Hepatocyte-specific activity of TSC22D4 triggers progressive NAFLD by impairing mitochondrial function

Gretchen Wolff; Minako Sakurai; Amit Mhamane; Maria Troullinaki; Adriano Maida; Ioannis K Deligiannis; Kelvin Yin; Peter Weber; Jakob Morgenstern; Annika Wieder; Yun Kwon; Revathi Sekar; Anja Zeigerer; Michael Roden; Matthias Blüher; Nadine Volk; Tanja Poth; Thilo Hackert; Lena Wiedmann; Francesca De Angelis Rigotti; Juan Rodriguez-Vita; Andreas Fischer; Rajesh Mukthavaram; Pattraranee Limphong; Kiyoshi Tachikawa; Priya Karmali; Joseph Payne; Padmanabh Chivukula; Bilgen Ekim-Üstünel; Celia P Martinez-Jimenez; Julia Szendrödi; Peter Nawroth; Stephan Herzig

doi:10.1016/j.molmet.2022.101487

Hepatocyte-specific activity of TSC22D4 triggers progressive NAFLD by impairing mitochondrial function

Mol Metab. 2022 Jun:60:101487. doi: 10.1016/j.molmet.2022.101487. Epub 2022 Apr 1.

Authors

Gretchen Wolff¹, Minako Sakurai¹, Amit Mhamane¹, Maria Troullinaki¹, Adriano Maida¹, Ioannis K Deligiannis², Kelvin Yin³, Peter Weber¹, Jakob Morgenstern¹, Annika Wieder¹, Yun Kwon¹, Revathi Sekar¹, Anja Zeigerer¹, Michael Roden⁴, Matthias Blüher⁵, Nadine Volk⁶, Tanja Poth⁷, Thilo Hackert⁸, Lena Wiedmann⁹, Francesca De Angelis Rigotti⁹, Juan Rodriguez-Vita⁹, Andreas Fischer¹⁰, Rajesh Mukthavaram¹¹, Pattraranee Limphong¹¹, Kiyoshi Tachikawa¹¹, Priya Karmali¹¹, Joseph Payne¹¹, Padmanabh Chivukula¹¹, Bilgen Ekim-Üstünel¹, Celia P Martinez-Jimenez¹², Julia Szendrödi¹, Peter Nawroth¹, Stephan Herzig¹³

Affiliations

¹ Institute for Diabetes and Cancer (IDC), Helmholtz Diabetes Center, Helmholtz Centre Munich, Neuherberg, Germany; Joint Heidelberg-IDC Translational Diabetes Program, Inner Medicine 1, Heidelberg University Hospital, Heidelberg, Germany; German Center for Diabetes Research (DZD), Neuherberg, Germany; Chair Molecular Metabolic Control, Technical University Munich, Munich, Germany.
² Helmholtz Pioneer Campus (HPC), Helmholtz Zentrum München, Neuherberg, Germany.
³ Helmholtz Pioneer Campus (HPC), Helmholtz Zentrum München, Neuherberg, Germany; University of Cambridge, Cancer Research UK Cambridge Institute, Robinson Way, Cambridge, United Kingdom.
⁴ Division of Endocrinology and Diabetology, Medical Faculty, Heinrich Heine University, Dusseldorf, Germany; Institute for Clinical Diabetology, German Diabetes Center, Leibniz Center for Diabetes Research at Heinrich Heine University, Dusseldorf, Germany.
⁵ Helmholtz Institute for Metabolic, Obesity and Vascular Research (HI-MAG), Helmholtz Zentrum München, Germany; Medical Department III - Endocrinology, Nephrology, Rheumatology, University of Leipzig Medical Center, University of Leipzig, Germany.
⁶ Tissue Bank of the National Center for Tumor Diseases (NCT) Heidelberg, Germany; Institute of Pathology, Heidelberg University Hospital, Germany.
⁷ CMCP - Center for Model System and Comparative Pathology, Institute of Pathology, Heidelberg University Hospital, Heidelberg, Germany.
⁸ Department of General, Visceral and Transplant Surgery, Heidelberg University Hospital, Heidelberg, Germany.
⁹ Division Vascular Signaling and Cancer (A270), German Cancer Research Center (DKFZ), Heidelberg, Germany.
¹⁰ Division Vascular Signaling and Cancer (A270), German Cancer Research Center (DKFZ), Heidelberg, Germany; Department of Endocrinology and Clinical Chemistry, Heidelberg University Hospital, Heidelberg, Germany.
¹¹ Arcturus Therapeutics, San Diego, CA, USA.
¹² Helmholtz Pioneer Campus (HPC), Helmholtz Zentrum München, Neuherberg, Germany; TUM School of Medicine, Technical University of Munich, Munich, Germany.
¹³ Institute for Diabetes and Cancer (IDC), Helmholtz Diabetes Center, Helmholtz Centre Munich, Neuherberg, Germany; Joint Heidelberg-IDC Translational Diabetes Program, Inner Medicine 1, Heidelberg University Hospital, Heidelberg, Germany; German Center for Diabetes Research (DZD), Neuherberg, Germany; Chair Molecular Metabolic Control, Technical University Munich, Munich, Germany. Electronic address: Stephan.herzig@helmholtz-muenchen.de.

