首页> 外文期刊>International immunology. >Serum DNase I, soluble Fas/FasL levels and cell surface Fas expression in patients with SLE: a possible explanation for the lack of efficacy of hrDNase I treatment.
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Serum DNase I, soluble Fas/FasL levels and cell surface Fas expression in patients with SLE: a possible explanation for the lack of efficacy of hrDNase I treatment.

机译:SLE患者的血清DNase I,可溶性Fas / FasL水平和细胞表面Fas表达:这可能是hrDNase I治疗无效的原因。

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摘要

The objectives of the study are to evaluate DNase I serum levels and their correlation with soluble Fas (sFas) and soluble Fas ligand (sFasL) and with cell surface Fas expression in patients with systemic lupus erythematosus (SLE), thus contributing to the dysregulated apoptosis typical of the disease. The methods include the following: Serum DNase I levels in patients and in controls were detected using the dot blot method and quantified by densitometry; sFas and sFasL were quantified using an ELISA system. Cell surface Fas expression was evaluated by FACS analysis. Apoptosis was studied by means of internucleosomal DNA degradation using a commercially available kit. The results are as follows: We found a significant difference in DNase I, sFas and sFasL serum levels between patients and controls. Levels of DNase I <7.79 ng ml(-1) are more represented in patients with SLE. Active SLE is strongly associated with high sFas levels and detectable sFasL. DNase I does not correlate with sFas or sFasL, whereas it correlates with T cell surface Fas expression that is higher in patients with active SLE than in healthy controls. Finally, administration of exogenous human recombinant DNase (hrDNase) I to freshly isolated T cells up-regulates cell surface Fas expression and induces increased susceptibility to Fas-mediated apoptosis. In conclusion, our findings confirm that DNase I is low in SLE and suggest that it may play a role in apoptosis in SLE by regulating the surface expression of the cell death molecule Fas. This role may contribute to explain the inefficacy of hrDNase I in SLE, a treatment proposed for the ability of DNase I to remove DNA from auto-antigenic nucleoprotein complexes.
机译:该研究的目的是评估系统性红斑狼疮(SLE)患者中DNase I的血清水平及其与可溶性Fas(sFas)和可溶性Fas配体(sFasL)以及与细胞表面Fas表达的相关性,从而有助于细胞凋亡失调典型的疾病。这些方法包括:用斑点印迹法检测患者和对照组的血清DNase I水平,并通过光密度测定法进行定量。使用ELISA系统对sFas和sFasL进行定量。通过FACS分析评估细胞表面Fas表达。使用市售试剂盒通过核小体间DNA降解研究凋亡。结果如下:我们发现患者和对照组之间的DNase I,sFas和sFasL血清水平存在显着差异。 SLE患者中DNase I <7.79 ng ml(-1)的水平更高。活动性SLE与高sFas水平和可检测的sFasL密切相关。 DNase I与sFas或sFasL不相关,而与活动性SLE患者中T细胞表面Fas表达相关,高于健康对照组。最后,将外源人重组DNase(hrDNase)I给予新鲜分离的T细胞可上调细胞表面Fas表达并诱导对Fas介导的细胞凋亡的敏感性增加。总之,我们的发现证实DNase I在SLE中较低,并暗示它可能通过调节细胞死亡分子Fas的表面表达而在SLE细胞凋亡中起作用。这种作用可能有助于解释hrDNase I在SLE中的无效性,这是一种针对DNase I从自身抗原性核蛋白复合物中去除DNA的能力而提出的治疗方法。

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