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      Frequent HLA class I alterations in human prostate cancer: molecular mechanisms and clinical relevance

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          NLRC5: a key regulator of MHC class I-dependent immune responses.

          The expression of MHC class I molecules is crucial for the initiation and regulation of adaptive immune responses against pathogens. NOD-, LRR- and CARD-containing 5 (NLRC5) was recently identified as a specific transactivator of MHC class I genes (CITA). NLRC5 and the master regulator for MHC class II genes, class II transactivator (CIITA), interact with similar MHC promoter-bound factors. Here, we provide a broad overview of the molecular mechanisms behind MHC class I transcription and the role of the class I transactivator NLRC5 in MHC class I-dependent immune responses.
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            Implications for immunosurveillance of altered HLA class I phenotypes in human tumours.

            HLA class I downregulation is a frequent event associated with tumour invasion and development. Altered HLA class I tumour phenotypes can have profound effects on T-cell and natural killer (NK)-cell antitumour responses. Here, Federico Garrido and colleagues analyse these altered tumour phenotypes in detail, indicating their potential relevance for implementation of immunotherapeutic protocols and strategies to overcome tumour escape mechanisms.
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              Natural history of HLA expression during tumour development.

              HLA expression is frequently altered in tumours compared to the tissue from which they originate. Given the central role of MHC products in the restriction of T-cell recognition, regulation of tumour HLA expression might be a strategy for the evasion of immune surveillance by the malignant cells. Federico Garrido, Peter Stern and colleagues present data from a variety of tumour types, suggesting that HLA class I alterations may occur at a particular step between the development of an in situ lesion and an invasive carcinoma.
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                Author and article information

                Journal
                Cancer Immunology, Immunotherapy
                Cancer Immunol Immunother
                Springer Nature
                0340-7004
                1432-0851
                January 2016
                November 26 2015
                January 2016
                : 65
                : 1
                : 47-59
                Article
                10.1007/s00262-015-1774-5
                26611618
                5819768c-c26e-4266-a83e-7abfa3fb5a90
                © 2016

                http://www.springer.com/tdm

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