Consensus nomenclature for CD8 + T cell phenotypes in cancer

Apetoh, L.; Smyth, M.J.; Drake, C.G.; Abastado, J.P.; Apte, R.N.; Ayyoub, M.; Blay, J.Y.; Bonneville, M.; Butterfield, L.H.; Caignard, A.; Castelli, C.; Cavallo, F.; Celis, E.; Chen, L.; Colombo, M.P.; Comin-Anduix, B.; Coukos, G.; Dhodapkar, M.V.; Dranoff, G.; Frazer, I.H.; Fridman, W.H.; Gabrilovich, D.I.; Gilboa, E.; Gnjatic, S.; Jäger, D.; Kalinski, P.; Kaufman, H.L.; Kiessling, R.; Kirkwood, J.; Knuth, A.; Liblau, R.; Lotze, M.T.; Lugli, E.; Marincola, F.; Melero, I.; Melief, C.J.; Mempel, T.R.; Mittendorf, E.A.; Odun, K.; Overwijk, W.W.; Palucka, A.K.; Parmiani, G.; Ribas, A.; Romero, P.; Schreiber, R.D.; Schuler, G.; Srivastava, P.K.; Tartour, E.; Valmori, D.; van der Burg, S.H.; van der Bruggen, P.; van den Eynde, B.J.; Wang, E.; Zou, W.; Whiteside, T.L.; Speiser, D.E.; Pardoll, D.M.; Restifo, N.P.; Anderson, A.C.

doi:10.1080/2162402X.2014.998538

Consensus nomenclature for CD8 + T cell phenotypes in cancer

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Serval ID

serval:BIB_D1DB47249851

Type

Article: article from journal or magazin.

Publication sub-type

Review (review): journal as complete as possible of one specific subject, written based on exhaustive analyses from published work.

Collection

Publications

Institution

UNIL/CHUV

Title

Consensus nomenclature for CD8 + T cell phenotypes in cancer

Journal

Oncoimmunology

Author(s)

Apetoh L., Smyth M.J., Drake C.G., Abastado J.P., Apte R.N., Ayyoub M., Blay J.Y., Bonneville M., Butterfield L.H., Caignard A., Castelli C., Cavallo F., Celis E., Chen L., Colombo M.P., Comin-Anduix B., Coukos G., Dhodapkar M.V., Dranoff G., Frazer I.H., Fridman W.H., Gabrilovich D.I., Gilboa E., Gnjatic S., Jäger D., Kalinski P., Kaufman H.L., Kiessling R., Kirkwood J., Knuth A., Liblau R., Lotze M.T., Lugli E., Marincola F., Melero I., Melief C.J., Mempel T.R., Mittendorf E.A., Odun K., Overwijk W.W., Palucka A.K., Parmiani G., Ribas A., Romero P., Schreiber R.D., Schuler G., Srivastava P.K., Tartour E., Valmori D., van der Burg S.H., van der Bruggen P., van den Eynde B.J., Wang E., Zou W., Whiteside T.L., Speiser D.E., Pardoll D.M., Restifo N.P., Anderson A.C.

ISSN

2162-4011 (Print)
2162-402X (Electronic)

ISSN-L

2162-4011

Publication state

Published

Issued date

2015

Peer-reviewed

Oui

Volume

Number

Pages

e998538

Language

english

Notes

Publication types: Point of View ; research-article Identifiant PubMed Central: PMC4485711

Abstract

Whereas preclinical investigations and clinical studies have established that CD8(+) T cells can profoundly affect cancer progression, the underlying mechanisms are still elusive. Challenging the prevalent view that the beneficial effect of CD8(+) T cells in cancer is solely attributable to their cytotoxic activity, several reports have indicated that the ability of CD8(+) T cells to promote tumor regression is dependent on their cytokine secretion profile and their ability to self-renew. Evidence has also shown that the tumor microenvironment can disarm CD8(+) T cell immunity, leading to the emergence of dysfunctional CD8(+) T cells. The existence of different types of CD8(+) T cells in cancer calls for a more precise definition of the CD8(+) T cell immune phenotypes in cancer and the abandonment of the generic terms "pro-tumor" and "antitumor." Based on recent studies investigating the functions of CD8(+) T cells in cancer, we here propose some guidelines to precisely define the functional states of CD8(+) T cells in cancer.

Keywords

anergy, anticancer immunity, CD8 + T cells, cytotoxicity, exhaustion, effector, IFNγ, senescence, stemness

OAI-PMH

oai:serval.unil.ch:BIB_D1DB47249851

DOI

10.1080/2162402X.2014.998538

Pubmed

26137416

Web of science

000354224400020

Open Access

Yes