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Exploiting the glioblastoma peptidome to discover novel tumour-associated antigens for immunotherapy
Author(s) -
Valérie Dutoit,
Christel HeroldMende,
Norbert Hilf,
Oliver Schoor,
Philipp Beckhove,
Judith Bucher,
Katharina Dorsch,
Sylvia Flohr,
Jens Fritsche,
Peter Lewandrowski,
Jennifer Lohr,
HansGeorg Rammensee,
Stefan Stevanović,
Claudia Trautwein,
Verona Vass,
Steffen Walter,
Paul R. Walker,
Toni Weinschenk,
Harpreet SinghJasuja,
PierreYves Dietrich
Publication year - 2012
Publication title -
brain
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.142
H-Index - 336
eISSN - 1460-2156
pISSN - 0006-8950
DOI - 10.1093/brain/aws042
Subject(s) - glioblastoma , immunotherapy , antigen , cancer immunotherapy , computational biology , medicine , cancer research , immunology , biology , immune system
Peptides presented at the cell surface reflect the protein content of the cell; those on HLA class I molecules comprise the critical peptidome elements interacting with CD8 T lymphocytes. We hypothesize that peptidomes from ex vivo tumour samples encompass immunogenic tumour antigens. Here, we uncover >6000 HLA-bound peptides from HLA-A*02(+) glioblastoma, of which over 3000 were restricted by HLA-A*02. We prioritized in-depth investigation of 10 glioblastoma-associated antigens based on high expression in tumours, very low or absent expression in healthy tissues, implication in gliomagenesis and immunogenicity. Patients with glioblastoma showed no T cell tolerance to these peptides. Moreover, we demonstrated specific lysis of tumour cells by patients' CD8(+) T cells in vitro. In vivo, glioblastoma-specific CD8(+) T cells were present at the tumour site. Overall, our data show the physiological relevance of the peptidome approach and provide a critical advance for designing a rational glioblastoma immunotherapy. The peptides identified in our study are currently being tested as a multipeptide vaccine (IMA950) in patients with glioblastoma.

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