Abstract

Liver cirrhosis is a major cause of morbidity and mortality in Veterans, primarily due to complications such as ascites and hepatic encephalopathy (HE). HE is linked with a systemic pro-inflammatory milieu propagated by an impaired intestinal barrier and gut dysbiosis. Despite maximal therapy (lactulose/rifaximin), a significant proportion of Veterans have HE that continues to recur, which is a major burden on their caregivers and VHA system. We have recently published a small randomized trial of fecal microbial transplantation (FMT), in this population, which was safe and prevented total and HE-related hospitalizations. This was associated with favorable bile acid (BA) and microbial changes which lasted for >1 year with one FMT. A similar small oral capsule FMT trial is underway at our center with good safety signals. There is also evidence in non-cirrhotic FMT studies that microbe-free portions can be as effective as full FMT. However, the mechanism of action of FMT in cirrhosis is needs further investigation. We hypothesize that ?Fecal microbial transplant delivered from the combined oral and rectal route is safe, well- tolerated and associated with lower hospitalizations, improved modulation of gut microbial composition and functionality and brain function in patients with hepatic encephalopathy compared to those treated with FMT from either routes alone or with placebo; this improvement is mediated by microbial products?. We will test this hypothesis using two translational aims Aim 1: To determine the effect of dual oral and rectal administration of FMT from a rational donor on clinical outcomes (hospitalizations, brain function, quality of life) and host-microbiota interactions (microbial composition and bile acid composition with systemic and intestinal inflammation), compared to single route of administration and placebo, in cirrhotic patients with HE using a randomized, phase II clinical trial. Outpatients with recurrent HE (n=100) will be randomized into four groups (Group 1: Dual oral and rectal FMT, Group 2: Oral FMT and rectal placebo, Group 3: Oral placebo and Rectal FMT and Group 4: Oral and rectal placebo) and followed for 6 months under an FDA IND double-blind clinical trial. FMT donors will be selected using machine learning on the basis of beneficial taxa from OpenBiome donors (collaborator), which will be used for all FMT-assigned subjects. The primary outcome is all-cause hospitalizations. Patients will undergo baseline evaluation for cirrhosis severity, brain function, intestinal permeability along with collection of serum and stool and fecal bile acid profile analysis. Patients will be followed till 6 months for outcomes. We will define the effect of FMT on systemic inflammation, intestinal permeability, bile acid profile, and its linkage with microbial composition and clinical outcomes between groups.
Aim 2 : To determine the effect of human FMT on neuro-inflammation and gut microbial function using germ-free mice and conventional cirrhotic mice with microbe-rich and microbe-free (sterile) supernatants from the FMT donors. It is not clear which components of the FMT material, the microbes or their products such as bile acids, mediate its effects. Entire and microbe-free supernatants generated from pooled FMT donor samples, recipients? baseline samples and post-FMT samples, will be used to humanize GF mice. In addition, conventional cirrhotic mice will receive healthy donor material using the same protocol. Differences in neuro-inflammation will be studied between conventional cirrhotic and GF mice after colonization and between those colonized with entire samples and with only microbial products. A specific change in intestinal bile acid profile as a mediator of these changes will be investigated. The team has been working cohesively with expertise in clinical and translational cirrhosis research in Veterans. These results will set the foundation for future trials determining the role of FMT in liver disease and help define better donor-patient matches from a microbial perspective in this underserved population.

Public Health Relevance

Chronic liver disease, leading to cirrhosis is epidemic in Veterans. A major complication of cirrhosis is hepatic encephalopathy (HE), that can cause lasting brain damage if it recurs. Current treatments for HE target inflammation produced in the bowels but are often not effective. Our preliminary study showed that feces from a healthy donor, also known as fecal microbial transplant (FMT), was safe using an enema and oral capsule routes. However, it is not clear which route or combination of fecal transplant administration would be helpful in preventing hospitalizations in HE patients. It is also unclear whether it is the microbes in the FMT or their products that are associated with the improvement. Our proposed trial studies the effect of oral and enema routes of FMT in Veterans with HE to prevent hospitalizations, and also aims to find out which FMT components are associated with improvement using animal models.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
2I01CX001076-05A1
Application #
9657201
Study Section
Special Emphasis Panel (ZRD1)
Project Start
2015-01-01
Project End
2023-03-31
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
5
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
VA Veterans Administration Hospital
Department
Type
DUNS #
146678115
City
Richmond
State
VA
Country
United States
Zip Code
23249

  Publications

Bajaj, Jasmohan S; Kakiyama, Genta; Cox, I Jane et al. (2018) Alterations in gut microbial function following liver transplant. Liver Transpl 24:752-761
Reuter, Bradley; Walter, Kara; Bissonnette, Julien et al. (2018) Assessment of the spectrum of hepatic encephalopathy: A multicenter study. Liver Transpl 24:587-594
Burroughs, Thomas K; Wade, James B; Ellwood, Michael S et al. (2018) Effect of Post-Traumatic Stress Disorder on Cognitive Function and Covert Hepatic Encephalopathy Diagnosis in Cirrhotic Veterans. Dig Dis Sci 63:481-485
Patidar, Kavish R; Kang, Le; Bajaj, Jasmohan S et al. (2018) Fractional excretion of urea: A simple tool for the differential diagnosis of acute kidney injury in cirrhosis. Hepatology 68:224-233
Ahluwalia, Vishwadeep; Wade, James B; White, Melanie B et al. (2018) Brain Integrity Changes Underlying Cognitive and Functional Recovery Postliver Transplant Continue to Evolve Over 1 Year. Transplantation 102:461-470
Bajaj, Jasmohan S; Thacker, Leroy R; Fagan, Andrew et al. (2018) Gut microbial RNA and DNA analysis predicts hospitalizations in cirrhosis. JCI Insight 3:
Li, Xiaojiaoyang; Liu, Runping; Huang, Zhiming et al. (2018) Cholangiocyte-derived exosomal long noncoding RNA H19 promotes cholestatic liver injury in mouse and humans. Hepatology 68:599-615
Liu, Runping; Li, Xiaojiaoyang; Huang, Zhiming et al. (2018) C/EBP homologous protein-induced loss of intestinal epithelial stemness contributes to bile duct ligation-induced cholestatic liver injury in mice. Hepatology 67:1441-1457
Acharya, Chathur; Sahingur, Sinem Esra; Bajaj, Jasmohan S (2017) Microbiota, cirrhosis, and the emerging oral-gut-liver axis. JCI Insight 2:
Betrapally, Naga S; Gillevet, Patrick M; Bajaj, Jasmohan S (2017) Gut microbiome and liver disease. Transl Res 179:49-59

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