首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Enhancing the effect of secreted cyclophilin B on immunosuppressive activity of cyclosporine.
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Enhancing the effect of secreted cyclophilin B on immunosuppressive activity of cyclosporine.

机译:增强分泌的亲环蛋白B对环孢素免疫抑制活性的影响。

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BACKGROUND: Cyclophilin B (CyPB) is a cyclosporine (CsA)-binding protein, located within intracellular vesicles and secreted in biological fluids. In previous works, we reported that CyPB specifically interacts with the T-cell membrane and potentiates the ability of CsA to inhibit CD3-induced proliferation of T lymphocytes. METHODS: CyPB levels were measured in plasma from healthy donors and transplant patients. The role of extracellular CyPB on the distribution and activity of CsA was investigated first by studies on the uptake of free and CyPB-complexed drug by blood cells, and second by studies on the inhibitory effects of these two compounds on the CD3-induced proliferation of peripheral blood mononuclear cells. RESULTS: A significant increase in plasma CyPB level was observed for CsA-treated patients (13+/-6.4 nM, n=42) in comparison with untreated donors (4.3+/-2.1 nM, n=34). In vitro, extracellular CyPB dose dependently modified CsA distribution between plasma, erythrocyte, and lymphocyte contents, by both retaining the complexed drug extracellularly and promoting its specific accumulation within peripheral blood mononuclear cells. Moreover, the enhanced ability of CyPB-complexed CsA to suppress CD3-induced T-cell proliferation was preserved in the presence of other blood cells, implying specific targeting of the drug to sensitive cells. Furthermore, although a large interindividual variability of sensitivity to the drug was confirmed for 18 individuals, we found that CyPB potentiated the activity of CsA in restoring a high sensitivity to the immunosuppressant. CONCLUSION: These results suggest that plasma CyPB may contribute to the acceptance and the good maintenance of organ transplantation by enhancing the immunosuppressive activity of CsA through a receptor-mediated incorporation of CyPB-complexed CsA within peripheral blood lymphocytes.
机译:背景:亲环蛋白B(CyPB)是一种环孢菌素(CsA)结合蛋白,位于细胞内囊泡中,并分泌于生物体液中。在以前的工作中,我们报道了CyPB与T细胞膜特异性相互作用,增强了CsA抑制CD3诱导的T淋巴细胞增殖的能力。方法:测定健康供体和移植患者血浆中的CyPB水平。首先通过研究血细胞对游离和CyPB复合药物的摄取,然后通过研究这两种化合物对CD3诱导的CD3增殖的抑制作用来研究胞外CyPB对CsA的分布和活性的作用。外周血单核细胞。结果:与未经治疗的供体(4.3 +/- 2.1 nM,n = 34)相比,经CsA治疗的患者(13 +/- 6.4 nM,n = 42)血浆CyPB水平显着增加。在体外,细胞外CyPB剂量通过在细胞外保留复合药物并促进其在外周血单核细胞内的特异性积累,来修饰血浆,红细胞和淋巴细胞含量之间的CsA分布。此外,在存在其他血细胞的情况下,CyPB复合CsA抑制CD3诱导的T细胞增殖的能力得到了增强,这意味着该药物可特异性靶向敏感细胞。此外,尽管已确认18位个体对药物的敏感性存在较大的个体差异,但我们发现CyPB增强了CsA的活性,从而恢复了对免疫抑制剂的高敏感性。结论:这些结果表明血浆CyPB可能通过受体介导的CyPB复合CsA在外周血淋巴细胞中的掺入而增强CsA的免疫抑制活性,从而有助于器官移植的接受和良好的维持。

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