Reduced mitochondrial resilience enables non-canonical induction of apoptosis after TNF receptor signaling in virus-infected hepatocytes

Sandra Lampl; Marianne K Janas; Sainitin Donakonda; Marcus Brugger; Kerstin Lohr; Annika Schneider; Katrin Manske; Laura E Sperl; Susan Kläger; Bernhard Küster; Jennifer Wettmarshausen; Constanze Müller; Melanie Laschinger; Daniel Hartmann; Norber Hüser; Fabiana Perocchi; Philippe Schmitt-Kopplin; Franz Hagn; Lars Zender; Veit Hornung; Christoph Borner; Andreas Pichlmair; Hamid Kashkar; Martin Klingenspor; Marco Prinz; Sabrina Schreiner; Marcus Conrad; Philipp J Jost; Hans Zischka; Katja Steiger; Martin Krönke; Dietmar Zehn; Ulrike Protzer; Mathias Heikenwälder; Percy A Knolle; Dirk Wohlleber

doi:10.1016/j.jhep.2020.06.026

Reduced mitochondrial resilience enables non-canonical induction of apoptosis after TNF receptor signaling in virus-infected hepatocytes

J Hepatol. 2020 Dec;73(6):1347-1359. doi: 10.1016/j.jhep.2020.06.026. Epub 2020 Jun 26.

Authors

Sandra Lampl¹, Marianne K Janas¹, Sainitin Donakonda¹, Marcus Brugger¹, Kerstin Lohr¹, Annika Schneider¹, Katrin Manske¹, Laura E Sperl², Susan Kläger³, Bernhard Küster³, Jennifer Wettmarshausen⁴, Constanze Müller⁵, Melanie Laschinger⁶, Daniel Hartmann⁶, Norber Hüser⁶, Fabiana Perocchi⁷, Philippe Schmitt-Kopplin⁸, Franz Hagn⁹, Lars Zender¹⁰, Veit Hornung¹¹, Christoph Borner¹², Andreas Pichlmair¹³, Hamid Kashkar¹⁴, Martin Klingenspor¹⁵, Marco Prinz¹⁶, Sabrina Schreiner¹⁷, Marcus Conrad¹⁸, Philipp J Jost¹⁹, Hans Zischka²⁰, Katja Steiger²¹, Martin Krönke¹⁴, Dietmar Zehn²², Ulrike Protzer²³, Mathias Heikenwälder²⁴, Percy A Knolle²⁵, Dirk Wohlleber¹

Affiliations

¹ Institute of Molecular Immunology and Experimental Oncology, University Hospital München rechts der Isar; Technical University of Munich, Munich, Germany.
² Institute of Structural Biology, Helmholtz Zentrum Munich, Neuherberg, Germany.
³ Structural Membrane Biochemistry, Bavarian NMR Center at the Department of Chemistry and Institute for Advanced Study, Technical University of Munich, Garching, Germany.
⁴ Institute for Obesity and Diabetes, Helmholtz Zentrum München, Neuherberg, Germany.
⁵ Research Unit Analytical Biogeochemistry, Helmholtz Zentrum München, Neuherberg, Germany.
⁶ Clinic of Surgery, University Hospital München rechts der Isar; Technical University of Munich, Munich, Germany.
⁷ Research Unit Analytical Biogeochemistry, Helmholtz Zentrum München, Neuherberg, Germany; Munich Cluster for Systems Neurology, Munich, Germany.
⁸ Research Unit Analytical Biogeochemistry, Helmholtz Zentrum München, Neuherberg, Germany; Chair of Analytical Food Chemistry, Technical University of Munich, Freising-Weihenstephan, Germany.
⁹ Institute of Structural Biology, Helmholtz Zentrum Munich, Neuherberg, Germany; Structural Membrane Biochemistry, Bavarian NMR Center at the Department of Chemistry and Institute for Advanced Study, Technical University of Munich, Garching, Germany.
¹⁰ Division of Gastroenterology and Oncology, University Hospital Tübingen, Tübingen, Germany.
¹¹ Center for Integrated Protein Science (CIPSM), Gene Center and Department of Biochemistry, Ludwig-Maximilians-Universität München, München, Germany.
¹² Institute of Molecular Medicine and Cell Research, Faculty of Medicine, University of Freiburg, Freiburg, Germany.
¹³ Institute of Virology, Technical University of Munich, Munich, Germany.
¹⁴ Cologne Excellence Cluster on Cellular Stress Response in Aging-Associated Diseases, University of Cologne, Cologne, Germany; Institute for Microbiology and Hygiene, and Center of Molecular Medicine, University of Cologne, Cologne, Germany.
¹⁵ Molecular Nutritional Medicine, Else Kröner-Fresenius Center, Technical University of Munich, Freising-Weihenstephan, Germany.
¹⁶ Institute of Neuropathology, Medical Faculty, University of Freiburg, Germany.
¹⁷ Institute of Virology, Helmholtz-Zentrum München, Neuherberg, Germany.
¹⁸ Institute of Metabolism and Cell Death, Helmhotz Zentrum MUnich, Neuherberg, Germany.
¹⁹ III. Medical Department for Hematology and Oncology, Klinikum rechts der Isar, Technical University of Munich, Munich, Germany.
²⁰ Institute of Molecular Toxicology and Pharmacology, Helmholtz Zentrum München/German Research Center for Environmental Health GmbH, Neuherberg, Germany; Institute of Toxicology and Environmental Hygiene, School of Medicine, Technical University of Munich, Munich, Germany.
²¹ Institute of Pathology, Technical University of Munich, Munich, Germany.
²² Institute of Physiology and Immunology, Technical University of Munich, Freising-Weihenstephan, Germany.
²³ Institute of Virology, Technical University of Munich, Munich, Germany; Institute of Virology, Helmholtz-Zentrum München, Neuherberg, Germany; German Center for Infection research (DZIF), Munich Partner Site, Germany.
²⁴ Institute of Chronic Inflammation and Cancer, German-Cancer-Research Center, Heidelberg, Germany.
²⁵ Institute of Molecular Immunology and Experimental Oncology, University Hospital München rechts der Isar; Technical University of Munich, Munich, Germany; Institute of Physiology and Immunology, Technical University of Munich, Freising-Weihenstephan, Germany. Electronic address: percy.knolle@tum.de.

