Alcohol inhibits T-cell glucose metabolism and hepatitis in ALDH2-deficient mice and humans: roles of acetaldehyde and glucocorticoids

Yanhang Gao; Zhou Zhou; Tianyi Ren; Seung-Jin Kim; Yong He; Wonhyo Seo; Adrien Guillot; Yanhua Ding; Ruihong Wu; Shuang Shao; Xiaomei Wang; Hong Zhang; Wei Wang; Dechun Feng; Mingjiang Xu; Elaine Han; Wei Zhong; Zhanxiang Zhou; Pal Pacher; Junqi Niu; Bin Gao

doi:10.1136/gutjnl-2018-316221

Alcohol inhibits T-cell glucose metabolism and hepatitis in ALDH2-deficient mice and humans: roles of acetaldehyde and glucocorticoids

Gut. 2019 Jul;68(7):1311-1322. doi: 10.1136/gutjnl-2018-316221. Epub 2018 Aug 18.

Authors

Yanhang Gao^#^{1

2}, Zhou Zhou^#¹, Tianyi Ren^#^{1

2}, Seung-Jin Kim¹, Yong He¹, Wonhyo Seo¹, Adrien Guillot¹, Yanhua Ding², Ruihong Wu², Shuang Shao², Xiaomei Wang², Hong Zhang², Wei Wang¹, Dechun Feng¹, Mingjiang Xu¹, Elaine Han¹, Wei Zhong³, Zhanxiang Zhou³, Pal Pacher⁴, Junqi Niu², Bin Gao¹

Affiliations

¹ Laboratory of Liver Diseases, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, Maryland, USA.
² Department of Hepatology, First Affiliated Hospital, Jilin University, Changchun, China.
³ Center for Translational Biomedical Research, University of North Carolina at Greensboro, Kannapolis, North Carolina, USA.
⁴ Laboratory of Cardiovascular Physiology and Tissue Injury, National Institutes of Health/NIAAA, Bethesda, Maryland, USA.

^# Contributed equally.

Abstract

Objective: Aldehyde dehydrogenase 2 (ALDH2), a key enzyme to detoxify acetaldehyde in the liver, exists in both active and inactive forms in humans. Individuals with inactive ALDH2 accumulate acetaldehyde after alcohol consumption. However, how acetaldehyde affects T-cell hepatitis remains unknown.

Design: Wild-type (WT) and Aldh2 knockout (Aldh2^-/-) mice were subjected to chronic ethanol feeding and concanavalin A (ConA)-induced T-cell hepatitis. Effects of acetaldehyde on T-cell glucose metabolism were investigated in vitro. Human subjects were recruited for binge drinking and plasma cortisol and corticosterone measurement.

Results: Ethanol feeding exacerbated ConA-induced hepatitis in WT mice but surprisingly attenuated it in Aldh2^-/- mice despite higher acetaldehyde levels in Aldh2^-/- mice. Elevation of serum cytokines and their downstream signals in the liver post-ConA injection was attenuated in ethanol-fed Aldh2^-/- mice compared to WT mice. In vitro exposure to acetaldehyde inhibited ConA-induced production of several cytokines without affecting their mRNAs in mouse splenocytes. Acetaldehyde also attenuated interferon-γ production in phytohaemagglutinin-stimulated human peripheral lymphocytes. Mechanistically, acetaldehyde interfered with glucose metabolism in T cells by inhibiting aerobic glycolysis-related signal pathways. Finally, compared to WT mice, ethanol-fed Aldh2^-/- mice had higher levels of serum corticosterone, a well-known factor that inhibits aerobic glycolysis. Blockade of corticosterone partially restored ConA-mediated hepatitis in ethanol-fed Aldh2^-/- mice. Acute alcohol drinking elevated plasma cortisol and corticosterone levels in human subjects with higher levels in those with inactive ALDH2 than those with active ALDH2.

Conclusions: ALDH2 deficiency is associated with elevated acetaldehyde and glucocorticoids post-alcohol consumption, thereby inhibiting T-cell activation and hepatitis.

Keywords: AKT; Concanavalin A; T-cell hepatitis; binge drinking; glucose metabolism; glycolysis.

Publication types

Research Support, N.I.H., Intramural
Research Support, Non-U.S. Gov't

MeSH terms

Aldehyde Dehydrogenase, Mitochondrial / physiology*
Animals
Binge Drinking / metabolism*
Binge Drinking / pathology
Concanavalin A
Corticosterone / blood
Disease Models, Animal
Ethanol
Glucose / metabolism*
Hepatitis / etiology
Hepatitis / metabolism*
Hepatitis / prevention & control*
Humans
Hydrocortisone / blood
Mice
T-Lymphocytes / physiology*

Substances

Concanavalin A
Ethanol
Aldehyde Dehydrogenase, Mitochondrial
Glucose
Corticosterone
Hydrocortisone

Grants and funding

P30 DK056350/DK/NIDDK NIH HHS/United States