在接受腹膜透析的终末期肾病和糖尿病患者中,碘糊精消除磷酸盐并改善心脏肥厚和瓣膜钙化。

Takeyuki Hiramatsu, Takahiro Hayasaki, Akinori Hobo, Shinji Furuta, Koki Kabu, Yukio Tonozuka, Yoshiyasu Iida
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引用次数: 0

摘要

在终末期肾病(ESRD)患者中,心血管疾病是常见的合并症,也是影响临床预后的重要因素之一。据报道,钙沉积与血浆磷酸盐有关。基于Icodextrin (Ico)的腹膜透析(PD)比基于葡萄糖(Glu)的腹膜透析(PD)有许多优点。我们的目的是确定抑制ESRD和糖尿病(DM)患者接受ico - PD的动脉硬化和瓣膜疾病的因素。在这项回顾性研究中,我们评估了Ico-based PD (n = 20)对ESRD和dm患者磷酸盐消除和心血管疾病进展的影响,并将结果与Glu-based PD (n = 20)进行了比较。与Glu组相比,Ico组左心室质量指数(LVMI)和主动脉瓣钙化(AVC)评分显著降低,每日磷酸盐消除量显著增加。此外,平均每日磷酸盐消除与LVMI和AVC评分的改善呈显著负相关。我们的研究表明,与葡萄糖相比,碘糊精能够从体内清除更多的磷酸盐,这表明磷酸盐清除可能是控制PD合并DM患者心血管疾病的一种潜在手段。
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Icodextrin eliminates phosphate and ameliorates cardiac hypertrophy and valvular calcification in patients with end-stage renal disease and diabetes mellitus undergoing peritoneal dialysis.

Among end-stage renal disease (ESRD) patients, cardiovascular disease is a common comorbidity and one of most important factors affecting clinical prognosis. Calcium deposition has been reported to correlate with plasma phosphate. Icodextrin (Ico)-based peritoneal dialysis (PD) has many advantages over glucose (Glu)-based PD. We aimed to identify factors that suppress arteriosclerosis and valvular disease in patients with ESRD and diabetes mellitus (DM) undergoing Ico-based PD. In this retrospective study, we evaluated the effects of Ico-based PD (n = 20) on phosphate elimination and cardiovascular disease progression in patients with ESRD andDM, and we compared the results with those for Glu-based PD (n = 20). Left ventricular mass index (LVMI) and aortic valve calcification (AVC) score were significantly decreased and daily phosphate elimination was significantly increased in the Ico group compared with the Glu group. Furthermore, mean daily phosphate elimination was significantly and negatively correlated with the amelioration in LVMI and AVC score. Our study suggests that, compared with glucose, icodextrin has the ability to eliminate more phosphate from the body, indicating that phosphate elimination might potentially be a means of controlling cardiovascular disease in PD patients with DM.

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