These studies were supported by the Crohn’s and Colitis Foundation of Canada. The authors have no conflict of interest to report with regard to this manuscript. “
“Memory cross-reactive CD8+ T-cell responses may induce protection or immunopathology upon secondary viral challenge. To elucidate the potential role of T cells in sequential flavivirus infection,
we characterized cross-reactive CD4+ and CD8+ T-cell responses between attenuated and pathogenic Japanese encephalitis virus (JEV) and pathogenic West Nile virus (WNV). A previously reported WNV NS4b CD8+ T-cell epitope and its JEV variant elicited CD8+ T-cell responses in both JEV- and WNV-infected mice. The peptide variant homologous to the immunizing virus induced greater cytokine secretion and activated higher frequencies of epitope-specific MI-503 solubility dmso Staurosporine cost CD8+ T cells. However, there was a virus-dependent, peptide variant-independent pattern of
cytokine secretion; the IFNγ+-to-IFNγ+TNFα+ CD8+ T-cell ratio was greater in JEV- than in WNV-infected mice. Despite similarities in viral burden for pathogenic WNV and JEV viruses, CD8+ T cells from pathogenic JEV-immunized mice exhibited functional and phenotypic profiles similar to those seen for the attenuated JEV strain. Patterns of killer cell lectin-like receptor G1 (KLRG1) and CD127 expression differed by virus type, with a rapid expansion and contraction of short-lived effector cells in JEV infection and persistence of high levels of short-lived effector cells in WNV infection. Such cross-reactive T-cell responses to primary infection may affect the outcomes of sequential flavivirus infections. The arthropod-borne Flaviviruses co-circulate in different geographic regions worldwide and include important human pathogens. The Japanese encephalitis serogroup includes Japanese encephalitis virus (JEV), the leading cause of viral encephalitis among children in Southeast Asia, and West Nile virus (WNV), which causes neuroinvasive disease in adults in temperate regions 1. A live-attenuated JEV vaccine, SA14-14-2,
has been licensed in China, but currently, there is no licensed WNV vaccine Urocanase for humans 2. The flavivirus genome encodes three structural (C, prM, envelope (E)) and seven nonstructural genes (NS1, NS2a, NS2b, NS3, NS4a, NS4b, NS5). Both the humoral and cellular arms of the immune system are vital to protect mice from JEV and WNV encephalitis 3–6. Protective CD8+ and CD4+ T-cell epitopes residing in the WNV NS4b and NS3 proteins, respectively, play an important antiviral role through cytokine production and cytotoxic activity 7–9. Heterologous immunity to related or unrelated viral pathogens induces protection or immunopathology upon a secondary viral challenge due to cross-reactive memory CD8+ T-cell responses 10, 11.