Hackett R J, Davis L S, Lipsky P E
Harold C. Simmons Arthritis Research Center, Southwestern Medical School, The University of Texas Health Science Center at Dallas 75235.
J Immunol. 1988 Apr 15;140(8):2639-44.
The effect of rTNF-alpha on human T cell function was examined and compared with that of rIL-1 beta by assessing the ability of each cytokine to support mitogen-induced proliferation, IL-2 production, and IL-2R expression. TNF-alpha and IL-1 beta each enhanced DNA synthesis induced by PHA or immobilized mAb to the CD3 molecular complex. In addition, each cytokine increased the number of cells entering the G1 phase of the cell cycle and augmented IL-2R expression. The combination of optimal concentrations of these factors supported these responses to a greater extent than either cytokine alone, suggesting that T cell responsiveness is independently regulated by the action of at least two separate monocyte derived cytokines. Whereas TNF-alpha had little effect, IL-1 beta augmented IL-2 mRNA expression and IL-2 production by mitogen-stimulated cells. Furthermore, IL-1 beta enhanced proliferation with increasing length of culture. Whereas TNF-alpha also enhanced proliferation late in culture, it was less effective in this regard than IL-1 beta. Thus, IL-1 beta and TNF-alpha augment mitogen-induced T cell proliferation by increasing the number of cells initially activated and by promoting subsequent cell cycle progression. They differ, however, in their capacity to promote IL-2 mRNA and IL-2 production and therefore ongoing T cell proliferation.
通过评估每种细胞因子支持有丝分裂原诱导的增殖、白细胞介素-2(IL-2)产生和IL-2受体表达的能力,研究了重组肿瘤坏死因子-α(rTNF-α)对人T细胞功能的影响,并与重组白细胞介素-1β(rIL-1β)进行了比较。TNF-α和IL-1β均可增强由PHA或固定化抗CD3分子复合物单克隆抗体诱导的DNA合成。此外,每种细胞因子均增加进入细胞周期G1期的细胞数量,并增强IL-2受体表达。这些因子的最佳浓度组合比单独使用任何一种细胞因子都能更大程度地支持这些反应,这表明T细胞反应性至少受两种不同的单核细胞衍生细胞因子的作用独立调节。虽然TNF-α作用很小,但IL-1β可增加有丝分裂原刺激细胞的IL-2 mRNA表达和IL-2产生。此外,IL-1β随着培养时间延长增强增殖。虽然TNF-α在培养后期也增强增殖,但在这方面不如IL-1β有效。因此,IL-1β和TNF-α通过增加最初活化的细胞数量和促进随后的细胞周期进程来增强有丝分裂原诱导的T细胞增殖。然而,它们在促进IL-2 mRNA和IL-2产生以及因此持续的T细胞增殖的能力方面存在差异。
