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首页> 外文期刊>Peritoneal dialysis international: Journal of the International Society for Peritoneal Dialysis >Can N-acetylcysteine preserve peritoneal function and morphology in encapsulating peritoneal sclerosis?
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Can N-acetylcysteine preserve peritoneal function and morphology in encapsulating peritoneal sclerosis?

机译:N-乙酰半胱氨酸能否在封装腹膜硬化中保留腹膜功能和形态?

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摘要

Long-term use of the peritoneum as a dialysis membrane results in progressive irreversible dysfunction, described as peritoneal fibrosis. Oxidative stress during peritoneal dialysis has been established in many studies. Generation of reactive oxygen species (ROS) by conventional peritoneal dialysis solutions, regardless of whether produced by high glucose, angiotensin II, or glucose degradation products may be responsible for progressive membrane dysfunction. The well-known antioxidant molecule N-acetylcysteine (NAC) is capable of direct scavenging of ROS. The aim of the present study was to investigate the effect of NAC therapy on both progression and regression of encapsulating peritoneal sclerosis (EPS). We divided 49 nonuremic Wistar albino rats into four groups: Control group-2 mL isotonic saline intraperitoneally (IP) daily for 3 weeks; CG group-2 mL/200 g 0.1% chlorhexidine gluconate (CG) and 15% ethanol dissolved in saline injected IP daily for a total of 3 weeks; Resting group-CG (weeks 1 - 3), plus peritoneal resting (weeks 4 - 6); NAC-R group-CG (weeks 1 - 3), plus 2 g/L NAC (weeks 4 - 6). At the end of the experiment, all rats underwent a 1-hour peritoneal equilibration test with 25 mL 3.86% PD solution. Dialysate-to-plasma ratio (D/P) urea, dialysate white blood cell count (per cubic milliliter), ultrafiltration (UF) volume, and morphology changes of parietal peritoneum were examined. The CG group progressed to encapsulating peritoneal sclerosis, characterized by loss of UF, increased peritoneal thickness, inflammation, and ultimately, development of fibrosis. Resting produced advantages only in dialysate cell count; with regard to vascularity and dialysate cell count, NAC was more effective than was peritoneal rest. Interestingly, we observed no beneficial effects of NAC on fibrosis. That finding may be a result of our experimental severe peritoneal injury model. However, decreased inflammation and vascularity with NAC therapy were promising results in regard to membrane protection.
机译:长期使用腹膜作为透析膜会导致进行性不可逆功能障碍,称为腹膜纤维化。在许多研究中已经确定了腹膜透析过程中的氧化应激。常规的腹膜透析溶液产生活性氧(ROS),无论是由高葡萄糖,血管紧张素II还是葡萄糖降解产物产生,都可能是进行性膜功能障碍的原因。众所周知的抗氧化剂分子N-乙酰半胱氨酸(NAC)能够直接清除ROS。本研究的目的是研究NAC治疗对封装性腹膜硬化(EPS)的进展和消退的影响。我们将49只非尿毒症Wistar白化病大鼠分为四组:对照组:腹膜内(IP)2 mL等渗盐水(IP),持续3周。 CG组每天溶于IP溶液中的2 mL / 200 g 0.1%葡萄糖酸氯己定葡萄糖酸盐(CG)和15%乙醇溶解于IP注射液中,共3周;静息组-CG(第1-3周),加上腹膜休息(第4-6周); NAC-R组CG(第1-3周),加上2 g / L NAC(第4-6周)。实验结束时,所有大鼠均用25 mL 3.86%PD溶液进行1小时的腹膜平衡试验。检查了透析液与血浆的比率(D / P)尿素,透析液白细胞计数(每立方毫升),超滤(UF)体积以及顶叶腹膜的形态变化。 CG组发展为包囊性腹膜硬化症,其特征在于UF丢失,腹膜厚度增加,发炎,并最终发展为纤维化。休息仅在透析液细胞计数方面产生优势。在血管和透析液细胞计数方面,NAC比腹膜休息更为有效。有趣的是,我们没有观察到NAC对纤维化的有益作用。这个发现可能是我们实验性严重腹膜损伤模型的结果。然而,就膜保护而言,使用NAC治疗减少炎症和血管是有希望的结果。

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