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首页> 外文期刊>International immunopharmacology >Thalidomide can costimulate or suppress CD4+ cells' ability to incorporate (H3)-thymidine--dependence on the primary stimulant.
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Thalidomide can costimulate or suppress CD4+ cells' ability to incorporate (H3)-thymidine--dependence on the primary stimulant.

机译:沙利度胺可以共刺激或抑制CD4 +细胞掺入(H3)-胸苷的能力-依赖于主要刺激物。

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摘要

Thalidomide is a drug that can enhance mitogen- and antigen-stimulated cells' ability to synthesize IL-2. To assess if thalidomide could concomitantly enhance the synthesis of IFN-gamma and incorporation of [H3]-thymidine, peripheral blood mononuclear cells (PBMC) were incubated in the presence or absence of thalidomide and staphylococcal enterotoxin A (SEA), anti-CD3, Con-A or PHA. After 18 h, the cultures were sampled for IL-2. At the termination of the 3-day cultures, they were assayed for IFN-gamma and incorporation of [H3]-thymidine. Regardless of the mitogen used to stimulate the PBMC, the thalidomide-treated PBMC produced more IL-2 than controls. Thalidomide enhanced IFN-gamma synthesis in the Con-A and anti-CD3-stimulated PBMC. It suppressed the ability of SEA and PHA-stimulated PBMC to incorporate [H3]-thymidine, whereas it enhanced incorporation of [H3]-thymidine in PBMCs stimulated with anti-CD3. When the PBMC were enriched for CD4+ or CD8+ cells, the SEA- and anti-CD3-stimulated CD4+ cells responded far better than the CD8+ cells in the synthesis of IL-2 and incorporation of [H3]-thymidine. In the thalidomide-treated SEA-stimulated CD4+ and CD8+ cells, thalidomide acted as a costimulant to enhance the synthesis of IL-2. In the anti-CD3-stimulated thalidomide-treated cultures of PBMC enriched for CD4+ cells, thalidomide acted as a costimulant to enhance the incorporation [H3]-thymidine. Thalidomide cooperated with all of the mitogens to enhance T-cell synthesis of IL-2. However, depending on the stimulant, thalidomide could suppress or enhance PBMC incorporation of [H3]-thymidine. The SEA-stimulated cells targeted by thalidomide to suppress incorporation of [H3]-thymidine were CD4+. CD4+ cells stimulated with anti-CD3 were enhanced by thalidomide in their ability to synthesize IL-2 and to incorporate [H3]-thymidine. Increased production of IL-2 by activated T cells may be a mechanism through which thalidomide exerts its immunomodulatory effects.
机译:沙利度胺是一种可以增强有丝分裂原和抗原刺激的细胞合成IL-2的能力的药物。为了评估沙利度胺是否可以同时增强IFN-γ的合成和[H3]-胸苷的掺入,在存在或不存在沙利度胺和葡萄球菌肠毒素A(SEA),抗CD3的情况下孵育外周血单个核细胞(PBMC), Con-A或PHA。 18小时后,对培养物取样IL-2。在3天的培养结束时,测定它们的IFN-γ和[H3]-胸苷的掺入。不管用于刺激PBMC的有丝分裂原,沙利度胺处理的PBMC产生的IL-2均比对照多。沙利度胺增强了Con-A和抗CD3刺激的PBMC中的IFN-γ合成。它抑制了SEA和PHA刺激的PBMC掺入[H3]-胸腺嘧啶核苷的能力,而它增强了[H3]-胸腺嘧啶核苷在抗CD3刺激的PBMC中的掺入。当PBMC富含CD4 +或CD8 +细胞时,SEA-和抗CD3刺激的CD4 +细胞在IL-2合成和[H3]-胸苷掺入中的反应远好于CD8 +细胞。在沙利度胺治疗的SEA刺激的CD4 +和CD8 +细胞中,沙利度胺充当促进IL-2合成的共刺激剂。在富含CD4 +细胞的PBMC的抗CD3刺激的沙利度胺处理的培养物中,沙利度胺起着促进[H3]-胸苷掺入的共刺激作用。沙利度胺与所有有丝分裂原协同作用以增强IL-2的T细胞合成。然而,取决于刺激剂,沙利度胺可以抑制或增强[H3]-胸苷的PBMC掺入。沙利度胺靶向抑制[H3]-胸苷掺入的SEA刺激细胞为CD4 +。沙利度胺增强了抗CD3刺激的CD4 +细胞的合成IL-2和整合[H3]-胸苷的能力。活化的T细胞增加IL-2的产生可能是沙利度胺发挥其免疫调节作用的机制。

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