1. Pre-existing virus-specific CD8+ T-cells provide protection against pneumovirus-induced disease in mice
- Author
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Claire J. P. Boog, Peter J.S. van Kooten, Andrew J. Easton, Alice J. A. M. Sijts, Andrea Gröne, Dietmar M. W. Zaiss, Cornelis P. J. Bekker, Mary J. van Helden, David J. Topham, and Dirk H. Busch
- Subjects
BM-DC, bone marrow derived DC ,CD8-Positive T-Lymphocytes ,Epitope ,Mice ,DC, dendritic cell ,0302 clinical medicine ,DCp, peptide-loaded DC ,Cytotoxic T cell ,Pneunomia virus of mice ,p.i., post infection ,Mice, Inbred BALB C ,0303 health sciences ,Pneumovirus ,i.p., intraperitoneal ,Adoptive Transfer ,Respiratory Syncytial Viruses ,SEM, standard error of mean ,3. Good health ,Killer Cells, Natural ,FI, formalin inactivated ,hRSV, human respiratory syncytial virus ,MLN, mediastinal lymph node ,Pneumoviruses ,Infectious Diseases ,Molecular Medicine ,Female ,BAL, bronchoalveolar lavage ,NK, natural killer ,Murine pneumonia virus ,Biology ,Article ,Virus ,Interferon-gamma ,03 medical and health sciences ,i.v., intravenous ,Immunology and Microbiology(all) ,parasitic diseases ,Animals ,Pneumovirus Infections ,NK cell ,030304 developmental biology ,QR355 ,ID, infectious dose ,General Veterinary ,General Immunology and Microbiology ,NS, nonstructural ,Influenza A Virus, H3N2 Subtype ,Public Health, Environmental and Occupational Health ,EID, egg ID ,i.n., intranasal ,pfu, plaque forming units ,Dendritic cell ,veterinary(all) ,Virology ,Immunology ,Pneumovirus vaccine ,Interleukin-4 ,PVM, pneunomia virus of mice ,CD8+ T-cell ,BALF, BAL fluid ,Immunologic Memory ,Vaccine ,CD8 ,030215 immunology - Abstract
Highlights ► NK cells and CD8+ T-cells expand relatively late following pneumovirus infection. ► Memory CD8+ T-cells support type 1 skewing of pneumovirus-specific responses. ► Memory CD8+ T-cells prevent pneumovirus-induced immunopathology. ► CD8+ T-cell targeted immunization protects against pneumovirus-induced disease., Pneumoviruses such as pneumonia virus of mice (PVM), bovine respiratory syncytial virus (bRSV) or human (h)RSV are closely related pneumoviruses that cause severe respiratory disease in their respective hosts. It is well-known that T-cell responses are essential in pneumovirus clearance, but pneumovirus-specific T-cell responses also are important mediators of severe immunopathology. In this study we determined whether memory- or pre-existing, transferred virus-specific CD8+ T-cells provide protection against PVM-induced disease. We show that during infection with a sublethal dose of PVM, both natural killer (NK) cells and CD8+ T-cells expand relatively late. Induction of CD8+ T-cell memory against a single CD8+ T-cell epitope, by dendritic cell (DC)-peptide immunization, leads to partial protection against PVM challenge and prevents Th2 differentiation of PVM-induced CD4 T-cells. In addition, adoptively transferred PVM-specific CD8+ T-cells, covering the entire PVM-specific CD8+ T-cell repertoire, provide partial protection from PVM-induced disease. From these data we infer that antigen-specific memory CD8+ T-cells offer significant protection to PVM-induced disease. Thus, CD8+ T-cells, despite being a major cause of PVM-associated pathology during primary infection, may offer promising targets of a protective pneumovirus vaccine.
- Published
- 2012
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