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Novel HLA-A2-restricted human metapneumovirus epitopes reduce viral titers in mice and are recognized by human T cells
Affiliation:1. Sultan Abdulhamid Han Training and Research Hospital, Department of Cardiology, Istanbul, Turkey;2. Dr. Siyami Ersek Thoracic and Cardiovascular Surgery Center, Training and Research Hospital, Department of Cardiology, Istanbul, Turkey;3. Duzce University, Department of Cardiology, Duzce, Turkey;4. Texas A&M University, Department of Cardiology, TX, USA;5. Urla State Hospital, Urla, Izmir, Turkey;6. Yeshiva University, Albert Einstein College of Medicine, Montefiore Medical Center, Department of Allergy/Immunology, Bronx, New York, USA;7. Dortyol State Hospital, Department of Cardiology, Dortyol, Hatay, Turkey
Abstract:Human metapneumovirus (HMPV) is a major cause of morbidity and mortality from acute lower respiratory tract illness, with most individuals seropositive by age five. Despite the presence of neutralizing antibodies, secondary infections are common and can be severe in young, elderly, and immunocompromised persons. Preclinical vaccine studies for HMPV have suggested a need for a balanced antibody and T cell immune response to enhance protection and avoid lung immunopathology. We infected transgenic mice expressing human HLA-A*0201 with HMPV and used ELISPOT to screen overlapping and predicted epitope peptides. We identified six novel HLA-A2 restricted CD8+ T cell (TCD8) epitopes, with M39–47 (M39) immunodominant. Tetramer staining detected M39-specific TCD8 in lungs and spleen of HMPV-immune mice. Immunization with adjuvant-formulated M39 peptide reduced lung virus titers upon challenge. Finally, we show that TCD8 from HLA-A*0201 positive humans recognize M39 by IFNγ ELISPOT and tetramer staining. These results will facilitate HMPV vaccine development and human studies.
Keywords:Human metapneumovirus  Paramyxovirus  Vaccine  T cell response  Respiratory infections
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