A mutated intron sequence codes for an antigenic peptide recognized by cytolytic T lymphocytes on a human melanoma.
PG Coulie, F Lehmann, B Lethe… - Proceedings of the …, 1995 - National Acad Sciences
PG Coulie, F Lehmann, B Lethe, J Herman, C Lurquin, M Andrawiss, T Boon
Proceedings of the National Academy of Sciences, 1995•National Acad SciencesWe have identified an antigen recognized on a human melanoma by autologous cytolytic T
lymphocytes. It is encoded by a gene that is expressed in many normal tissues. Remarkably,
the sequence coding for the antigenic peptide is located across an exon-intron junction. A
point mutation is present in the intron that generates an amino acid change that is essential
for the recognition of the peptide by the anti-tumor cytotoxic T lymphocytes. This observation
suggests that the T-cell-mediated surveillance of the integrity of the genome may extend to …
lymphocytes. It is encoded by a gene that is expressed in many normal tissues. Remarkably,
the sequence coding for the antigenic peptide is located across an exon-intron junction. A
point mutation is present in the intron that generates an amino acid change that is essential
for the recognition of the peptide by the anti-tumor cytotoxic T lymphocytes. This observation
suggests that the T-cell-mediated surveillance of the integrity of the genome may extend to …
We have identified an antigen recognized on a human melanoma by autologous cytolytic T lymphocytes. It is encoded by a gene that is expressed in many normal tissues. Remarkably, the sequence coding for the antigenic peptide is located across an exon-intron junction. A point mutation is present in the intron that generates an amino acid change that is essential for the recognition of the peptide by the anti-tumor cytotoxic T lymphocytes. This observation suggests that the T-cell-mediated surveillance of the integrity of the genome may extend to some intronic regions.
National Acad Sciences