Human breast tumor-infiltrating CD8+ T cells retain polyfunctionality despite PD-1 expression

Colt A. Egelston; Christian Avalos; Travis Y. Tu; Diana L. Simons; Grecia Jimenez; Jae Yoon Jung; Laleh G. Melstrom; Kim Margolin; John H. Yim; Laura Kruper; Joanne Mortimer; Peter P. Lee

doi:10.1038/s41467-018-06653-9

Human breast tumor-infiltrating CD8+ T cells retain polyfunctionality despite PD-1 expression

Colt A. Egelston(City of Hope), Christian Avalos(City of Hope), Travis Y. Tu(City of Hope), Diana L. Simons(City of Hope), Grecia Jimenez(City of Hope), Jae Yoon Jung(Norton Healthcare), Laleh G. Melstrom(City of Hope), Kim Margolin(City of Hope), John H. Yim(City of Hope), Laura Kruper(City of Hope), Joanne Mortimer(City of Hope), Peter P. Lee(City Of Hope National Medical Center)

Nature Communications

October 10, 2018

10.1038/s41467-018-06653-9

Cited by 125Open Access

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Abstract

Abstract Functional CD8 + T cells in human tumors play a clear role in clinical prognosis and response to immunotherapeutic interventions. PD-1 expression in T cells involved in chronic infections and tumors such as melanoma often correlates with a state of T-cell exhaustion. Here we interrogate CD8 + tumor-infiltrating lymphocytes (TILs) from human breast and melanoma tumors to explore their functional state. Despite expression of exhaustion hallmarks, such as PD-1 expression, human breast tumor CD8 + TILs retain robust capacity for production of effector cytokines and degranulation capacity. In contrast, melanoma CD8 + TILs display dramatic reduction of cytokine production and degranulation capacity. We show that CD8 + TILs from human breast tumors can potently kill cancer cells via bi-specific antibodies. Our data demonstrate that CD8 + TILs in human breast tumors retain polyfunctionality, despite PD-1 expression, and suggest that they may be harnessed for effective immunotherapies.

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