Abstract

Alcoholic liver disease and cirrhosis are one of the leading causes of morbidity and mortality in the US, as well as in the VA Health System. However, despite several programs to prevent and treat alcohol abuse, a significant proportion of affected Veterans continue to drink, even in the setting of cirrhosis. This can lead to a substantial burden that stems from an unchecked inflammatory milieu and endotoxemia due to bacterial translocation that precipitates infections, multi-organ failure and death. These patients are poor candidates for abstinence pharmacological therapy, are often non-adherent and cannot be offered liver transplant due to their continued drinking. Therefore prevention of this unchecked inflammation and bacterial translocation is critical; however, the exact mechanisms behind these are unclear, which is a major gap in our knowledge. Bile acids (BAs) and gut microbiota are key components of the intestinal milieu, whose interaction impacts bacterial translocation and inflammation. Our group has focused on delineating the role of microbiota, using culture- independent analyses, with inflammation and their modulation by BAs, especially the membrane-destabilizing secondary BAs in cirrhosis. We also discovered that actively drinking cirrhotics have a highly significant increase in fecal secondary BAs and intestinal inflammatory cytokine expression that may mediate intestinal injury and potentiate inflammation in these patients. Therefore, the study of the role of secondary BAs in the pathogenesis of intestinal and systemic inflammation in the context of altered gut microbiota or dysbiosis, in actively drinking cirrhotics compared to abstinent alcoholic cirrhotics and cirrhotics with non-alcoholic liver disease is critical in delineating the role of the intestinal milieu in the progression of liver disease. Our central hypothesis: Patients with cirrhosis, especially alcoholic cirrhotic patients who continue to drink, develop enhanced intestinal and systemic inflammation due to an increase in secondary bile acids associated with altered gut microbiota. This central hypothesis will be tested using these two specific aims:
Specific aim 1 : To define the effect of secondary bile acids on systemic and gut inflammation, gut microbiome and endotoxemia in cirrhotic patients with continued alcohol abuse compared to abstinent alcoholic cirrhotics and non-alcoholic cirrhotics using a systems biology approach. We will study the interaction of BAs with microbiome of the duodenal, ileal, colonic and fecal origin with systemic and intestinal wall inflammation in age- and cirrhosis-severity matched actively drinking cirrhotics compared to abstinent alcoholic cirrhotics, cirrhotic with NAFLD and healthy controls using a systems biology approach in 100 subjects.
Specific Aim 2 : To define the role of bile acids and gut microbiota in the pathogenesis of the increased intestinal and systemic inflammation, endotoxemia and bacterial translocation in a germ-free mouse model after colonization with stool from alcoholic cirrhotic patients. We will be utilizing germ-free mice to elucidate the individual contributions of bile acids and microbiota on endotoxemia, inflammation and bacterial translocation. Six groups of germ-free mice will be used: 1) without intervention 2) fed deoxycholic acid alone 3) colonized with healthy human stool 4) colonized with alcoholic cirrhotic stool. Each group will be evaluated for intestinal and systemic inflammation, endotoxemia, BA profile (serum, gallbladder, liver, fecal, intestinal contents) and microbiome changes (Groups 3-4) will be performed after colonization and compared between groups. The studies will provide a novel integrative platform to study the role of secondary bile acids and gut microbiota in the development of intestinal and systemic inflammation in all cirrhotic patients using cutting-edge translational and systems biology approaches. We expect the results of this proposal to increase our insight into the development of focused therapeutic approaches that benefit this underserved population of Veterans.

Public Health Relevance

Liver cirrhosis due to alcohol is a major reason for death in Veterans. Affected patients are not candidates for medicines for sobriety or for liver transplant because of their drinking. They are also hospitalized and die at a higher rate than those who do not drink. The major causes of death are infections and inflammation caused by bacteria that go through their bowel wall. Therefore we need to stop this inflammation from occurring by studying the bowel microbes and their interactions with molecules such as bile acids, which can impact bowel integrity. We propose to study the interaction of bile acids with microbes in the bowels of cirrhotic patients who continue to drink compared to other cirrhotics and healthy people. We will also study the effect of bile acids and microbes independently and together on inflammation by transplanting stool from affected patients into germ-free mice or mice without any microbes. These studies will help us find out the mechanisms behind why these Veterans have inflammation and infections and help us design treatments to prevent these in the future.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01CX001076-03
Application #
9278099
Study Section
Gastroenterology (GAST)
Project Start
2015-01-01
Project End
2018-12-31
Budget Start
2017-01-01
Budget End
2017-12-31
Support Year
3
Fiscal Year
2017
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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