Identification of BING-4 Cancer Antigen Translated From an Alternative Open Reading Frame of a Gene in the Extended MHC Class II Region Using Lymphocytes From a Patient With a Durable Complete Regression Following Immunotherapy

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The Journal of Immunology, 2002, 168: 2402-2407.
Copyright © 2002 by The American Association of Immunologists

Identification of BING-4 Cancer Antigen Translated From an Alternative Open Reading Frame of a Gene in the Extended MHC Class II Region Using Lymphocytes From a Patient With a Durable Complete Regression Following Immunotherapy

Steven A. Rosenberg¹, Panida Tong-On, Yong Li, John P. Riley, Mona El-Gamil, Maria R. Parkhurst and Paul F. Robbins

Center for Cancer Research, National Cancer Institute, Institutes of Health, Bethesda, MD 20892

Multiple human cancer Ags have been identified, although littleis known concerning which would be most effectively used incancer immunotherapy. To gain insight into the selection ofappropriate Ags, the immunologic reactivity of a patient whohad a durable complete regression of melanoma metastases wasmeasured. PBMCs were directly cloned using the monoclonal anti-CD3Ab OKT3 and IL-2 without any bias introduced by previous culture.A lymphocyte clone recognized a previously unknown shared melanomaAg that was identified as the BING-4 protein encoded in a gene-richregion of the extended class II MHC. The HLA-A2-restricted BING-4immunodominant peptide was translated from a 10-aa-long alternativeopen reading frame. In vitro sensitization against this peptidegenerated lymphocytes reactive against HLA-A2⁺ melanomas. Real-timesemiquantitative RT-PCR analysis revealed that 8 of 15 melanomacell lines overexpressed BING-4, and this correlated with recognitionby lymphocytes. Overexpression was not found in normal tissuesor other tumor types. Thus, BING-4 represents another candidateAg for possible use in the immunotherapy of patients with melanoma.

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