Fecal Microbiota Transplantation in Patients with Alcohol-Associated Cirrhosis: A Clinical Trial (Aug 2025, n=19) "significant reduction in hepatic encephalopathy severity" FMT 

Fecal Microbiota Transplants

Michael Harrop

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https://www.mdpi.com/2077-0383/14/17/5981

Abstract​


Background: Gut microbiota dysregulation is increasingly recognized as a key contributor to the progression of liver cirrhosis and its complications, particularly hepatic encephalopathy. Fecal microbiota transplantation (FMT) has emerged as a novel therapeutic strategy aimed at restoring intestinal microbial homeostasis and modulating systemic inflammation.

Methods: This prospective, single-center clinical trial evaluated the short-term safety and efficacy of FMT in patients with alcohol-related liver cirrhosis. Clinical assessment, liver stiffness (via elastography), steatosis (controlled attenuation parameter), inflammatory biomarkers, and extended biochemical panels were analyzed at baseline, one week and one month post-FMT. A control group receiving standard medical therapy was used for comparison.

Results: FMT was associated with a significant reduction in hepatic encephalopathy severity (p = 0.014), sustained improvements in liver stiffness (p = 0.027) and decreased steatosis (p = 0.025). At one month, C-reactive protein and neutrophil-to-lymphocyte ratio both declined significantly (p = 0.043), indicating a measurable anti-inflammatory effect. No serious adverse events were recorded. In comparison with controls, FMT recipients showed lower systemic inflammation and improved neuropsychiatric status.

Conclusions
: FMT demonstrated a favorable safety profile and yielded early clinical and biochemical benefits in patients with cirrhosis. These preliminary findings support the potential utility of microbiota-based interventions in chronic liver disease and warrant validation in larger, multicenter trials.
The colonoscopic procedure was performed using standard protocols, including bowel preparation with polyethylene glycol solutions.

Donors:
Fecal donors were selected from among both patient relatives and unrelated healthy volunteers. Preference was given to young individuals without comorbidities, who provided written informed consent. All donors underwent rigorous clinical and paraclinical screening to minimize the risk of contamination, as recommended by other studies in the literature on this subject [21,22]. Blood samples were collected for general assessment, including complete blood count, general biochemical and coagulation tests and also specific investigations to exclude HIV, hepatitis and autoimmune diseases. Additionally, stool samples were examined for occult bleeding, as well as for bacterial, parasitic and other infectious agents. Screening also included a mandatory questionnaire to identify potential epidemiological risks capable of transmitting infectious or other diseases to immunocompromised recipients with cirrhosis.
 
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