Abstract

Alcoholic liver disease (ALD) is one of the most common forms of chronic liver injury in the United States. Chronic ethanol consumption results in toxic metabolites in the liver and increases endothelial senescence and dysfunction leading to inflammation and liver damage. Aging is linked with the severity and poor prognosis of various liver diseases including alcoholic liver diseases and is associated gradual alteration of structure and function in liver tissues and cells including liver sinusoidal endothelial cells. Endothelial dysfunction is an early pathophysiological hallmark in the development of liver disease. Senescence, the cellular equivalent of aging, was proposed to be involved in endothelial dysfunction. Indeed, enhanced cellular senescence was associated with a poor outcome in alcohol-related fatty liver disease, while increased hepatic senescence mediators such as p21 and TNF-? that were related to liver/endothelial dysfunction in ALD cirrhosis. Increasing evidence supports that non-coding RNAs (ncRNAs) play a central role in various cellular pathways by regulating gene expression. Indeed, there is a strong link between ethanol metabolism and endotoxin/lipopolysaccharide (LPS) induced cellular senescence and endothelial dysfunction in ALDs. Hepatic sinusoids, connected directly to the portal circulation, serve as the first barrier against these inflammatory and noxious stimuli. We have novel preliminary data showing that selective ncRNA/microRNA genes are aberrantly expressed in liver specimens from ALD animals and are regulated and involved in ethanol metabolism. In particular, we have found: (a) intra-gastric ethanol feeding significantly increased the expression of cellular senescence initiators EGR1, PAI-1 and Id1 and silenced p53 effectors E2F1 and IGFBP3; (b) ethanol enhanced microRNA-34a and p53 expressions and altered their target genes such as SIRT1, PPAR? and HNF4?, which leads to senescence phenotypes in liver sinusoidal endothelial cells (LSECs); (c) Inhibition of miR-34a/p53/TLR4 by anti-miR-34a/p53 Morpholino and CRISPR/cas9 approaches has successfully recovered alcoholic liver injury in ethanol treated mice in vivo. Although the combined evidence supports a link between ncRNAs and alcoholic liver disease, there is a critical need to determine the underlying mechanism whereby ethanol-dependent miRNAs promote alcoholic liver injury. Our long-term goal is to determine underlying mechanisms contributing to alcohol- induced liver disease so that new mechanism-based, clinically effective prevention or treatment strategies can be developed. The objective for this proposal is to determine how ethanol- dependent ncRNAs mediate endothelial dysfunction and senescence in the progression of alcoholic liver diseases. Our central hypothesis is that ethanol-dependent miRNAs contribute to alcoholic liver injury through regulation of cellular senescence and dysfunction in endothelial cells. This hypothesis was formulated based upon the existing literature and our own preliminary data described above. The following three specific aims are proposed: First, we will determine the effects of ncRNA mediated cellular senescence and endothelial dysfunction in senescence accelerated mice with alcoholic liver injury in vivo (Aim 1). Second, we will identify the downstream targets of p53-miR-34a axis that are involved in endothelial senescence and dysfunction in miR-34a and p53 knockout mice in vivo (Aim 2). Further, we will determine the effects of endothelial progenitor cell related ncRNAs enriched extracellular vesicles on anti-senescence/anti- endothelial dysfunction and recovery of alcoholic liver injury in vivo (Aim 3). At the completion of the proposed research, it is our expectation to have an important positive impact because a mechanistic understanding of the role ncRNAs play in alcohol related injury, endothelial cell and senescence mediated liver disease is likely to provide a foundation for the development of evidence-based clinically useful approaches to treat or prevent human alcoholic liver diseases including US veterans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
2I01BX001724-09A1
Application #
9774478
Study Section
Special Emphasis Panel (ZRD1)
Project Start
2012-07-01
Project End
2023-09-30
Budget Start
2019-10-01
Budget End
2020-09-30
Support Year
9
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Rlr VA Medical Center
Department
Type
DUNS #
608434697
City
Indianapolis
State
IN
Country
United States
Zip Code
46202

  Publications

Zhou, Tianhao; Wu, Nan; Meng, Fanyin et al. (2018) Knockout of secretin receptor reduces biliary damage and liver fibrosis in Mdr2-/- mice by diminishing senescence of cholangiocytes. Lab Invest 98:1449-1464
Kennedy, Lindsey; Hargrove, Laura; Demieville, Jennifer et al. (2018) Blocking H1/H2 histamine receptors inhibits damage/fibrosis in Mdr2-/- mice and human cholangiocarcinoma tumorigenesis. Hepatology :
Meng, Fanyin; Kennedy, Lindsey; Hargrove, Laura et al. (2018) Ursodeoxycholate inhibits mast cell activation and reverses biliary injury and fibrosis in Mdr2-/- mice and human primary sclerosing cholangitis. Lab Invest 98:1465-1477
Kennedy, Lindsey; Hargrove, Laura; Demieville, Jennifer et al. (2018) Knockout of l-Histidine Decarboxylase Prevents Cholangiocyte Damage and Hepatic Fibrosis in Mice Subjected to High-Fat Diet Feeding via Disrupted Histamine/Leptin Signaling. Am J Pathol 188:600-615
Ehrlich, Laurent; Scrushy, Marinda; Meng, Fanyin et al. (2018) Biliary epithelium: A neuroendocrine compartment in cholestatic liver disease. Clin Res Hepatol Gastroenterol 42:296-305
Lewis, Phillip L; Su, Jimmy; Yan, Ming et al. (2018) Complex bile duct network formation within liver decellularized extracellular matrix hydrogels. Sci Rep 8:12220
Ehrlich, Laurent; O'Brien, April; Hall, Chad et al. (2018) ?7-nAChR Knockout Mice Decreases Biliary Hyperplasia and Liver Fibrosis in Cholestatic Bile Duct-Ligated Mice. Gene Expr 18:197-207
Sato, Keisaku; Meng, Fanyin; Giang, Thao et al. (2018) Mechanisms of cholangiocyte responses to injury. Biochim Biophys Acta Mol Basis Dis 1864:1262-1269
Cai, Yuli; Li, Honggui; Liu, Mengyang et al. (2018) Disruption of adenosine 2A receptor exacerbates NAFLD through increasing inflammatory responses and SREBP1c activity. Hepatology 68:48-61
Guo, Xin; Shu, Chang; Li, Honggui et al. (2017) Cyclic GMP-AMP Ameliorates Diet-induced Metabolic Dysregulation and Regulates Proinflammatory Responses Distinctly from STING Activation. Sci Rep 7:6355

Showing the most recent 10 out of 42 publications