接受透析治疗的儿童因细胞内氧化应激增加而导致细胞因子合成异常。
Abnormal cytokine synthesis as a consequence of increased intracellular oxidative stress in children treated with dialysis.
作者信息
Zachwieja Jacek, Zaniew Marcin, Runowski Dariusz, Lewandowska-Stachowiak Maria, Stefaniak Ewa, Siwińska Aldona
机构信息
Department of Pediatric Nephrology, Poznań University of Medical Sciences, Poznań, Poland.
出版信息
Nephron Clin Pract. 2005;101(2):c100-8. doi: 10.1159/000086348. Epub 2005 Jun 14.
BACKGROUND/AIM: End-stage renal disease (ESRD) induces a clinical state of immunodeficiency with a higher incidence of infections and higher mortality due to infectious complications compared with the normal population. The definite mechanism responsible for the host defense alterations is not well understood. The aim of the study was to investigate intracellularly the relationship between cytokine synthesis and oxidative stress in peripheral blood lymphocytes in children with ESRD.
METHODS
Twenty-one children (age 11.7 +/- 5.8 years) with ESRD treated with hemodialysis (HD; n = 10) and peritoneal dialysis (PD; n = 11) were studied. Nine healthy children of comparable age formed the control group. To determine intracellular oxidative stress we used dihydrorhodamine-123 (DHR), which after oxidation to rhodamine-123 (RHO) emitted a bright fluorescent signal. Intracellular oxidation of DHR in T lymphocytes reflected intracellular oxidative stress. The intracellular synthesis of cytokines (IL-2, IFN-gamma, IL-4, IL-6) was also measured. Both parameters were detected at a single-cell level by flow cytometry. Lymphocyte subsets were evaluated using the monoclonal antibodies conjugated with fluorochromes.
RESULTS
We found that in T lymphocytes the mean fluorescence intensity (MFI), which reflected intracellular oxidative stress, was increased in ESRD patients compared to the controls (CD3+: 34.77 +/- 11.55 vs. 22.55 +/- 4.97, p < 0.01; CD3+CD8+: 34.31 +/- 12.17 vs. 20.77 +/- 4.89, p < 0.01; CD3+CD4+: 36.06 +/- 6.98 vs. 24.44 +/- 7.68, p < 0.001). HD patients showed slightly higher MFI compared to PD patients in CD3+ cells (39.32 +/- 11.70 vs. 30.63 +/- 10.20, NS), in CD3+CD8+ cells (37.90 +/- 14.32 vs. 31.06 +/- 9.34, NS) and in CD3+CD4+ cells (40.10 +/- 2.28 vs. 29.33 +/- 7.06, p < 0.001). The intracellular synthesis of IL-2 was higher in ESRD patients compared to the controls, both in CD3+ cells (31.34 +/- 9.80 vs. 20.49 +/- 15.26%, p < 0.05) and in CD3+CD4+ cells (36.10 +/- 8.69 vs. 24.03 +/- 16.95%, p < 0.05). The intracellular synthesis of IFN-gamma, IL-4 and IL-6 was significantly lower in the ESRD group compared to the controls. Interestingly, in patients treated with HD, negative correlations between the degree of intracellular oxidative stress and intracellular cytokine synthesis in CD3+ lymphocytes were found.
CONCLUSION
Our results show that patients with ESRD, especially those treated with HD, present increased oxidative stress in T lymphocytes, which may lead to decreased cytokine synthesis and abnormal immune response.
背景/目的:终末期肾病(ESRD)会引发免疫缺陷的临床状态,与正常人群相比,感染发生率更高,且因感染并发症导致的死亡率更高。宿主防御改变的确切机制尚不清楚。本研究的目的是在细胞内研究ESRD患儿外周血淋巴细胞中细胞因子合成与氧化应激之间的关系。
方法
对21例接受血液透析(HD;n = 10)和腹膜透析(PD;n = 11)治疗的ESRD患儿(年龄11.7±5.8岁)进行研究。9名年龄相仿的健康儿童组成对照组。为测定细胞内氧化应激,我们使用了二氢罗丹明-123(DHR),其氧化为罗丹明-123(RHO)后会发出明亮的荧光信号。T淋巴细胞中DHR的细胞内氧化反映了细胞内氧化应激。还测定了细胞因子(IL-2、IFN-γ、IL-4、IL-6)的细胞内合成。通过流式细胞术在单细胞水平检测这两个参数。使用与荧光染料偶联的单克隆抗体评估淋巴细胞亚群。
结果
我们发现,与对照组相比,ESRD患者T淋巴细胞中反映细胞内氧化应激的平均荧光强度(MFI)增加(CD3 +:34.77±11.55对22.55±4.97,p <0.01;CD3 + CD8 +:34.31±12.17对20.77±4.89,p <0.01;CD3 + CD4 +:36.06±6.98对24.44±7.68,p <0.001)。在CD3 +细胞(39.32±11.70对30.63±10.20,无显著性差异)、CD3 + CD8 +细胞(37.90±14.32对31.06±9.34,无显著性差异)和CD3 + CD4 +细胞(40.10±2.28对29.33±7.06,p <0.001)中,HD患者的MFI略高于PD患者。与对照组相比,ESRD患者IL-2的细胞内合成在CD3 +细胞(31.34±9.80对20.49±15.26%,p <0.05)和CD3 + CD4 +细胞(36.10±8.69对24.03±16.95%,p <0.05)中均更高。ESRD组中IFN-γ-、IL-4和IL-6的细胞内合成显著低于对照组。有趣的是,在接受HD治疗的患者中,发现CD3 +淋巴细胞中细胞内氧化应激程度与细胞内细胞因子合成之间存在负相关。
结论
我们的结果表明,ESRD患者,尤其是接受HD治疗的患者,T淋巴细胞中氧化应激增加,这可能导致细胞因子合成减少和免疫反应异常。
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