PMID: 32598967
DOI: 10.1016/j.jhep.2020.06.026

Abstract

Background & aims: Selective elimination of virus-infected hepatocytes occurs through virus-specific CD8 T cells recognizing peptide-loaded MHC molecules. Herein, we report that virus-infected hepatocytes are also selectively eliminated through a cell-autonomous mechanism.

Methods: We generated recombinant adenoviruses and genetically modified mouse models to identify the molecular mechanisms determining TNF-induced hepatocyte apoptosis in vivo and used in vivo bioluminescence imaging, immunohistochemistry, immunoblot analysis, RNAseq/proteome/phosphoproteome analyses, bioinformatic analyses, mitochondrial function tests.

Results: We found that TNF precisely eliminated only virus-infected hepatocytes independently of local inflammation and activation of immune sensory receptors. TNF receptor I was equally relevant for NF-kB activation in healthy and infected hepatocytes, but selectively mediated apoptosis in infected hepatocytes. Caspase 8 activation downstream of TNF receptor signaling was dispensable for apoptosis in virus-infected hepatocytes, indicating an unknown non-canonical cell-intrinsic pathway promoting apoptosis in hepatocytes. We identified a unique state of mitochondrial vulnerability in virus-infected hepatocytes as the cause for this non-canonical induction of apoptosis through TNF. Mitochondria from virus-infected hepatocytes showed normal biophysical and bioenergetic functions but were characterized by reduced resilience to calcium challenge. In the presence of unchanged TNF-induced signaling, reactive oxygen species-mediated calcium release from the endoplasmic reticulum caused mitochondrial permeability transition and apoptosis, which identified a link between extrinsic death receptor signaling and cell-intrinsic mitochondrial-mediated caspase activation.

Conclusion: Our findings reveal a novel concept in immune surveillance by identifying a cell-autonomous defense mechanism that selectively eliminates virus-infected hepatocytes through mitochondrial permeability transition.

Lay summary: The liver is known for its unique immune functions. Herein, we identify a novel mechanism by which virus-infected hepatocytes can selectively eliminate themselves through reduced mitochondrial resilience to calcium challenge.

Keywords: Antiviral immunity; Hepatocyte apoptosis; Mitochondrial function; Mitochondrial permeability transition; TNF.

Publication types

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

MeSH terms

Animals
Apoptosis / immunology
Calcium Signaling
Caspase 8 / metabolism*
Cells, Cultured
Hepatocytes* / metabolism
Hepatocytes* / virology
Humans
Mice
Mitochondria, Liver* / immunology
Mitochondria, Liver* / metabolism
Mitochondrial Transmembrane Permeability-Driven Necrosis
Receptors, Tumor Necrosis Factor, Type I / metabolism*
Signal Transduction
Tumor Necrosis Factor-alpha / metabolism

Substances

Receptors, Tumor Necrosis Factor, Type I
Tumor Necrosis Factor-alpha
Caspase 8