbiota of RA patients, and in particular the decrease in Faecalibacterium, would promote pain sensitization phenomena, the lack of top-down inhibitory control, and thus chronic pain despite the control of joint inflammation.

To test this hypothesis, the investigating team will compare the composition of the gut microbiota of patients with RA in inflammatory flare, RA in pain-free remission, RA without inflammation with chronic pain, healthy subjects without pain, and patients with fibromyalgia without inflammatory rheumatism. Microbial analysis by 16S ribosomal RNA gene sequencing and quantification of major microbiota-derived fecal metabolites (including short-chain fatty acids and tryptophan derivatives and vesicles

Next, investigators will also functionally evaluate the impact of the gut microbiota on pain sensitization. For this purpose, the research team will use in vitro experimental models (intestinal barrier models (Caco2) and neurons of vagal afferents (primary cultures obtained from murine jugular and nuchal ganglia). In an in vivo study, some faeces samples will be used to humanize the mouse microbiota and then evaluate the impact on tactile sensitivity (Von-Frey).

Conditions

Rheumatoid Arthritis; Fibromyalgia

Study Design

• Observational Model Type: COHORT
• Study Time Perspective: CROSS_SECTIONAL

Study Groups

Patients with RA without inflammation with persistent chronic pain

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Blood sampling and others interventions

Intervention Type: OTHER

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Patients with an active RA (in inflammatory flare)

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Blood sampling and others interventions

Intervention Type: OTHER

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Patients with RA in remission without pain

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Blood sampling and others interventions

Intervention Type: OTHER

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

fibromyalgia patients

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Blood sampling and others interventions

Intervention Type: OTHER

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Control subjects: healthy volunteers

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Blood sampling and others interventions

Intervention Type: OTHER

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Interventions

Blood sampling and others interventions

Blood sampling, faeces collection, questionnaires, tactile sensitivity, sensorial tests

Intervention Type: OTHER

Eligibility Criteria

Inclusion Criteria

For all :

• Age ≥ 18 years old

For A1 Group (3 groups of RA patients of 25 patients each):

• Subject with Rheumatoid Arthritis (RA) meeting the American College of Rheumatology / European League Against Rheumatism ACR/EULAR 2010 criteria, without disease-modifying treatment or with conventional treatment initiated for at least 3 months (at stable dosage for more than 6 weeks)

For A1-1 group : active RA

• DAS28>3.2 with increased CRP (> laboratory standard),
• VAS (Visual Analogic Scale)>5/10 with no other explanation than inflammatory rheumatism

For A1-2 group : RA without inflammation with persistent chronic pain (>3 months) despite control of inflammation and no other identified cause:

• no swollen joint,
• CRP normal (< laboratory standard),
• VAS>5/10

For A1-3 groupe : RA in remission without pain:

• DAS28 ≤2.6,
• no swollen joint,
• CRP normal (< laboratory standard),
• VAS≤2/10

For A2 Group (1 group of 25 Fibromyalgia patients):

• Subjects with Fibromyalgia meeting 2016 diagnostic criteria
• VAS>5/10
• FIRST (FIbromyalgia Rapid Screening Tool) ≥5

For A3 Group (1 group of 25 healthy subjects ):

• healthy and pain-free controls subjects with no progressive disease,
• VAS≤2/10,
• FIRST =0

Exclusion Criteria

• biological therapy for RA: within the previous year for rituximab, within < 4 intervals between anti-TNF, anti-IL6R, or CTLA4-Ig injections and within the previous 15 days for JAKi (JAK inhibitor)
• Corticosteroids > 10 mg/d per os at inclusion
• Corticosteroids > 20 mg/d per os or bolus within 15 days prior to inclusion
• Non-steroidal anti-inflammatory drugs (NSAIDs) and pain medication in the previous week
• Current oral anti-diabetic or proton pump inhibitor (PPI) therapy
• Antibiotic therapy in the previous 3 months
• Infection, cancer in the last 5 years prior to inclusion
• History of other systemic inflammatory/autoimmune diseases
• Not affiliated to a social security
• Patient unwilling or unable to give consent: patient under guardianship or conservatorship,
• Mentally impaired, dementia, language barrier
• Patient under court protection
• Pregnant or breastfeeding woman
• Refusal of written consent

• Minimum Eligible Age: 18 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: Yes

Sponsors

University Hospital, Montpellier

OTHER

Sponsor Role: lead

Responsible Party

Responsibility Role: SPONSOR

Principal Investigators

Claire I DAIEN, MD-PhD

Role: STUDY_DIRECTOR

Centre Hospitalier Universitaire de Montpellier Montpellier

Locations

CHU montpellier - department of rheumatology

Montpellier, , France

Site Status: RECRUITING

Countries

France

Central Contacts

Claire I DAIEN, MD-PhD

Role: CONTACT

c-daien@chu-montpellier.fr

467338710 ext. +33

Facility Contacts

claire DAIEN, MD - PhD

Role: primary

c-daien@chu-montpellier.fr

0033467336733

Other Identifiers

RECHMPL22_0385

Identifier Type: -

Identifier Source: org_study_id