论文信息 - Type I Interferon Signaling Disrupts the Hepatic Urea Cycle and Alters Systemic Metabolism to Suppress T Cell Function

Type I Interferon Signaling Disrupts the Hepatic Urea Cycle and Alters Systemic Metabolism to Suppress T Cell Function

Summary Infections induce complex host responses linked to antiviral defense, inflammation, and tissue damage and repair. We hypothesized that the liver, as a central metabolic hub, may orchestrate systemic metabolic changes during infection. We infected mice with chronic lymphocytic choriomeningitis virus (LCMV), performed RNA sequencing and proteomics of liver tissue, and integrated these data with serum metabolomics at different infection phases. Widespread reprogramming of liver metabolism occurred early after infection, correlating with type I interferon (IFN-I) responses. Viral infection induced metabolic alterations of the liver that depended on the interferon alpha/beta receptor (IFNAR1). Hepatocyte-intrinsic IFNAR1 repressed the transcription of metabolic genes, including Otc and Ass1, which encode urea cycle enzymes. This led to decreased arginine and increased ornithine concentrations in the circulation, resulting in suppressed virus-specific CD8+ T cell responses and ameliorated liver pathology. These findings establish IFN-I-induced modulation of hepatic metabolism and the urea cycle as an endogenous mechanism of immunoregulation. Video Abstract

[1] E. Wherry,et al. Molecular and cellular insights into T cell exhaustion , 2015, Nature Reviews Immunology.

[2] M. Netea,et al. The Cellular and Molecular Basis of Translational Immunometabolism. , 2015, Immunity.

[3] Steven J. M. Jones,et al. Circos: an information aesthetic for comparative genomics. , 2009, Genome research.

[4] Chun Jimmie Ye,et al. Parsing the Interferon Transcriptional Network and Its Disease Associations , 2016, Cell.

[5] Gordon K Smyth,et al. Statistical Applications in Genetics and Molecular Biology Linear Models and Empirical Bayes Methods for Assessing Differential Expression in Microarray Experiments , 2011 .

[6] R. Medzhitov. Origin and physiological roles of inflammation , 2008, Nature.

[7] Michael D. Buck,et al. Metabolic Instruction of Immunity , 2017, Cell.

[8] M. Vignuzzi,et al. Inhibition of Polyamine Biosynthesis Is a Broad-Spectrum Strategy against RNA Viruses , 2016, Journal of Virology.

[9] D. Gabrilovich. Myeloid-Derived Suppressor Cells , 2017, Cancer Immunology Research.

[10] A. Bergthaler,et al. The lipid-sensor TREM2 aggravates disease in a model of LCMV-induced hepatitis , 2017, Scientific Reports.

[11] G. Hotamışlıgil. Inflammation, metaflammation and immunometabolic disorders , 2017, Nature.

[12] A. Pegg,et al. Polyamine metabolism and cancer: treatments, challenges and opportunities , 2018, Nature Reviews Cancer.

[13] M. Tomita,et al. Serum metabolomics reveals γ-glutamyl dipeptides as biomarkers for discrimination among different forms of liver disease. , 2011, Journal of hepatology.

[14] R. Zinkernagel,et al. T cell-mediated hepatitis in mice infected with lymphocytic choriomeningitis virus. Liver cell destruction by H-2 class I- restricted virus-specific cytotoxic T cells as a physiological correlate of the 51Cr-release assay? , 1986, The Journal of experimental medicine.

[15] D. Wheatley,et al. Recombinant human arginase inhibits the in vitro and in vivo proliferation of human melanoma by inducing cell cycle arrest and apoptosis , 2011, Pigment cell & melanoma research.

[16] M. Mann,et al. Universal sample preparation method for proteome analysis , 2009, Nature Methods.

[17] P. Murray. Amino acid auxotrophy as a system of immunological control nodes , 2016, Nature Immunology.

[18] J. Locasale,et al. Distinct Regulation of Th17 and Th1 Cell Differentiation by Glutaminase-Dependent Metabolism , 2018, Cell.

[19] Abhishek K. Jha,et al. Network integration of parallel metabolic and transcriptional data reveals metabolic modules that regulate macrophage polarization. , 2015, Immunity.

[20] R. Dantzer,et al. From inflammation to sickness and depression: when the immune system subjugates the brain , 2008, Nature Reviews Neuroscience.

[21] Maxim N. Artyomov,et al. Type 1 Interferons Induce Changes in Core Metabolism that Are Critical for Immune Function. , 2016, Immunity.

[22] M. Watford. The urea cycle: Teaching intermediary metabolism in a physiological setting , 2003 .

[23] P. Cheng,et al. Metabolic therapy with PEG-arginase induces a sustained complete remission in immunotherapy-resistant melanoma , 2018, Journal of Hematology & Oncology.