Abstract

Objective: Fibrotic organ responses have recently been identified as long-term complications in diabetes. Indeed, insulin resistance and aberrant hepatic lipid accumulation represent driving features of progressive non-alcoholic fatty liver disease (NAFLD), ranging from simple steatosis and non-alcoholic steatohepatitis (NASH) to fibrosis. Effective pharmacological regimens to stop progressive liver disease are still lacking to-date.

Methods: Based on our previous discovery of transforming growth factor beta-like stimulated clone (TSC)22D4 as a key driver of insulin resistance and glucose intolerance in obesity and type 2 diabetes, we generated a TSC22D4-hepatocyte specific knockout line (TSC22D4-HepaKO) and exposed mice to control or NASH diet models. Mechanistic insights were generated by metabolic phenotyping and single-nuclei RNA sequencing.

Results: Hepatic TSC22D4 expression was significantly correlated with markers of liver disease progression and fibrosis in both murine and human livers. Indeed, hepatic TSC22D4 levels were elevated in human NASH patients as well as in several murine NASH models. Specific genetic deletion of TSC22D4 in hepatocytes led to reduced liver lipid accumulation, improvements in steatosis and inflammation scores and decreased apoptosis in mice fed a lipogenic MCD diet. Single-nuclei RNA sequencing revealed a distinct TSC22D4-dependent gene signature identifying an upregulation of mitochondrial-related processes in hepatocytes upon loss of TSC22D4. An enrichment of genes involved in the TCA cycle, mitochondrial organization, and triglyceride metabolism underscored the hepatocyte-protective phenotype and overall decreased liver damage as seen in mouse models of hepatocyte-selective TSC22D4 loss-of-function.

Conclusions: Together, our data uncover a new connection between targeted depletion of TSC22D4 and intrinsic metabolic processes in progressive liver disease. Hepatocyte-specific reduction of TSC22D4 improves hepatic steatosis and promotes hepatocyte survival via mitochondrial-related mechanisms thus paving the way for targeted therapies.

Keywords: Fibrosis; Hepatocyte-specific; NAFLD; NASH; TSC22D4.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Diabetes Mellitus, Type 2* / metabolism
Fibrosis
Hepatocytes / metabolism
Humans
Insulin Resistance*
Lipids
Mice
Mice, Inbred C57BL
Mitochondria / metabolism
Non-alcoholic Fatty Liver Disease* / metabolism
Transcription Factors / metabolism

Substances

Lipids
TSC22D4 protein, human
Transcription Factors