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    Immunology. 2006 Oct;119(2):203-11.

    Splice variants of human FOXP3 are functional inhibitors of human CD4+ T-cell activation.

    Smith EL, Finney HM, Nesbitt AM, Ramsdell F, Robinson MK.

    UCB-Celltech., Slough, UK. Emma.Smith@UCB-group.com

    FOXP3 has been identified as a key regulator of immune homeostasis. Mutations within the FOXP3 gene result in dysregulated CD4+ T-cell function and elevated cytokine production, leading to lymphoproliferative disease. FOXP3 expression in CD4+ T cells is primarily detected with the CD4+ CD25+ regulatory T-cell population. In humans the protein is detected as a doublet following immunoblot analysis. The lower band of the doublet has been identified as a splice isoform lacking a region corresponding to exon 2. The aim of this study was to investigate whether the splice variant form lacking exon 2 and a new novel splice variant lacking both exons 2 and 7, were functional inhibitors of CD4+ T-cell activation. The data generated showed that full-length FOXP3 and both splice variant forms of the protein were functional repressors of CD4+ T-cell activation.

    PMID: 17005002 [PubMed - indexed for MEDLINE]

    PMCID: 1782350

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