[24] Zlatko Trajanoski,et al. Proteomic analysis of human cataract aqueous humour: Comparison of one-dimensional gel LCMS with two-dimensional LCMS of unlabelled and iTRAQ®-labelled specimens. , 2011, Journal of proteomics.

[25] Linda V. Sinclair,et al. Control of amino-acid transport by antigen receptors coordinates the metabolic reprogramming essential for T cell differentiation , 2013, Nature Immunology.

[26] R. Schreiber,et al. Metabolic Competition in the Tumor Microenvironment Is a Driver of Cancer Progression , 2015, Cell.

[27] Takla Griss,et al. Serine Is an Essential Metabolite for Effector T Cell Expansion. , 2017, Cell metabolism.

[28] E. Wherry,et al. Redefining Chronic Viral Infection , 2009, Cell.

[29] M Aguet,et al. Functional role of type I and type II interferons in antiviral defense. , 1994, Science.

[30] Amy-Joan L Ham,et al. Sample preparation and digestion for proteomic analyses using spin filters , 2005, Proteomics.

[31] Pornpimol Charoentong,et al. ClueGO: a Cytoscape plug-in to decipher functionally grouped gene ontology and pathway annotation networks , 2009, Bioinform..

[32] R. Steinman,et al. Direct Type I IFN but Not MDA5/TLR3 Activation of Dendritic Cells Is Required for Maturation and Metabolic Shift to Glycolysis after Poly IC Stimulation , 2014, PLoS biology.

[33] S. Akira,et al. Control of coronavirus infection through plasmacytoid dendritic-cell–derived type I interferon , 2007, Blood.

[34] C. Jack,et al. Alzheimer's Disease Neuroimaging Initiative , 2008 .

[35] Paul J. Hoffman,et al. Comprehensive Integration of Single-Cell Data , 2018, Cell.

[36] R. Fingerhut,et al. Kinetic mutations in argininosuccinate synthetase deficiency: characterisation and in vitro correction by substrate supplementation , 2016, Journal of Medical Genetics.

[37] Linda V. Sinclair,et al. Antigen receptor control of amino acid transport coordinates the metabolic re-programming that is essential for T cell differentiation , 2013, Nature immunology.

[38] G. Superti-Furga,et al. Superoxide Dismutase 1 Protects Hepatocytes from Type I Interferon-Driven Oxidative Damage , 2015, Immunity.

[39] Keiichiro Suzuki,et al. Metabolic shift induced by systemic activation of T cells in PD-1-deficient mice perturbs brain monoamines and emotional behavior , 2017, Nature Immunology.

[40] Y. Ilan,et al. Viral Diseases of the Liver , 2013, Liver Immunology.

[41] A. Sher,et al. Type I interferons in infectious disease , 2015, Nature Reviews Immunology.

[42] Wei Shi,et al. featureCounts: an efficient general purpose program for assigning sequence reads to genomic features , 2013, Bioinform..

[43] M. Mann,et al. L-Arginine Modulates T Cell Metabolism and Enhances Survival and Anti-tumor Activity , 2016, Cell.

[44] P. Chambon,et al. Targeted Somatic Mutagenesis in Mouse Epidermis , 2001, Hormone Research in Paediatrics.

[45] E. White,et al. Autophagy maintains tumor growth through circulating arginine , 2018, Nature.

[46] Christopher T. Jones,et al. A diverse array of gene products are effectors of the type I interferon antiviral response , 2011, Nature.

[47] Ruslan Medzhitov,et al. Evolution of Inflammatory Diseases , 2012, Current Biology.

[48] David M. Wilson,et al. Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures , 2018, Cell.

[49] Mathias Leblanc,et al. Cooperative Metabolic Adaptations in the Host Can Favor Asymptomatic Infection and Select for Attenuated Virulence in an Enteric Pathogen , 2018, Cell.

[50] F. Chisari,et al. Noncytopathic Clearance of Lymphocytic Choriomeningitis Virus from the Hepatocyte , 1999, The Journal of experimental medicine.

[51] Jacques Colinge,et al. IsobarPTM: A software tool for the quantitative analysis of post-translationally modified proteins☆ , 2013, Journal of proteomics.

[52] R. Satija,et al. Normalization and variance stabilization of single-cell RNA-seq data using regularized negative binomial regression , 2019, Genome Biology.

[53] M. Wangpaichitr,et al. Negative argininosuccinate synthetase expression in melanoma tumours may predict clinical benefit from arginine-depleting therapy with pegylated arginine deiminase , 2012, British Journal of Cancer.

[54] Michael Schuler,et al. Efficient temporally controlled targeted somatic mutagenesis in hepatocytes of the mouse , 2004, Genesis.

[55] Karl Mechtler,et al. General statistical modeling of data from protein relative expression isobaric tags. , 2011, Journal of proteome research.

[56] G. Berghe. The role of the liver in metabolic homeostasis: Implications for inborn errors of metabolism , 1991, Journal of Inherited Metabolic Disease.

