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
Author
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Kurte, Mónica
Author
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López, Mercedes
Author
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Aguirre, Adam
Author
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Escobar, Alejandro
Author
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Aguillón Gutiérrez, Juan Carlos
Author
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Charo, Jehad
Author
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Larsen, Christian G.
Author
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Kiessling, Rolf
Author
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Salazar Onfray, Flavio
Admission date
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2019-03-11T12:50:51Z
Available date
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2019-03-11T12:50:51Z
Publication date
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2004
Cita de ítem
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Journal of Immunology, Volumen 173, Issue 3, 2018, Pages 1731-1737
Identifier
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00221767
Identifier
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10.4049/jimmunol.173.3.1731
Identifier
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https://repositorio.uchile.cl/handle/2250/164107
Abstract
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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 EL-10 homologue peptide also caused a dose-dependent inhibition of the IFN-γ-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, pepti
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