Semiquantitative analysis of Th1 and Th2 cytokine expression in CD3+, CD4+, and CD8+renal-cell-carcinoma-infiltrating lymphocytes

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作者
Ursula Elsässer-Beile
Thomas Grussenmeyer
Dorothee Gierschner
Barbara Schmoll
Wolfgang Schultze-Seemann
Ulrich Wetterauer
Jürgen Schulte Mönting
机构
[1] Urological Department,
[2] University of Freiburg,undefined
[3] Experimental Research Group,undefined
[4] Stefan Meier Str. 8,undefined
[5] D-79106 Freiburg,undefined
[6] Germany Fax: +49-761-203-5496,undefined
[7] Institute of Medical Biometry,undefined
[8] University of Freiburg,undefined
[9] D-79106 Freiburg,undefined
[10] Germany,undefined
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Key words Renal cell carcinoma; TIL; Cytokine expression;
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摘要
The mRNA expression of Th1 and Th2 cytokines was compared in freshly isolated CD3+ tumor-infiltrating lymphocytes (CD3+ TIL) and in autologous CD3+ peripheral blood lymphocytes (CD3+ PBL) obtained simultaneously from 20 patients with renal cell carcinomas (RCC). In addition cytokine expression was compared in CD4+ TIL and CD8+ TIL from another group of 20 patients with RCC. TIL were isolated from mechanically disaggregated tumor material and PBL from peripheral blood by gradient centrifugation and subsequent selection with anti-CD3, anti-CD4 or anti-CD8 magnetic beads. In these pure lymphocyte preparations the constitutive expression of interleukin-1 (IL-1), IL-2, IL-10, interferon γ (IFN), and tumor necrosis factor α (TNF) was determined by using a polymerase-chain-reaction-assisted mRNA amplification assay. In the CD3+ TIL, levels of mRNA for IFN, IL-10, IL-1 and TNF were significantly higher than in the autologous CD3+ PBL whereas IL-2 expression was rather low and did not differ in the two populations. Comparison of cytokine mRNA expression in CD4+ TIL and simultaneously obtained CD8+ TIL revealed a significantly higher expression of IFN in the CD8+ cells. These data reflect an in vivo activation of RCC-infiltrating lymphocytes at the mRNA level with respect to the Th1 as well as the Th2 immune response. Th1 activation seems to be most evident in the CD8+ TIL.
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页码:204 / 208
页数:4
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