[57] L. Sturman,et al. Enhanced Growth of a Murine Coronavirus in Transformed Mouse Cells , 1972, Infection and immunity.

[58] Y. Leung,et al. Pegylated recombinant human arginase (rhArg-peg5,000mw) inhibits the in vitro and in vivo proliferation of human hepatocellular carcinoma through arginine depletion. , 2007, Cancer research.

[59] J. Nicholson,et al. Metabolic phenotyping and systems biology approaches to understanding metabolic syndrome and fatty liver disease. , 2014, Gastroenterology.

[60] R. Sun,et al. Limiting Cholesterol Biosynthetic Flux Spontaneously Engages Type I IFN Signaling , 2015, Cell.

[61] Ruslan Medzhitov,et al. Homeostasis, Inflammation, and Disease Susceptibility , 2015, Cell.

[62] J. Fox,et al. Argininosuccinate Synthetase Is a Functional Target for a Snake Venom Anti-hypertensive Peptide , 2009, The Journal of Biological Chemistry.

[63] P. Kubes,et al. Immune surveillance by the liver , 2013, Nature Immunology.

[64] B. Gao,et al. Hepatocytes: a key cell type for innate immunity , 2015, Cellular and Molecular Immunology.

[65] Sung Woo Kim,et al. Arginine metabolism and nutrition in growth, health and disease , 2009, Amino Acids.

[66] A. Gropman,et al. Urea Cycle Disorders Overview , 2015 .

[67] I. Amit,et al. Single-cell spatial reconstruction reveals global division of labor in the mammalian liver , 2016, Nature.

[68] E. Wherry,et al. Immune Memory and Exhaustion: Clinically Relevant Lessons from the LCMV Model. , 2015, Advances in experimental medicine and biology.

[69] Russell G. Jones,et al. Enhancing CD8 T-cell memory by modulating fatty acid metabolism , 2009, Nature.

[70] Le Li,et al. p53 regulation of ammonia metabolism through urea cycle controls polyamine biosynthesis , 2019, Nature.

[71] Percy A. Knolle,et al. Living in the liver: hepatic infections , 2012, Nature Reviews Immunology.

[72] Ying Jiang,et al. A proton nuclear magnetic resonance metabonomics approach for biomarker discovery in nonalcoholic fatty liver disease. , 2011, Journal of proteome research.

[73] E. Pearce,et al. Metabolic pathways in immune cell activation and quiescence. , 2013, Immunity.

[74] Alexander Lercher,et al. CD8+ T cells induce cachexia during chronic viral infection , 2019, Nature Immunology.

[75] E. Ruppin,et al. Diversion of aspartate in ASS1-deficient tumors fosters de novo pyrimidine synthesis , 2015, Nature.

[76] R. Chamuleau,et al. Nitrogen metabolism and ornithine cycle function. , 1990, Physiological reviews.

[77] Gabi Kastenmüller,et al. Targeted metabolomics and medication classification data from participants in the ADNI1 cohort , 2017, Scientific Data.

[78] P. Murray,et al. Proliferating Helper T Cells Require Rictor/mTORC2 Complex to Integrate Signals from Limiting Environmental Amino Acids* , 2016, The Journal of Biological Chemistry.

[79] R. Medzhitov,et al. An evolutionary perspective on immunometabolism , 2019, Science.

[80] Susumu Goto,et al. KEGG: Kyoto Encyclopedia of Genes and Genomes , 2000, Nucleic Acids Res..

[81] Charity W. Law,et al. voom: precision weights unlock linear model analysis tools for RNA-seq read counts , 2014, Genome Biology.

[82] B. Rehermann,et al. The liver as an immunological organ , 2006, Hepatology.

[83] I. N. Crispe,et al. Hepatocytes as Immunological Agents , 2016, The Journal of Immunology.

[84] D. Shawcross,et al. Systemic inflammation and ammonia in hepatic encephalopathy , 2012, Metabolic Brain Disease.

[85] M. Mann,et al. Parts per Million Mass Accuracy on an Orbitrap Mass Spectrometer via Lock Mass Injection into a C-trap*S , 2005, Molecular & Cellular Proteomics.

[86] E. Pearce,et al. Immunometabolism governs dendritic cell and macrophage function , 2016, The Journal of experimental medicine.

[87] D. Adams,et al. Systemic Viral Infections and Collateral Damage in the Liver , 2006, The American Journal of Pathology.

[88] B. Rehermann,et al. Immunology of hepatitis B virus and hepatitis C virus infection , 2005, Nature Reviews Immunology.

[89] T. Junt,et al. Type I interferons directly regulate lymphocyte recirculation and cause transient blood lymphopenia. , 2006, Blood.

[90] Linda V. Sinclair,et al. Metabolic regulation of hepatitis B immunopathology by myeloid-derived suppressor cells , 2015, Nature Medicine.

[91] G. von Heijne,et al. Tissue-based map of the human proteome , 2015, Science.