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Systemic Endotoxin in Peritoneal Dialysis Patients

机译:腹膜透析患者的全身内毒素

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Previous reports linked systemic endotoxemia in dialysis patients to increased markers of inflammation, cardiovascular disease, and mortality. Many peritoneal dialysis (PD) patients use acidic, hypertonic dialysates, which could potentially increase gut permeability, resulting in systemic endotoxemia. However, the results from studies measuring endotoxin in PD patients are discordant. We therefore measured systemic endotoxin in 55 PD outpatients attending for routine assessment of peritoneal membrane function; mean age 58.7 +/- 16.4 years, 32 (58.2%) male, 21 (38.2%) diabetic, median duration of PD treatment 19.5 (13 - 31) months, 32 (58.2%) using 22.7 g/L dextrose dialysates, and 47 (85.5%) icodextrin. The median systemic endotoxin concentration was 0.0485 (0.0043 - 0.103) Eu/mL. We found no association between endotoxin levels and patient demographics, markers of inflammation, serum albumin, N-terminal pro-brain natriuretic peptide, extracellular volume measured by bioimpedance, blood pressure, PD prescriptions or peritoneal membrane transporter status, or medications. The measurement of endotoxin can be lowered by failure to effectively release protein-bound endotoxin prior to analysis and increased by contamination when taking blood samples and processing and storing the samples. Additionally, contamination with li-glucan from fungal cell walls and the use of different assays to analyze endotoxin can also give differing results. These factors may help to explain the disparate results reported in different studies. Our study would suggest that exposure to standard peritoneal dialysates does not substantially increase systemic endotoxin. However, until endotoxin assays can measure free and bound endotoxin separately, the role of endotoxin causing inflammation in PD patients remains to be determined.
机译:以前的报告将透析患者的全身内毒素联系在炎症,心血管疾病和死亡率增加的增加。许多腹膜透析(PD)患者使用酸性高渗透析液,这可能会增加肠道渗透性,导致系统性内毒性。然而,来自PD患者中毒素测量的研究的结果不和谐。因此,我们在参加常规评估腹膜膜功能的55个PD门诊患者中测量了系统内毒素;平均58.7 +/- 16.4岁,32(58.2%)男性,21(38.2%)糖尿病,Pd治疗中值持续时间19.5(13-11)个月,32(58.2%)使用22.7g / l葡萄糖透析液,和47(85.5%)Icodextrin。中值的全身内毒素浓度为0.0485(0.0043-0.103)EU / mL。我们发现内毒素水平和患者人口统计学之间的关联,炎症的标记,血清白蛋白,N-末端促脑利钠肽,通过生物阻抗测量的细胞外体积,血压,Pd处方或腹膜转运蛋白或药物。通过在分析之前有效地释放蛋白质结合的内毒素并且在服用血液样品和加工并储存样品时,可以降低内毒素的测量。另外,从真菌细胞壁上污染Li-glucan以及使用不同的测定来分析内毒素也可以产生不同的结果。这些因素可能有助于解释不同研究报告的不同结果。我们的研究表明,暴露于标准的腹膜透析液并未显着增加全身内毒素。然而,直到内毒素测定可以分别测量自由和结合的内毒素,内毒素导致PD患者炎症的作用仍有待确定。

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