Abstract EN:

Human cytomegalovirus (HCMV) infects 50-100 % of the world population without overt symptoms but is pathogenic in immunosuppressed individuals. Cellular immunity plays a major role in the control of HCMV infection. Our data show potentiation of the CD4+ T cell response to a specific epitope of IE1 protein through shortening and relocation of an otherwise nuclear protein and suggest applications in vaccination. This response was due to endogenous presentation followed by exogenous presentation at later time points. Presentation was dependent on both proteasome and acidic compartments. We have also shown that although IE1-specific CD4+T cell clones were cytotoxic against peptide-pused targets, their cytotoxicity was undetectable on infected targets. The main reason for this lack of cytotocixity was found to be the selective inhibition of cytotoxicity of infected targets whereas IFN-g production was not impaired. Our data describe for the first the inhibition of cytotoxicity of CD4+ T lymphocytes against infected targets.