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Citations to this article

Tumor escape from immune recognition: lethal recurrent melanoma in a patient associated with downregulation of the peptide transporter protein TAP-1 and loss of expression of the immunodominant MART-1/Melan-A antigen.
M J Maeurer, … , W J Storkus, M T Lotze
M J Maeurer, … , W J Storkus, M T Lotze
Published October 1, 1996
Citation Information: J Clin Invest. 1996;98(7):1633-1641. https://doi.org/10.1172/JCI118958.
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Tumor escape from immune recognition: lethal recurrent melanoma in a patient associated with downregulation of the peptide transporter protein TAP-1 and loss of expression of the immunodominant MART-1/Melan-A antigen.

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Abstract

In the last few years, mutiple protein target antigens for immunorecognition by T cells have been identified on human melanoma. How melanoma lesions escape from functional antigen-specific immune recognition remains poorly understood. We have identified the concomitant loss of the immunodominant T cell-defined MART-1/Melan-A antigen and downregulation of the TAP-1 gene in a recurrent metastatic melanoma that was resected in 1993. This phenotype was not observed for an earlier autologous melanoma lesion resected in 1987. The "antigen loss" could be restored in the variant tumor cell line by simultaneously providing both the MART-1/Melan-A gene (by retroviral transfer) and the TAP-1 gene (by a bioballistic approach) resulting in tumor cell sensitivity to MART-1/Melan-A-specific cytotoxic T lymphocytes. This suggests that tumor escape from immune surveillance may have occurred in vivo as a sequential result of (a) antigen loss, and (b) downregulation of the peptide-transporter protein TAP-1 expression by this patient's tumor over a 6-yr period from 1987 to 1993. These results suggest that the characterization of the T cell response to melanoma in individual patients and definition of the immunologically relevant genetic defects in tumors may be required to select the most effective therapeutic strategies for a given patient.

Authors

M J Maeurer, S M Gollin, D Martin, W Swaney, J Bryant, C Castelli, P Robbins, G Parmiani, W J Storkus, M T Lotze

