1
Tokai University, Japan.
2
University of Tokyo, Japan.
3
National Institute of Infectious Diseases, Japan.
4
Soka University, Japan.
PMID: 32651230 DOI: 10.1074/jbc.RA120.014317
Abstract
Hepatitis B, a viral infection that affects the liver, is thought to affect over 257 million people worldwide, and long-term infection can lead to life-threatening issues such as cirrhosis or liver cancer. Chronic hepatitis B develops by the interaction between Hepatitis B virus (HBV) and host immune response. However, questions of how HBV-infected cells thwart immune system defenses remain unanswered. Extracellular vesicles (EVs) are used for cellular communication, carrying cargoes such as RNAs, proteins and lipids and delivering them intracellularly after being endocytosed by target cells. HBV-infected liver cells secrete several types of EVs into body fluids such as complete and incomplete virions, and exosomes. We previously demonstrated that monocytes that incorporated EVs moved to immunoregulatory phenotypes via upregulation of PD-L1, an immunocheckpoint molecule, and downregulation of CD69, a leukocyte activation molecule. In this study, we transfected mice with HBV using hydrodynamic injection and studied the effects of EVs secreted by HBV-infected liver cells. EVs secreted from cells with HBV replication strongly suppressed the immune response, inhibiting the eradication of HBV-replicating cells in the mice transfected with HBV. EVs were systemically incorporated in multiple organs, including liver, bone marrow (BM) and intestine. Intriguingly, the BM cells which incorporated EVs acquired intestinal tropism and the dendritic cell populations in the intestine increased. These findings suggest that the EVs secreted by HBV-infected liver cells exert immunosuppressive functions, and that an association between the liver, bone marrow and intestinal tract exists through EVs secreted from HBV-infected cells.
Keywords: PD-L1; dendritic cell; extracellular vesicles; hepatitis B virus (HBV, Hep B); hydrodynamic HBV transfection mouse model; immunosuppression; viral immunology.
Published under license by The American Society for Biochemistry and Molecular Biology, Inc. 作者: StephenW 时间: 2020-7-12 15:31