Monoclonal TCR-redirected tumor cell killing
Author(s) -
Nathaniel Liddy,
Giovanna Bossi,
Katherine J. Adams,
Anna Lissina,
Tara Mahon,
Namir J. Hassan,
Jessie Gavarret,
Frayne Bianchi,
Nicholas J. Pumphrey,
Kristin Ladell,
Emma Gostick,
Andrew K. Sewell,
Nikolai Lissin,
Naomi E. Harwood,
Peter Molloy,
Yang Li,
Brian Cameron,
Malkit Sami,
Emma Baston,
Penio Todorov,
Samantha Paston,
Rebecca Dennis,
Jane Harper,
Steven M. Dunn,
Rebecca Ashfield,
A. Johnson,
Yvonne McGrath,
Gabriela Plesa,
Carl H. June,
Michael Kalos,
David A. Price,
Annelise Vuidepot,
Daniel Williams,
Deborah H. Sutton,
Bent K. Jakobsen
Publication year - 2012
Publication title -
nature medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 19.536
H-Index - 547
eISSN - 1546-170X
pISSN - 1078-8956
DOI - 10.1038/nm.2764
Subject(s) - monoclonal antibody , t cell receptor , epitope , t cell , immunotherapy , cancer research , immune system , cancer immunotherapy , biology , streptamer , cancer cell , cd3 , immunology , cancer , antigen , antibody , cd8 , genetics
T cell immunity can potentially eradicate malignant cells and lead to clinical remission in a minority of patients with cancer. In the majority of these individuals, however, there is a failure of the specific T cell receptor (TCR)–mediated immune recognition and activation process. Here we describe the engineering and characterization of new reagents termed immune-mobilizing monoclonal TCRs against cancer (ImmTACs). Four such ImmTACs, each comprising a distinct tumor-associated epitope-specific monoclonal TCR with picomolar affinity fused to a humanized cluster of differentiation 3 (CD3)-specific single-chain antibody fragment (scFv), effectively redirected T cells to kill cancer cells expressing extremely low surface epitope densities. Furthermore, these reagents potently suppressed tumor growth in vivo. Thus, ImmTACs overcome immune tolerance to cancer and represent a new approach to tumor immunotherapy.
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