eIF2α phosphorylation is required to prevent hepatocyte death and liver fibrosis in mice challenged with a high fructose diet

Woo-Gyun Choi; Jaeseok Han; Ji-Hyeon Kim; Mi-Jeong Kim; Jae-Woo Park; Benbo Song; Hee-Jeong Cha; Hye-Seon Choi; Hun-Taeg Chung; In-Kyu Lee; Tae-Sik Park; Maria Hatzoglou; Hueng-Sik Choi; Hyun Ju Yoo; Randal J Kaufman; Sung Hoon Back

doi:10.1186/s12986-017-0202-6

eIF2α phosphorylation is required to prevent hepatocyte death and liver fibrosis in mice challenged with a high fructose diet

Nutr Metab (Lond). 2017 Aug 1:14:48. doi: 10.1186/s12986-017-0202-6. eCollection 2017.

Authors

Woo-Gyun Choi^#¹, Jaeseok Han^#^{2

3}, Ji-Hyeon Kim^#^{1

4}, Mi-Jeong Kim¹, Jae-Woo Park¹, Benbo Song⁵, Hee-Jeong Cha⁶, Hye-Seon Choi¹, Hun-Taeg Chung¹, In-Kyu Lee⁷, Tae-Sik Park⁸, Maria Hatzoglou⁹, Hueng-Sik Choi¹⁰, Hyun Ju Yoo⁴, Randal J Kaufman², Sung Hoon Back¹

Affiliations

¹ School of Biological Sciences, University of Ulsan, Ulsan, 44610 Republic of Korea.
² Soonchunhyang Institute of Med-bio Science (SIMS), Soonchunhyang University, Cheonan-si, Choongchungnam-do, 31151 Republic of Korea.
³ Degenerative Diseases Program, Sanford Burnham Prebys Medical Discovery Institute, 10901 North Torrey Pines Road, La Jolla, CA 92037 USA.
⁴ Biomedical Research Center, Asan Medical Center, College of Medicine, University of Ulsan, Seoul, 05505 Republic of Korea.
⁵ NGM Biopharmaceuticals, Inc., 333 Oyster Point Blvd, South San Francisco, CA 94080 USA.
⁶ Department of Pathology, Ulsan University Hospital, University of Ulsan College of Medicine, Ulsan, 44043 Republic of Korea.
⁷ Department of Internal Medicine and Biochemistry and Cell Biology, Kyungpook National University School of Medicine, Daegu, 41944 Republic of Korea.
⁸ Department of Life Science, Gachon University, Seongnam, Republic of Korea.
⁹ Department of Nutrition, Case Western Reserve University School of Medicine, Cleveland, OH 44106 USA.
¹⁰ School of Biological Sciences and Technology, Chonnam National University, Gwangju, Republic of Korea.

^# Contributed equally.

Abstract

Background: Dietary fructose can rapidly cause fatty liver in animals through de novo lipogenesis (DNL) and contribute to the development and severity of nonalcoholic fatty liver disease (NAFLD). In response to diverse cellular insults including endoplasmic reticulum (ER) and oxidative stress, phosphorylation of the eukaryotic translation initiation factor 2 alpha subunit (eIF2α) attenuates general translation initiation, allowing cells to conserve resources and initiate adaptive gene expression to restore homeostasis. The present study aimed to investigate the role of eIF2α phosphorylation in protecting against NAFLD induced by high fructose ingestion in a hepatocyte-specific eIF2α-phosphorylation-deficient mouse model.

Methods: Hepatocyte-specific non-phosphorylatable (S51A) eIF2α knock-in (A/A;fTg/0;Cre^Hep/0, A/A^Hep ) mice were generated by crossing A/A;fTg/fTg mice with the floxed WT eIF2α transgene (fTg) with Alfp-Cre recombinase transgenic S/A;Cre^Hep/0 (S/A-Cre^Hep ) mice. Hepatocyte-specific eIF2α-phosphorylation-deficient 3-month-old mice or 12-month-old mice were fed a 60% high fructose diet (HFrD) for 16 or 5 wks, and the effects of eIF2α-phosphorylation deficiency on NADP/NADPH and GSSG/GSH levels, ROS-defense gene expression, oxidative damage, cell death, and fibrosis were observed.

Results: Prolonged fructose feeding to mice caused dysregulation of the unfolded protein response (UPR) sensor activation and UPR gene expression, and then led to decreased expression of several ROS defense genes including glutathione biogenesis genes. Nonetheless, these changes were not sufficient to induce the death of eIF2α phosphorylation-sufficient hepatocytes. However, there was a substantial increase in hepatocyte death and liver fibrosis in fructose-fed middle-aged mice deficient in hepatocyte-specific eIF2α phosphorylation because of diminished antioxidant capacity due to reduced expression of antioxidant enzymes (GPX1 and HO-1) and lower NADPH and glutathione levels, as well as a possible increase in ROS-induced damage from infiltrating NOX2-expressing leukocytes; all this led to a vicious cycle of hepatocyte death and leukocyte infiltration.

Conclusion: Our findings suggest that eIF2α phosphorylation maintains NADPH and GSH levels and controls the expression of ROS-defense genes, thereby protecting hepatocytes from oxidative stresses induced by fructose metabolism.

Keywords: Aging; Antioxidant enzymes; Fibrosis; Glutathione; High fructose diet; NADPH; Nonalcoholic fatty liver disease; Oxidative stress; eIF2α phosphorylation.

Abstract

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