A synthetic peptide homologous to functional domain of human IL-10 down-regulates expression of MHC class I and transporter associated with antigen processing 1/2 in human melanoma cells

被引:60
|
作者
Kurte, M
López, M
Aguirre, A
Escobar, A
Aguillón, JC
Charo, J
Larsen, CG
Kiessling, R
Salazar-Onfray, F
机构
[1] Univ Chile, Fac Med, Inst Biomed Sci, Disciplinary Program Immunol, Santiago 1027, Chile
[2] Karolinska Hosp, Radiumhemmet, Dept Pathol & Oncol, S-10401 Stockholm, Sweden
[3] Univ Aarhus, Marselisborg Hosp, Dept Dermatol, Aarhus C, Denmark
[4] Max Delbruck Ctr Mol Med, Berlin, Germany
来源
JOURNAL OF IMMUNOLOGY | 2004年 / 173卷 / 03期
关键词
D O I
10.4049/jimmunol.173.3.1731
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Tumor cells treated with IL-10 were shown to have decreased, but peptide-inducible expression of MHC class I, decreased sensitivity to MHC class I-restricted CTL, and increased NK sensitivity. These findings could be explained, at least partially, by a down-regulation of TAP1/TAP2 expression. In this study, IT9302, a nanomeric peptide (AYMTMKIRN), homologous to the C-terminal of the human IL-10 sequence, was demonstrated to mimic these previously described IL-10 effects on MHC class I-related molecules and functions. We observed a dose-dependent down-regulation of MHC class I at the cell surface of melanoma cells after 24-h treatment with IT9302. The IL-10 homologue peptide also caused a dose-dependent inhibition of the IFN-gamma-mediated surface induction of MHC class I in a melanoma cell line. We demonstrated, using Western blot and flow cytometry, that IT9302 inhibits the expression of TAP1 and TAP2 proteins, but not MHC class I H chain or low molecular protein molecules. Finally, peptide-treated melanoma cells were shown to be more sensitive to lysis by NK cells in a dose-dependent way. Taken together, these results demonstrate that a small synthetic peptide derived from IL-10 can mimic the Ag presentation-related effects mediated by this cytokine in human melanomas and increase tumor sensitivity to NK cells, which can be relevant in the designing of future strategies for cancer immune therapy.
引用
收藏
页码:1731 / 1737
页数:7
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