Cutting edge: MHC class II-restricted peptides containing the inflammation-associated marker 3-nitrotyrosine evade central tolerance and elicit a robust cell-mediated immune response

Nitrotyrosine is widely recognized as a surrogate marker of up-regulated inducible NO synthase expression at sites of inflammation. However, the potential immunogenicity Of autologous proteins containing nitrotyrosine has not previously been investigated. Herein, we used the I-E-K-restricted T cell epitope of pigeon/moth cytochrome c PCC/MCC88-103) to assess the ability of T cells to recognize ligands containing nitrotyrosine. Substitution of the single tyrosine (Y97) in PCC/MCC88-103 with nitrotyrosine abrogates recognition by the MCC88-103-specific T cell hybridoma 2B4. CBA (H2(K)) mice immunized with MCC88-103 or nitrated MCC88-103 peptides produce T cell responses that are mutually exclusive. Transgenic mice that constitutively express PCC under the control of an MHC class I promoter are tolerant toward immunization with MCC88-103 but exhibited a robust immune response against nitrated MCC88-103. Analysis of T cell hybridomas specific for nitrated-MCC88-103 indicated that subtle differences in TCR VDJ gene usage are sufficient to allow nitrotyrosine-specific T cells to escape the processes of central tolerance.