Rifaximin SSD in Dementia Trial (RIDE)

Overview

The Rifaximin in Dementia Trial (RIDE) is a Phase 1/2 clinical trial investigating the effects of rifaximin, a non-absorbable antibiotic, on patients with Alzheimer's disease (AD) and vascular dementia (VaD). This trial represents a novel approach targeting the gut-brain axis to potentially modify dementia progression["@nct"].

Overview

The Rifaximin in Dementia Trial (RIDE) is a Phase 1/2 clinical trial investigating the effects of rifaximin, a non-absorbable antibiotic, on patients with Alzheimer's disease (AD) and vascular dementia (VaD). This trial represents a novel approach targeting the gut-brain axis to potentially modify dementia progression["@nct"].

Rifaximin is a gut-targeted antibiotic that acts locally in the gastrointestinal tract with minimal systemic absorption. By modulating the gut microbiome, this trial tests the hypothesis that improving gut microbial function can reduce systemic inflammation and positively impact cognitive function in dementia patients.

Trial Details

| Attribute | Value |
|-----------|-------|
| NCT Number | [NCT06718686](https://clinicaltrials.gov/study/NCT06718686) |
| Phase | Phase 1/2 |
| Status | Recruiting |
| Enrollment | 20 patients (estimated) |
| Study Type | Interventional |
| Design | Sequential allocation, triple-blind (participant, care provider, outcomes assessor) |
| Start Date | December 30, 2024 |
| Primary Completion | December 2025 (estimated) |
| Completion | May 2026 (estimated) |

Sponsors and Collaborators

• Lead Sponsor: Jasmohan Bajaj, MD (Hunter Holmes McGuire VA Medical Center)
• Collaborator: Bausch Health Americas, Inc.
• Principal Investigator: Jasmohan Bajaj, MD (Richmond VA Medical Center)

Location

• Richmond VA Medical Center — Richmond, Virginia, United States
• Status: Currently recruiting

Study Hypothesis and Objectives

Hypothesis

Overall Objective

• Gut microbial structure and function
• Cognitive and daily function
• Caregiver burden

Mechanism of Action

Gut-Brain Axis Modulation

Rifaximin exerts its potential therapeutic effects through multiple mechanisms related to the [gut-brain axis](/mechanisms/gut-brain-axis):

1. Microbiome Modulation

• Selective antimicrobial action in the gut lumen
• Reduction of pathogenic bacterial overgrowth
• Preservation of beneficial gut bacteria
• Modulation of gut microbial diversity

2. Reduction of Systemic Inflammation

• Decreased gut-derived endotoxins (LPS)
• Reduced pro-inflammatory cytokines (IL-6, TNF-α, IL-1β)
• Increased anti-inflammatory cytokines (IL-10)
• Lower lipopolysaccharide-binding protein (LBP) levels

3. Metabolite Production

• Increased short-chain fatty acid (SCFA) production
• Modulation of bile acid metabolism
• Improved gut barrier function

4. Neuroprotective Effects

• Reduced neuroinflammation via decreased systemic inflammatory signals
• Potential reduction in amyloid-β burden
• Protection against tau pathology through decreased neuroinflammation

Why Rifaximin?

Rifaximin is an ideal candidate for gut-brain axis therapy because:

• Minimal systemic absorption: <1% systemic bioavailability
• Gut-selective action: Primarily acts in the gastrointestinal tract
• Good safety profile: Well-tolerated in previous clinical applications
• Broad-spectrum activity: Effective against gram-positive and gram-negative bacteria
• Low resistance development: Limited impact on gut bacterial resistance patterns

Study Design

Intervention Model

Blinding

Treatment Arms

| Arm | Intervention |
|-----|---------------|
| Placebo | Placebo tablet BID |
| Rifaximin SSD 40mg IR BID | Rifaximin SSD 40 mg IR tablet BID |

