Regulatory effects of transforming growth factor- <i>beta</i> on IL-2- and IL-4-dependent T cell-cycle progression.

  • J J Ruegemer
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • S N Ho
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • J A Augustine
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • J W Schlager
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • M P Bell
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • D J McKean
    Department of Immunology, Mayo Clinic , Rochester, MN 55905
  • R T Abraham
    Department of Immunology, Mayo Clinic , Rochester, MN 55905

書誌事項

公開日
1990-03-01
権利情報
  • https://academic.oup.com/pages/standard-publication-reuse-rights
DOI
  • 10.4049/jimmunol.144.5.1767
公開者
Oxford University Press (OUP)

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説明

<jats:title>Abstract</jats:title> <jats:p>Previous studies suggested that the potent immunosuppressive activities of transforming growth factor-beta (TGF-beta) were mediated in part through the inhibition of IL-2-dependent S-phase progression and mitosis of activated T cells. To further investigate the mechanism of T cell growth inhibition by TGF-beta, two constitutively activated murine T cell clones were employed as defined model systems for the growth factor-dependent phase of T cell proliferation. The Th cell line, HT-2, proliferated in response to either IL-2 or IL-4, whereas the cytotoxic T cell line, CT6, exhibited strict dependence on IL-2 for growth stimulation. In both cell lines, picomolar concentrations of TGF-beta inhibited S-phase progression stimulated by IL-2 or IL-4. TGF-beta pretreatment decreased the expression of high affinity IL-2R on HT-2 cells, but not on CT6 cells. In contrast, IL-2-stimulated transferrin receptor expression was markedly inhibited by TGF-beta in both T cell lines. Analyses of growth factor-dependent specific mRNA accumulation revealed that TGF-beta exerted selective inhibitory effects on gene expression in HT-2 and CT6 cells. TGF-beta significantly reduced early (1 to 2 h) increases in c-myc mRNA levels stimulated by IL-2 or IL-4 in both cell lines. In HT-2 cells, TGF-beta pretreatment also inhibited the early increase in granulocyte-macrophage CSF mRNA stimulated by IL-2 or IL-4. The inhibition of c-myc and granulocyte-macrophage cyte-macrophage CSF gene expression by TGF-beta was explained, at least in part, by suppression of the growth factor-dependent transcriptional activation of these genes. These studies suggest that inhibition of c-myc gene transcription may play a fundamental role in the antiproliferative effect of TGF-beta on IL-2- or IL-4-stimulated T cells.</jats:p>

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