Citations to this article
Citation Information: J Clin Invest. 1998;102(6):1258-1264. https://doi.org/10.1172/JCI4004.
Abstract
The immune system can recognize self antigens expressed by cancer cells. Differentiation antigens are prototypes of these self antigens, being expressed by cancer cells and their normal cell counterparts. The tyrosinase family proteins are well characterized differentiation antigens recognized by antibodies and T cells of patients with melanoma. However, immune tolerance may prevent immunity directed against these antigens. Immunity to the brown locus protein, gp75/ tyrosinase-related protein-1, was investigated in a syngeneic mouse model. C57BL/6 mice, which are tolerant to gp75, generated autoantibodies against gp75 after immunization with DNA encoding human gp75 but not syngeneic mouse gp75. Priming with human gp75 DNA broke tolerance to mouse gp75. Immunity against mouse gp75 provided significant tumor protection. Manifestations of autoimmunity were observed, characterized by coat depigmentation. Rejection of tumor challenge required CD4(+) and NK1.1(+) cells and Fc receptor gamma-chain, but depigmentation did not require these components. Thus, immunization with homologous DNA broke tolerance against mouse gp75, possibly by providing help from CD4(+) T cells. Mechanisms required for tumor protection were not necessary for autoimmunity, demonstrating that tumor immunity can be uncoupled from autoimmune manifestations.
Authors
L W Weber, W B Bowne, J D Wolchok, R Srinivasan, J Qin, Y Moroi, R Clynes, P Song, J J Lewis, A N Houghton
Total citations by year
Citations to this article in year 2004 (12)
| Title and authors | Publication | Year |
|---|---|---|
|
Immune surveillance in the skin: mechanisms and clinical consequences
TS Kupper, RC Fuhlbrigge |
Nature Reviews Immunology | 2004 |
|
Immune recognition of self in immunity against cancer
AN Houghton, JA Guevara-Patiño |
Journal of Clinical Investigation | 2004 |
|
Tumor antigens for cancer immunotherapy: therapeutic potential of xenogeneic DNA vaccines
R Srinivasan, JD Wolchok |
Journal of Translational Medicine | 2004 |
|
Plasmids encoding membrane-bound IL-4 or IL-12 strongly costimulate DNA vaccination against carcinoembryonic antigen (CEA)
R Chakrabarti, Y Chang, K Song, GJ Prud’homme |
Vaccine | 2004 |
|
CTLA-4 blockade in combination with xenogeneic DNA vaccines enhances T-cell responses, tumor immunity and autoimmunity to self antigens in animal and cellular model systems
PD Gregor, JD Wolchok, CR Ferrone, H Buchinshky, JA Guevara-Patiño, MA Perales, F Mortazavi, D Bacich, W Heston, JB Latouche, M Sadelain, JP Allison, HI Scher, AN Houghton |
Vaccine | 2004 |
|
Effective induction of antitumor immunity by immunization with plasmid DNA encoding TRP-2 plus neutralization of TGF-?
ZC Jia, LY Zou, B Ni, Y Wan, W Zhou, YB Lv, M Geng, YZ Wu |
Cancer Immunology, Immunotherapy | 2004 |
|
Immunoendocrinology in Health and Disease
N Martens, E Hooghe-Peters, R Hooghe |
Immunoendocrinology in Health and Disease | 2004 |
|
Granulocyte-Macrophage Colony Stimulating Factor: An Adjuvant for Cancer Vaccines
DZ Chang, W Lomazow, CJ Somberg, R Stan, MA Perales |
Hematology | 2004 |
|
T-Cell Chauvinists Versus Antibody Advocates—Can't We All Just Get Along?
PB Chapman |
Journal of Clinical Oncology | 2004 |
|
Steroidogenic Acute Regulatory (StAR)-Directed Immunotherapy Protects against Tumor Growth of StAR-Expressing Sp2-0 Cells in a Rodent Adrenocortical Carcinoma Model
D Ortmann, J Hausmann, F Beuschlein, K Schmenger, M Stahl, M Geissler, M Reincke |
Endocrinology | 2004 |
|
Vaccination-Induced Autoimmune Vitiligo Is a Consequence of Secondary Trauma to the Skin
C Lane, J Leitch, X Tan, J Hadjati, JL Bramson, Y Wan |
Cancer research | 2004 |
|
Effective induction of antitumor immunity by immunization with plasmid DNA encoding TRP-2 plus neutralization of TGF-beta.
Jia ZC, Zou LY, Ni B, Wan Y, Zhou W, Lv YB, Geng M, Wu YZ |
Cancer Immunology, Immunotherapy | 2004 |
Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)