ABSTRACT
Hepatitis C virus-mediated immune suppression is an underlying feature leading to the establishment of viral persistence and chronic infection. In particular, HCV core protein has been shown to exhibit significant immunosuppressive activity of T cells and antigen presenting cells. Using an HCV core transgenic mouse system, in which liver hepatocytes express core protein, it is possible to study the effects of core-mediated immune suppression in vivo during viral infection. In this protocol, we describe the procedures for evaluating antigen-specific CD8+ T cell responses in response to recombinant adenovirus infection in HCV core transgenic mice.
Subject(s)
CD8-Positive T-Lymphocytes/immunology , Hepacivirus/immunology , Hepatitis C/immunology , Adenoviridae/genetics , Animals , Cell Separation/instrumentation , Cell Separation/methods , Centrifugation, Density Gradient/instrumentation , Centrifugation, Density Gradient/methods , Flow Cytometry/instrumentation , Flow Cytometry/methods , Genetic Vectors/genetics , Hepatitis C/virology , Hepatocytes , Leukocytes, Mononuclear , Liver/cytology , Liver/immunology , Liver/virology , Mice , Mice, Transgenic , Primary Cell Culture/instrumentation , Primary Cell Culture/methods , Transduction, Genetic/instrumentation , Transduction, Genetic/methods , Viral Core Proteins/immunologyABSTRACT
The liver maintains an immunologically tolerant environment as a result of continuous exposure to food and bacterial constituents from the digestive tract. Hepatotropic pathogens can take advantage of this niche and establish lifelong chronic infections causing hepatic fibrosis and hepatocellular carcinoma. Macrophages (MÏ) play a critical role in regulation of immune responses to hepatic infection and regeneration of tissue. However, the factors crucial for MÏ in limiting hepatic inflammation or resolving liver damage have not been fully understood. In this report, we demonstrate that expression of C-type lectin receptor scavenger receptor-AI (SR-AI) is crucial for promoting M2-like MÏ activation and polarization during hepatic inflammation. Liver MÏ uniquely up-regulated SR-AI during hepatotropic viral infection and displayed increased expression of alternative MÏ activation markers, such as YM-1, arginase-1, and interleukin-10 by activation of mer receptor tyrosine kinase associated with inhibition of mammalian target of rapamycin. Expression of these molecules was reduced on MÏ obtained from livers of infected mice deficient for the gene encoding SR-AI (msr1). Furthermore, in vitro studies using an SR-AI-deficient MÏ cell line revealed impeded M2 polarization and decreased phagocytic capacity. Direct stimulation with virus was sufficient to activate M2 gene expression in the wild-type (WT) cell line, but not in the knockdown cell line. Importantly, tissue damage and fibrosis were exacerbated in SR-AI-/- mice following hepatic infection and adoptive transfer of WT bone-marrow-derived MÏ conferred protection against fibrosis in these mice. CONCLUSION: SR-AI expression on liver MÏ promotes recovery from infection-induced tissue damage by mediating a switch to a proresolving MÏ polarization state. (Hepatology 2017;65:32-43).
Subject(s)
Hepatitis/etiology , Liver Cirrhosis/etiology , Macrophage Activation , Scavenger Receptors, Class A/biosynthesis , Animals , Cells, Cultured , Female , Mice , Mice, Inbred C57BLABSTRACT
Understanding of antigen-presenting cell (APC) participation in tissue inflammation and metabolism has advanced through numerous studies using systems biology approaches. Previously unrecognized connections between these research areas have been elucidated in the context of inflammatory disease involving innate and adaptive immune responses. A new conceptual framework bridges APC biology, metabolism, and cytokines in the generation of effective T-cell responses. Exploring these connections is paramount to addressing the rising tide of multi-organ system diseases, particularly chronic diseases associated with metabolic syndrome, infection, and cancer. Focused research in these areas will aid the development of strategies to harness and manipulate innate immunology to improve vaccine development, anti-viral, anti-inflammatory, and anti-tumor therapies. This review highlights recent advances in APC "immunometabolism" specifically related to chronic viral and metabolic disease in humans. The goal of this review is to develop an abridged and consolidated outlook on recent thematic updates to APC immunometabolism in the areas of regulation and crosstalk between metabolic and inflammatory signaling and the integrated stress response and how these signals dictate APC function in providing T-cell activation Signal 3.