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Expression of melanoma-associated antigens in melanoma cell cultures
M Urosevic, B Braun, J Willers, G Burg, R Dummer
Experimental Dermatology 2005
Generation of RAGE-1 and MAGE-9 peptide-specific cytotoxic T-Lymphocyte lines for transfer in patients with renal cell carcinoma
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Melanocyte-specific, cytotoxic T cell responses in vitiligo: the effective variant of melanoma immunity?
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Pigment Cell Research 2005
Sequential Immune Escape and Shifting of T Cell Responses in a Long-Term Survivor of Melanoma
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Journal of immunology (Baltimore, Md. : 1950) 2005
Identification of multiple antigens recognized by tumor-infiltrating lymphocytes from a single patient: tumor escape by antigen loss and loss of MHC expression
HT Khong, QJ Wang, SA Rosenberg
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The promise of cancer vaccines
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Role of TAP-1 and/or TAP-2 antigen presentation defects in tumorigenicity of mouse melanoma
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Cellular Immunology 2004
Competition Among Peptides in Melanoma Vaccines for Binding to MHC Molecules
LW Thompson, CF Garbee, S Hibbitts, LH Brinckerhoff, RA Pierce, KA Chianese-Bullock, DH Deacon, VH Engelhard, CL Slingluff
Journal of Immunotherapy 2004
B cell chronic lymphocytic leukaemia cells have reduced capacity to upregulate expression of MHC class I in response to interferon-γ
H Juffs, N Fowler, R Saal, K Grimmett, S Beasley, B O'Sullivan, I Frazer, D Gill, R Thomas
Pathology 2004
Handbook of Cancer Vaccines
MA Morse, TM Clay, HK Lyerly
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Escape from immunotherapy: possible mechanisms that influence tumor regression/progression
Ahmad M, Rees RC, Ali SA
Cancer Immunology, Immunotherapy 2004
Chronic myelogenous leukemia shapes host immunity by selective deletion of high avidity leukemia-specific T-cells
Jeffrey J. Molldrem, Peter P. Lee, Shreya Kant, Eric Wieder, Weidong Jiang, Sijie Lu, Changqing Wang and Mark M. Davis
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Therapeutic vaccination with tumor cells that engage CD137
KE Hellstrom, I Hellstrom
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Association of TAP1 downregulation in human primary melanoma lesions with lack of spontaneous regression
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Immunisation with modified HPV16 E7 genes against mouse oncogenic TC-1 cell sublines with downregulated expression of MHC class I molecules
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Cancer Chemotherapy and Biological Response Modifiers Annual
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Loss of antigen-processing molecules in primary orbital melanoma
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Successful elimination of large established tumors and avoidance of antigen‐loss variants by aggressive adoptive T cell immunotherapy
K Matsui, LA OMara, PM Allen
International Immunology 2003
Induction of specific antitumor immunity in the mouse with the electrofusion product of tumor cells and dendritic cells
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Molecular Therapy 2003
Membrane Transporter Diseases
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Acute Leukemias IX
W Hiddemann, T Haferlach, M Unterhalt, T Büchner, J Ritter
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Downregulation of the proteasome subunits, transporter, and antigen presentation in hepatocellular carcinoma, and their restoration by interferon-gamma
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Suppression of Macrophage Function by Substances with a Molecular Weight Lower than 3000 Da in B16 Melanoma-Conditioned Medium
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Melanoma vaccines
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Adoptive T cell therapy using antigen-specific CD8+ T cell clones for the treatment of patients with metastatic melanoma: in vivo persistence, migration, and antitumor effect of transferred T cells
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Proceedings of the National Academy of Sciences 2002
Synthetic and natural non-live vectors: rationale for their clinical development in cancer vaccine protocols
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Vaccine 2002
Royal College of Radiologists Annual Undergraduate Essay Prize Melanoma: the New Smallpox? Can Vaccines be Used to Treat Melanoma?
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MICA triggering signal for NK cell tumor lysis is counteracted by HLA-G1-mediated inhibitory signal
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Immunity to cancer: attack and escape in T lymphocyte-tumor cell interaction
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Suppressive Effect of Shichimotsu-koka-to (Kampo Medicine) on Pulmonary Metastasis of B16 Melanoma Cells
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Gene Therapy of Cancer
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Generation of CTL recognizing an HLA-A*0201-restricted epitope shared by MAGE-A1, -A2, -A3, -A4, -A6, -A10, and -A12 tumor antigens: implication in a broad-spectrum tumor immunotherapy
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Journal of immunology (Baltimore, Md. : 1950) 2002
Absence of gamma-interferon-inducible lysosomal thiol reductase in melanomas disrupts T cell recognition of select immunodominant epitopes
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Journal of Experimental Medicine 2002
Absence of γ-Interferon–inducible Lysosomal Thiol Reductase in Melanomas Disrupts T Cell Recognition of Select Immunodominant Epitopes
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Peptide Vaccines for Cancer
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Cancer Investigation 2002
Lack of ifn-?-mediated induction of the class II transactivator (CIITA) through promoter methylation is predominantly found in developmental tumor cell lines
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International Journal of Cancer 2002
Preserved IFN-? production of circulating V?24 NKT cells in primary lung cancer patients
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T-cell-directed cancer vaccines: mechanisms of immune escape and immune tolerance
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Expert Opinion on Biological Therapy 2001
Decreased Intraindividual HLA Class I Expression is due to Reduced Transcription in Advanced Melanoma and Does Not Correlate with HLA-G Expression
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Journal of Investigative Dermatology 2001
High Expression of HLA-A2 on an Oral Squamous Cell Carcinoma with Down-Regulated Transporter for Antigen Presentation
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Introduction of Tapasin Gene Restores Surface Expression of HLA Class I Molecules, but Not Antigen Presentation of an HIV Envelope Peptide in a Hepatoma Cell Line
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TAP1 down-regulation in primary melanoma lesions: An independent marker of poor prognosis
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Diverse expansion potential and heterogeneous avidity in tumor-associated antigen-specific T lymphocytes from primary melanoma patients
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Lymphocyte-mediated immunosurveillance of epithelial cancers?
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Two Cases of Melanoma with a Spontaneous Regression in Primary Lesions Showing Rapid Progressive Disease. Analysis of the Hammond Effect
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Nishi Nihon Hifuka 2001
H2-Mβ1 and H2-Mβ2 Heterodimers Equally Promote CLIP Removal in I-A q Molecules from Autoimmune-prone DBA/1 Mice
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Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene
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Minimal Residual Disease in Melanoma
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A Novel Autocrine Pathway of Tumor Escape from Immune Recognition: Melanoma Cell Lines Produce a Soluble Protein That Diminishes Expression of the Gene Encoding the Melanocyte Lineage Melan-A/MART-1 Antigen Through Down-Modulation of Its Promoter
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Tumour immunotherapy: the adjuvant treatment of the21st century?
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Evidence for cytotoxic T lymphocyte response against human lung cancer: Reconstitution of antigenic epitope with peptide eluted from lung adenocarcinoma MHC class I
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IFN-γ Can Promote Tumor Evasion of the Immune System In Vivo by Down-Regulating Cellular Levels of an Endogenous Tumor Antigen
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MART-1 Is Expressed Less Frequently on Circulating Melanoma Cells in Patients Who Develop Distant Compared With Locoregional Metastases
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