Characterization of circulating T cells specific for tumor-associated antigens in melanoma patients

P P Lee; C Yee; P A Savage; L Fong; D Brockstedt; J S Weber; D Johnson; S Swetter; J Thompson; P D Greenberg; M Roederer; M M Davis

doi:10.1038/9525

Characterization of circulating T cells specific for tumor-associated antigens in melanoma patients

Nat Med. 1999 Jun;5(6):677-85. doi: 10.1038/9525.

Authors

P P Lee¹, C Yee, P A Savage, L Fong, D Brockstedt, J S Weber, D Johnson, S Swetter, J Thompson, P D Greenberg, M Roederer, M M Davis

Affiliation

¹ Howard Hughes Medical Institute/Department of Microbiology and Immunology, Stanford University, California 94305, USA.

PMID: 10371507
DOI: 10.1038/9525

Abstract

We identified circulating CD8+ T-cell populations specific for the tumor-associated antigens (TAAs) MART-1 (27-35) or tyrosinase (368-376) in six of eleven patients with metastatic melanoma using peptide/HLA-A*0201 tetramers. These TAA-specific populations were of two phenotypically distinct types: one, typical for memory/effector T cells; the other, a previously undescribed phenotype expressing both naive and effector cell markers. This latter type represented more than 2% of the total CD8+ T cells in one patient, permitting detailed phenotypic and functional analysis. Although these cells have many of the hallmarks of effector T cells, they were functionally unresponsive, unable to directly lyse melanoma target cells or produce cytokines in response to mitogens. In contrast, CD8+ T cells from the same patient were able to lyse EBV-pulsed target cells and showed robust allogeneic responses. Thus, the clonally expanded TAA-specific population seems to have been selectively rendered anergic in vivo. Peptide stimulation of the TAA-specific T-cell populations in other patients failed to induce substantial upregulation of CD69 expression, indicating that these cells may also have functional defects, leading to blunted activation responses. These data demonstrate that systemic TAA-specific T-cell responses can develop de novo in cancer patients, but that antigen-specific unresponsiveness may explain why such cells are unable to control tumor growth.

Publication types

Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, P.H.S.

MeSH terms

Antigens, Neoplasm / immunology
Antigens, Neoplasm / metabolism*
Antineoplastic Agents / therapeutic use
CD28 Antigens / immunology
CD28 Antigens / metabolism
CD57 Antigens / immunology
CD57 Antigens / metabolism
CD8-Positive T-Lymphocytes / immunology
Female
Flow Cytometry / methods
HLA-A2 Antigen / genetics
HLA-A2 Antigen / immunology
Humans
Hyaluronan Receptors / immunology
Hyaluronan Receptors / metabolism
Leukocyte Common Antigens / immunology
Leukocyte Common Antigens / metabolism
Lymphatic Metastasis / immunology
Lymphatic Metastasis / pathology
MART-1 Antigen
Melanoma / drug therapy
Melanoma / immunology*
Melanoma / pathology*
Melanoma / secondary
Membrane Glycoproteins / genetics
Membrane Glycoproteins / immunology
Monophenol Monooxygenase / genetics
Monophenol Monooxygenase / immunology
Neoplasm Proteins / genetics
Neoplasm Proteins / immunology
Peptide Fragments / genetics
Peptide Fragments / immunology
Receptors, IgG / immunology
Receptors, IgG / metabolism
Recombinant Proteins / genetics
Recombinant Proteins / immunology
T-Lymphocytes / immunology*
gp100 Melanoma Antigen

Substances

Antigens, Neoplasm
Antineoplastic Agents
CD28 Antigens
CD57 Antigens
HLA-A2 Antigen
Hyaluronan Receptors
MART-1 Antigen
MLANA protein, human
Membrane Glycoproteins
Neoplasm Proteins
PMEL protein, human
Peptide Fragments
Receptors, IgG
Recombinant Proteins
gp100 Melanoma Antigen
Monophenol Monooxygenase
Leukocyte Common Antigens

Abstract

Publication types

MeSH terms

Substances

Grants and funding