Treatment Duration

Eligibility Criteria

Inclusion Criteria

• Probable Alzheimer's Disease (AD) or Vascular Dementia (VaD) mild or moderate based on Clinical Dementia Rating Scale
• Males and Females Age ≥ 65 years
• Community living with availability of caregiver to accompany participant to study visits
• Able to consent or legal guardian who can consent (with participant assent)
• Legally authorized representative (LAR) and caregiver for the study is the same individual
• Fluency in written and spoken English (both participant and caregiver)

Exclusion Criteria

• Dementia not due to AD or VaD
• Clinically significant agitation or aggression (requiring antipsychotic medication)
• Delusions and/or hallucinations
• Severe psychopathology including major depression
• Unstable, severe, or poorly controlled medical conditions
• Visual and/or hearing disorder that prevents completion of neuropsychologic evaluations
• Diarrhea
• Hypersensitivity to rifaximin or any rifamycin antimicrobial agent
• Antibiotic use in the prior 6 months
• Taking medications that interact with Rifaximin (P-glycoprotein inhibitors require investigator discussion)
• History of alcohol and/or drug abuse
• Participation in another investigational drug trial in the last 30 days

Outcome Measures

Primary Outcomes

| Measure | Description | Time Frame |
|---------|-------------|------------|
| Change in stool and serum short-chain fatty acid levels | SCFA in stool and serum: rifaximin SSD phase vs placebo phase | 10 weeks |
| Change in bile acids in stool and serum | Bile acids: rifaximin SSD phase vs placebo phase | 10 weeks |

Secondary Outcomes

| Measure | Description | Time Frame |
|---------|-------------|------------|
| Systemic inflammatory change | Serum LBP, inflammatory cytokines (IL-6, TNF-α, IL-10, IL-1β) | 10 weeks |
| Stool microbiome composition | 16SrRNA microbiome composition and diversity | 10 weeks |
| Dementia biomarkers | Plasma Aβ42, Aβ40, Aβ42/40 ratio, p-tau181 | 10 weeks |
| MMSE | Change in Mini-Mental State Examination | 10 weeks |
| Cognitive testing (PHES) | Psychometric Hepatic Encephalopathy Score | 10 weeks |
| CDR-SB | Clinical Dementia Rating - Sum of Boxes | 10 weeks |
| EncephalApp Stroop performance | Off time and on time performance | 10 weeks |
| Critical flicker fusion analysis | CFF threshold | 10 weeks |
| Katz Index of Independence in ADL | Activity of Daily Living | 10 weeks |
| Lawton-Brody IADL | Instrumental Activities of Daily Living | 10 weeks |
| Zarit Burden Interview | Caregiver burden | 10 weeks |
| Sickness Impact profile | Quality of Life | 10 weeks |
| PROMIS-29 | Patient-Reported Outcomes Measurement Information System | 10 weeks |
| Safety | Serious adverse event rates | 10 weeks |

Clinical Relevance

Gut-Brain Axis in Dementia

• Gut microbiome dysbiosis is associated with cognitive decline
• Systemic inflammation from gut sources may contribute to neuroinflammation
• Modulating the gut microbiome may offer a novel therapeutic approach

Biomarkers Being Studied

• Amyloid-β: Aβ42/40 ratio (reduced ratio associated with cerebral amyloid)
• Tau: p-tau181 (marker of tau pathology and neuronal damage)
• Inflammatory markers: LBP, cytokines
• Microbiome markers: SCFAs, bile acids

Potential Impact

Related Pages

• [Gut-Brain Axis in Neurodegeneration](/mechanisms/gut-brain-axis)
• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Exenatide Parkinson's Trial](/clinical-trials/exenatide-parkinsons) — Another gut-brain axis therapy trial
• [Valacyclovir HSV1 Parkinson's Trial](/clinical-trials/valacyclovir-hsv1-pd) — Antiviral approach to neurodegeneration

References