磷酸盐作为心血管风险因素:对血管和内皮功能的影响。
Phosphate as a cardiovascular risk factor: effects on vascular and endothelial function.
机构信息
Renal Unit, Western Infirmary, University of Glasgow, Glasgow, UK.
Renal Unit, Western Infirmary, University of Glasgow, Glasgow, UK.
出版信息
Lancet. 2015 Feb 26;385 Suppl 1:S10. doi: 10.1016/S0140-6736(15)60325-7.
BACKGROUND
Hyperphosphataemia is a risk factor for accelerated cardiovascular disease in chronic kidney disease. The mechanism is poorly understood; it is unclear whether phosphate has direct effects or effects mediated via calcification or FGF23. We investigated direct effects of phosphate on endothelial function using myography to study rat and human blood vessels. In addition we assessed the effects of phosphate loading on endothelial function in a clinical study.
METHODS
Resistance vessels from patients with (n=12) and without (n=13) chronic kidney disease were incubated in normal or high phosphate. Vasoconstrictor and vasorelaxation responses were measured. Concentration-response curves were constructed and comparisons made. Identical experiments were performed in rat mesenteric vessels with and without phosphodiesterase type 5 inhibitor. A cross-over study was done in 19 healthy volunteers receiving phosphate supplements or binders and endothelial function measured by flow mediated dilatation (FMD). Primary outcome was percent change in FMD from baseline.
FINDINGS
Nine to 13 vessels were used in each group. Endothelium-dependent vasodilatation was impaired in high compared with normal phosphate in rat (mean maximum vasodilatation 64% [SE 9] vs 95 [1], p<0·001) and human vessels with (25·3 [11·1] vs 75·7 [13·6], p<0·001) and without chronic kidney disease (42·9 [12] vs 79·4 [8·2], p=0·003). In rat vessels, these effects were reversed by a phosphodiesterase type 5 inhibitor. In vivo in volunteers, endothelial function was reduced by phosphate loading (median maximum vasodilatation 3·38% [IQR 2·57-5·26] vs 8·4 [6·2-11·6], p<0·001); this effect was independent of serum phosphate concentration but associated with urinary phosphate excretion and serum FGF23 concentrations.
INTERPRETATION
Prolonged exposure to phosphate is associated with endothelial dysfunction, a direct effect of phosphate, which might contribute to cardiovascular risk in chronic kidney disease. In a high phosphate environment, endothelial and vascular dysfunction is evident in blood vessels and in man exposed to prolonged oral phosphate loading. These effects might be mediated by disruption of the NO pathway.
FUNDING
British Heart Foundation, Darlinda's Charity for Renal Research.
背景
高磷血症是慢性肾脏病加速心血管疾病的一个风险因素。其机制尚不清楚;不清楚磷酸盐是否有直接作用,还是通过钙化或 FGF23 发挥作用。我们通过血管张力测定法研究大鼠和人血管,研究了磷酸盐对内皮功能的直接作用。此外,我们在一项临床研究中评估了磷酸盐负荷对内皮功能的影响。
方法
将来自患有(n=12)和不患有(n=13)慢性肾脏病患者的阻力血管在正常或高磷酸盐中孵育。测量血管收缩和血管舒张反应。构建浓度-反应曲线并进行比较。在有和没有磷酸二酯酶 5 抑制剂的大鼠肠系膜血管中进行相同的实验。在 19 名健康志愿者中进行交叉研究,给予磷酸盐补充剂或结合剂,并通过血流介导的扩张(FMD)测量内皮功能。主要结果是 FMD 从基线的百分比变化。
结果
每组使用 9-13 个血管。与正常磷酸盐相比,高磷酸盐可损害大鼠(最大血管舒张率为 64%[9%] vs 95%[1],p<0·001)和有(最大血管舒张率为 25·3%[11·1] vs 75·7%[13·6],p<0·001)和无慢性肾脏病的人血管内皮依赖性血管舒张。在大鼠血管中,这些作用可被磷酸二酯酶 5 抑制剂逆转。在志愿者体内,磷酸盐负荷可降低内皮功能(最大血管舒张率中位数为 3·38%[2·57-5·26] vs 8·4%[6·2-11·6],p<0·001);该效应与血清磷酸盐浓度无关,但与尿磷酸盐排泄和血清 FGF23 浓度有关。
结论
长期暴露于磷酸盐与内皮功能障碍有关,这是磷酸盐的直接作用,可能导致慢性肾脏病中的心血管风险。在高磷酸盐环境中,在暴露于长期口服磷酸盐负荷的人血管和大鼠血管中都可见到内皮和血管功能障碍。这些作用可能是通过破坏 NO 途径介导的。
资助
英国心脏基金会,达琳达肾脏病研究慈善基金。
Zotero 插件