Alcoholic liver disease (ALD) accounts for ~50% of deaths due to cirrhosis and ~30% of all liver-related deaths in the US. How ethanol damages the liver remains poorly understood, and therapies are lacking or unproven. Our goal is to understand the pathogenesis of ALD. We observed widespread, reversible hepatic mitochondrial depolarization (mtDepo), increased mitophagic burden and elevated serum mitochondrial DNA (mtDNA) in mice after ethanol treatment. We propose to test the novel hypothesis that ethanol metabolism induces mtDepo, which in turn stimulates mitophagy. Markedly increased mitophagic burden overwhelms the capacity of lysosomes to process autophagosomes, particularly when processing of depolarized mitochondria into mitophagosomes and then into lysosomes is compromised after chronic ethanol exposure, leading to extracellular release of damaged mitochondria, mitophagosomes and/or autolysosomes containing mitochondrial damage-associated molecular pattern (mtDAMP) molecules to cause a profibrotic inflammatory response and liver injury.
In Specific Aim 1 using intravital multiphoton microscopy, we will explore if mtDepo occurs in living mice after chronic ethanol and is exacerbated by superimposed binge drinking and in an unique fibrosis-inducing ethanol/cholesterol model we developed. We will determine the relation of mtDepo to hepatic injury, inflammation and fibrosis. We will also explore if inhibition of acetaldehyde (AcAld) formation by alcohol dehydrogenase and CYP2E1 deficiency, accelerated AcAld oxidation by Alda-1, and FK506 (blocker of depolarization) decrease mtDepo and liver injury/inflammation/fibrosis after chronic ethanol.
In Aim 2, we will determine the relation of mtDepo to mitophagy. Using genetic and pharmacological interventions in combination with intravital and electron microscopy and analyses of molecular indicators of mitophagic flux, we will elucidate if ethanol-induced mtDepo initiates mitophagy or if mitophagy causes mtDepo. We will determine if mitophagy/mitophagosome processing is blunted by chronic, chronic plus cholesterol and chronic plus binge ethanol and further explore if inhibition of autophagic processing exacerbates liver injury/inflammation/fibrosis after chronic ethanol.
In Aim 3, we will characterize how mtDepo and compromised mitophagy/processing contribute to mtDAMP release after ethanol. We will characterize release into serum of mtDAMPs after acute ethanol and chronic, chronic plus cholesterol and chronic plus binge ethanol to determine the relationship of mtDAMP release to liver injury/inflammation/fibrosis. We will also determine how up and down-modulation of mtDepo, mitophagy and processing of mitophagosomes alters mtDAMP release after ethanol. This study will elucidate a novel link between early mitochondrial changes associated with ethanol metabolism and the later development of liver injury/inflammation/fibrosis and thus fill a critical gap in understanding ALD pathogenesis. This study should also identify new therapeutic targets of ALD and novel biomarkers for monitoring ALD severity/progression.

Public Health Relevance

The overall goal of this study is to elucidate the link between early mitochondrial changes associated with ethanol metabolism and the progression of alcoholic liver disease (ALD) so that new therapeutic targets and modalities for prevention/treatment of ALD can be identified. In previous experiments, we observed a novel and unprecedented reversible mitochondrial depolarization in livers of ethanol-treated mice. Using acute and chronic ethanol feeding models, including our newly developed unique fibrosis-inducing chronic ethanol plus cholesterol model, we will determine the relation of mitochondrial depolarization to mitophagy, mitochondria- derived inflammatory/fibrotic mediators called mitochondrial damage-associated molecular pattern molecules (mtDAMPs), and the later development of alcoholic liver injury, inflammation and fibrosis, thus filling a critical gap in understanding the pathogenesis of ALD.

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA025379-03
Application #
9920650
Study Section
Hepatobiliary Pathophysiology Study Section (HBPP)
Program Officer
Orosz, Andras
Project Start
2018-08-01
Project End
2023-04-30
Budget Start
2020-05-01
Budget End
2021-04-30
Support Year
3
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Medical University of South Carolina
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
183710748
City
Charleston
State
SC
Country
United States
Zip Code
29407