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Efficacy of UMT in CG Patients With PL
Sponsor: Peking University First Hospital
Summary
To clinically validate the pathological role of Cer accumulation and evaluate a novel microbiota-targeted intervention, we conducted a comprehensive analysis of bladder mucosal specimens from a well-characterized patient cohort stratified according to the established histopathological criteria for CG severity. Our findings revealed specific accumulation of the sphingolipid species Cer(d18:1/18:0) in high-risk CG tissues, which was absent in both low-risk and control groups. Notably, tissue levels of Cer(d18:1/18:0) demonstrated a strong positive correlation with histopathological grade, highlighting its clinical relevance as a driver of PL-CG progression and supporting its potential utility as a prognostic biomarker. Given the established association between the urinary microbiota and local metabolite production, and considering that the pathogenic urinary microbiota likely serves as the source of this immunomodulatory Cer, we designed and implemented a randomized controlled trial to assess therapeutic remodeling of the bladder microenvironment through UMT. Following the one-month regimen of weekly intravesical instillations, UMT significantly reduced disease burden in PL-CG patients. At the 12-week follow-up, the UMT group exhibited a substantially lower Interstitial Cystitis Symptom Index (ICSI) compared to controls, with an overall response rate of 58.18%. Significant improvements were also observed in key clinical symptoms, including daytime urinary frequency and voiding-related pain. Notably, clinical improvement occurred without a significant reduction in mucosal colonization levels of B. thetaiotaomicron. This observation suggests that UMT's efficacy does not arise from broad bacterial eradication but rather from functional modulation of the microbiota-host interface. Instead, therapeutic benefit was strongly associated with direct depletion of the pathogenic metabolite. Urinary Cer(d18:1/18:0) levels were markedly reduced following UMT, which coincided with the coordinated down-regulation of key pro-inflammatory cytokines in the bladder mucosa, including IL-6, TNF-α, IL-1β, and CXCL1. This sequential cascade thus establishes a clear mechanistic link between pathogenic metabolite clearance, resolution of inflammation, and symptomatic relief.
Official title: Efficacy of Urinary Microbiota Transplantation (UMT) in Cystitis Glandularis (CG) Patients With Pelvic Lipomatosis (PL)
Key Details
Gender
All
Age Range
18 Years - Any
Study Type
INTERVENTIONAL
Enrollment
110
Start Date
2025-02-01
Completion Date
2026-02-28
Last Updated
2026-04-15
Healthy Volunteers
Yes
Conditions
Interventions
Urinary Microbiota Transplantation (UMT)
This intervention is a rigorously prepared donor-derived urinary microbiota transplantation product. After passing strict multi-pathogen screening, donor urine is processed via differential centrifugation (3000g for 10min, 10000g for 20min, 100000g for 60min) and sequential sterile filtration through 0.45μm and 0.22μm PES membranes to isolate and purify the microbial fraction. The microbial pellet is resuspended in sterile PBS (autoclaved at 121℃ for 20min), supplemented with 1μM myriocin and metabolite-rich supernatant, and confirmed sterile via final sterility testing before clinical use. Participants receive intravesical instillation once weekly for 4 consecutive weeks for the treatment of high-risk chronic cystitis/interstitial cystitis.
0.9% Sodium Chloride Injection (Normal Saline, Placebo)
This arm receives intravesical instillation of sterile 0.9% sodium chloride injection (normal saline) as a placebo control. The placebo is identical in appearance, volume, and administration schedule to the urinary microbiota transplantation (UMT) product in the experimental arm, administered once weekly for 4 consecutive weeks to maintain the double-blind study design. The placebo has no therapeutic activity and is used to evaluate the efficacy and safety of UMT for the treatment of high-risk chronic cystitis/interstitial cystitis.
Locations (1)
Peking University First Hospital
Beijing, Beijing Municipality, China