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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

被引:226
作者
Maeurer, MJ
Gollin, SM
Martin, D
Swaney, W
Bryant, J
Castelli, C
Robbins, P
Parmiani, G
Storkus, WJ
Lotze, MT
机构
[1] UNIV PITTSBURGH, MED CTR, DEPT SURG, PITTSBURGH, PA 15260 USA
[2] UNIV PITTSBURGH, MED CTR, DEPT MOL GENET, PITTSBURGH, PA 15260 USA
[3] UNIV PITTSBURGH, MED CTR, DEPT BIOCHEM, PITTSBURGH, PA 15260 USA
[4] UNIV PITTSBURGH, GRAD SCH PUBL HLTH, DEPT HUMAN GENET, PITTSBURGH, PA 15260 USA
[5] UNIV PITTSBURGH, INST CANC, PITTSBURGH, PA 15260 USA
[6] IST NAZL TUMORI, DIV EXPT ONCOL, I-20133 MILAN, ITALY
来源
JOURNAL OF CLINICAL INVESTIGATION | 1996年 / 98卷 / 07期
关键词
tumor antigens; T cell recognition; TAP; human melanoma; antigen processing;
D O I
10.1172/JCI118958
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
In the last few years, mutiple protein target antigens for inmunorecognition 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 occured 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.
引用
收藏
页码:1633 / 1641
页数:9
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