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Effect of Low-Protein Diet and Inulin on Microbiota and Clinical Parameters in Patients with Chronic Kidney Disease

机译:低蛋白饮食和菊粉对慢性肾脏病患者微生物群和临床指标的影响

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摘要

Introduction: The gut microbiota has coevolved with humans for a mutually beneficial coexistence and plays an important role in health and disease. A dysbiotic gut microbiome may contribute to progression to chronic kidney disease (CKD) and CKD-related complications such as cardiovascular disease. Microbiota modulation through the administration of prebiotics may represent an important therapeutic target. Aim: We sought to evaluate the effects of a low-protein diet (LPD) (0.6 g/kg/day) with or without the intake of the prebiotic inulin (19 g/day) on microbiota and clinical parameters in CKD patients. Materials and Methods: We performed a longitudinal, prospective, controlled, and interventional study on 16 patients: 9 patients treated with LPD (0.6 g/kg/day) and inulin (19 g/day) and 7 patients (control group) treated only with LPD (0.6 g/kg/day). Clinical evaluations were performed and fecal samples were collected for a subsequent evaluation of the intestinal microbiota in all patients. These tests were carried out before the initiation of LPD, with or without inulin, at baseline (T0) and at 6 months (T2). The microbiota of 16 healthy control (HC) subjects was also analyzed in order to identify potential dysbiosis between patients and healthy subjects. Results: Gut microbiota of CKD patients was different from that of healthy controls. The LPD was able to significantly increase the frequencies of Akkermansiaceae and Bacteroidaceae and decrease the frequencies of Christensenellaceae, Clostridiaceae, Lactobacillaceae, and Pasteurellaceae. Only Bifidobacteriaceae were increased when the LPD was accompanied by oral inulin intake. We showed a significant reduction of serum uric acid (SUA) and C-reactive protein (CRP) in patients treated with LPD and inulin ( = 0.018 and = 0.003, respectively), an improvement in SF-36 (physical role functioning and general health perceptions; = 0.03 and = 0.01, respectively), and a significant increase of serum bicarbonate both in patients treated with LPD ( = 0.026) or with LPD and inulin ( = 0.01). Moreover, in patients treated with LPD and inulin, we observed a significant reduction in circulating tumor necrosis factor alpha (TNF-α) ( = 0.041) and plasma nicotinamide adenine dinucleotide phosphate (NADPH) oxidase (NOX2) ( = 0.027) levels. We did not find a significant difference in the circulating levels of Interleukin (IL)-1β ( = 0.529) and IL-6 ( = 0.828) in the two groups. Conclusions: LPD, associated or not with inulin, modified gut microbiota and modulated inflammatory and metabolic parameters in patients with CKD. Our results suggest that interventions attempting to modulate the gut microbiome may represent novel strategies to improve clinical outcomes in CKD patients and may provide useful therapeutic effects.
机译:简介:肠道菌群已与人类共同进化,实现了互惠共存,并在健康和疾病中发挥着重要作用。营养不良的肠道微生物组可能会导致慢性肾脏疾病(CKD)和与CKD相关的并发症(例如心血管疾病)的进展。通过施用益生元来调节微生物群可能代表了重要的治疗目标。目的:我们试图评估低蛋白饮食(LPD)(0.6 g / kg /天)是否摄入益生菌菊粉(19 g /天)对CKD患者微生物群和临床指标的影响。材料和方法:我们对16例患者进行了纵向,前瞻性,对照和干预性研究:9例接受LPD(0.6 g / kg /天)和菊粉(19 g /天)的患者,7例(对照组)仅接受治疗LPD(0.6克/千克/天)。进行了临床评估并收集了粪便样本,用于随后评估所有患者的肠道菌群。这些测试是在基线(T0)和6个月(T2)开始有或没有菊粉的LPD之前进行的。还分析了16位健康对照(HC)受试者的微生物群,以鉴定患者和健康受试者之间的潜在营养不良。结果:CKD患者肠道菌群与健康对照组不同。 LPD能够显着增加Akkermansiaceae和Bacteroidaceae的频率,并降低Christensenellaceae,Closstridaceae,Lactobacillaceae和Pasteurellaceae的频率。当LPD伴随口服菊粉摄入时,仅双歧杆菌科增加。我们显示LPD和菊粉治疗的患者的血清尿酸(SUA)和C反应蛋白(CRP)显着降低(分别为0.018和0.003),SF-36有所改善(生理作用和一般健康) LPD(= 0.026)或LPD和菊粉(= 0.01)治疗的患者血清碳酸氢盐的显着增加;分别为0.03和0.01),并且血清碳酸氢盐的显着增加。此外,在接受LPD和菊粉治疗的患者中,我们观察到循环肿瘤坏死因子α(TNF-α)(= 0.041)和血浆烟酰胺腺嘌呤二核苷酸磷酸(NADPH)氧化酶(NOX2)(= 0.027)水平显着降低。我们没有发现两组白细胞介素(IL)-1β(= 0.529)和IL-6(= 0.828)的循环水平有显着差异。结论:CKD患者的LPD与菊粉是否相关,肠道菌群改变,炎症和代谢参数调节有关。我们的结果表明,尝试调节肠道微生物组的干预措施可能代表改善CKD患者临床结局的新颖策略,并可能提供有用的治疗效果。

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