IL-2 Regulates Perforin and Granzyme Gene Expression in CD8 super(+) T Cells Independently of Its Effects on Survival and Proliferation
Perforin and the serine protease granzymes are key effectors of CD8 super(+) T cell granule-mediated cytotoxicity, but the requirements for their expression remain largely undefined. We show in this study that IL-2 increased the expression of perforin and granzyme A, B, and C mRNA; intracellular gra...
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Veröffentlicht in: | Journal of Immunology 2005-12, Vol.175 (12), p.8003-8010 |
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Sprache: | eng |
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Zusammenfassung: | Perforin and the serine protease granzymes are key effectors of CD8 super(+) T cell granule-mediated cytotoxicity, but the requirements for their expression remain largely undefined. We show in this study that IL-2 increased the expression of perforin and granzyme A, B, and C mRNA; intracellular granzyme B protein levels; and cytolytic function in a dose-dependent manner during primary activation of murine CD8 super(+) T cells in vitro. Two approaches showed that these responses were not a consequence of the effects of IL-2 on cell survival and proliferation. First, IL-2 enhancement of perforin and granzyme expression was equivalent in CD8 super(+) T cells from wild-type and bcl-2 transgenic mice, although only the latter cells survived in low concentrations or the absence of added IL-2. This property of bcl-2 transgenic T cells also allowed the demonstration that induction of granzyme A, B, and C mRNA and granzyme B protein required exogenous IL-2, whereas induction of perforin and IFN- gamma expression did not. Second, analysis of perforin and granzyme mRNA levels in cells separated according to division number using the dye CFSE showed that the effects of IL-2 were unrelated to division number. Together, these findings indicate that IL-2 can directly regulate perforin and granzyme gene expression in CD8 super(+) T cells independently of its effects on cell survival and proliferation. |
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ISSN: | 0022-1767 1365-2567 |