在急性小鼠疟疾期间,用白细胞介素2在体内治疗可减少寄生虫血症,恢复ifn - γ基因表达和t细胞增殖。

B Lucas, L H Kasper, K Smith, A Haque
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引用次数: 0

摘要

在这项研究中,我们描述了宿主免疫系统在急性约氏疟原虫感染后发生的功能改变。此外,我们还提出了一个问题,即细胞因子治疗是否可以恢复免疫反应性改变的短暂状态。与免疫和正常动物相比,急性感染小鼠对刀豆蛋白A (Con A)或交联抗cd3单抗的淋巴细胞增殖反应显著减弱。这种情况与IL-2产生不良有关。在体内用重组IL-2 (IL-2)处理可显著降低小鼠感染急性期的寄生率(从24% +/- 6%降至8% +/- 3%)。尽管寄生虫病有所减少,但70%的IL-2治疗小鼠在感染后第17天死亡。在体内用rIL-2治疗急性感染小鼠,可部分但显著地恢复对tcr介导的(交联抗cd3单抗)或Con - a诱导刺激的淋巴细胞增殖反应。IL-4、IL-5、GM-CSF和tnf - α的转录本在未接受il -2治疗的急性感染小鼠的脾细胞中表达。急性感染小鼠体内未检测到的IL-2、ifn - γ、IL-6、IL-10 mrna可通过给药IL-2逆转。我们认为,在感染的急性期,一些低反应的t细胞具有逆转的潜力,这种逆转也表现在细胞因子基因表达水平上。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In vivo treatment with interleukin 2 reduces parasitemia and restores IFN-gamma gene expression and T-cell proliferation during acute murine malaria.

In this study, we describe the functional alterations in the host immune system that occur following acute infection with Plasmodium yoelii. Further, we have addressed the question whether the transient condition of altered immune responsiveness can be restored by a cytokine therapy. The lymphoproliferative response towards concanavalin A (Con A) or to cross-linked anti-CD3 mAb was significantly diminished in acutely infected mice compared to immune and normal animals. This condition was associated with poor production of IL-2. In vivo treatment with recombinant IL-2 (rIL-2) resulted in marked diminution of parasitemia (from 24% +/- 6% to 8% +/- 3%) in mice during the acute phase of infection. Despite this diminution in parasitemia, 70% of the IL-2 treated mice died by day 17 post infection. In vivo treatment with rIL-2 led to a partial but significant restoration in lymphoproliferative response to TCR-mediated (cross-linked anti-CD3 mAb) or to Con A-induced stimulation in acutely infected mice. The transcripts for IL-4, IL-5, GM-CSF, and TNF-alpha were expressed in the splenocytes from acutely infected mice not treated with rIL-2. mRNAs for IL-2, IFN-gamma, IL-6, IL-10 which were not detected in acutely infected mice could be reversed by administration of rIL-2 in vivo. We suggest that some of the hyporesponsive T-cells in the acute phase of infection have the potential to be reversed, and this reversal is manifested also at the level of cytokine gene expression.

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