Department of Cellular Physiology and Metabolism, University of Geneva, CMU, 1 Rue Michel-Servet, CH-1211, Geneva 4, Switzerland.
National Centre of Competence in Research, NCCRKidney, CH, Switzerland.
J Physiol. 2017 Nov 15;595(22):6905-6922. doi: 10.1113/JP274927. Epub 2017 Oct 15.
Body Na content is tightly controlled by regulated urinary Na excretion. The intrarenal mechanisms mediating adaptation to variations in dietary Na intake are incompletely characterized. We confirmed and expanded observations in mice that variations in dietary Na intake do not alter the glomerular filtration rate but alter the total and cell-surface expression of major Na transporters all along the kidney tubule. Low dietary Na intake increased Na reabsorption in the proximal tubule and decreased it in more distal kidney tubule segments. High dietary Na intake decreased Na reabsorption in the proximal tubule and increased it in distal segments with lower energetic efficiency. The abundance of apical transporters and Na delivery are the main determinants of Na reabsorption along the kidney tubule. Tubular O consumption and the efficiency of sodium reabsorption are dependent on sodium diet.
Na excretion by the kidney varies according to dietary Na intake. We undertook a systematic study of the effects of dietary salt intake on glomerular filtration rate (GFR) and tubular Na reabsorption. We examined the renal adaptive response in mice subjected to 7 days of a low sodium diet (LSD) containing 0.01% Na , a normal sodium diet (NSD) containing 0.18% Na and a moderately high sodium diet (HSD) containing 1.25% Na . As expected, LSD did not alter measured GFR and increased the abundance of total and cell-surface NHE3, NKCC2, NCC, α-ENaC and cleaved γ-ENaC compared to NSD. Mathematical modelling predicted that tubular Na reabsorption increased in the proximal tubule but decreased in the distal nephron because of diminished Na delivery. This prediction was confirmed by the natriuretic response to diuretics targeting the thick ascending limb, the distal convoluted tubule or the collecting system. On the other hand, HSD did not alter measured GFR but decreased the abundance of the aforementioned transporters compared to NSD. Mathematical modelling predicted that tubular Na reabsorption decreased in the proximal tubule but increased in distal segments with lower transport efficiency with respect to O consumption. This prediction was confirmed by the natriuretic response to diuretics. The activity of the metabolic sensor adenosine monophosphate-activated protein kinase (AMPK) was related to the changes in tubular Na reabsorption. Our data show that fractional Na reabsorption is distributed differently according to dietary Na intake and induces changes in tubular O consumption and sodium transport efficiency.
体内钠含量受调节性尿钠排泄的严格控制。介导饮食钠摄入变化适应的肾内机制尚未完全阐明。我们证实并扩展了在小鼠中的观察结果,即饮食钠摄入的变化不会改变肾小球滤过率,但会改变整个肾脏小管中主要钠转运体的总表达和细胞表面表达。低饮食钠摄入增加了近端小管的钠重吸收,减少了远端肾脏小管段的钠重吸收。高饮食钠摄入减少了近端小管的钠重吸收,增加了能量效率较低的远端段的钠重吸收。顶端转运体的丰度和钠输送是肾脏小管中钠重吸收的主要决定因素。管状 O 消耗和钠重吸收效率取决于钠饮食。
肾脏的钠排泄随饮食钠摄入而变化。我们进行了一项系统研究,以研究饮食盐摄入量对肾小球滤过率 (GFR) 和管状钠重吸收的影响。我们检查了在低钠饮食 (LSD) 中接受 7 天饮食的小鼠的肾脏适应反应,该饮食含有 0.01%的钠,在正常钠饮食 (NSD) 中含有 0.18%的钠,在中等高钠饮食 (HSD) 中含有 1.25%的钠。正如预期的那样,LSD 没有改变测量的 GFR,并且与 NSD 相比,增加了总蛋白和细胞表面 NHE3、NKCC2、NCC、α-ENaC 和裂解的 γ-ENaC 的丰度。数学模型预测,由于 Na 输送减少,近端小管的钠重吸收增加,但远端肾单位的钠重吸收减少。利尿剂对厚升支、远端卷曲小管或收集系统的靶向作用证实了这一预测。另一方面,HSD 没有改变测量的 GFR,但与 NSD 相比,降低了上述转运体的丰度。数学模型预测,由于 O 消耗的相对转运效率降低,近端小管的钠重吸收减少,但远端段的钠重吸收增加。利尿剂的利尿作用证实了这一预测。代谢传感器腺苷一磷酸激活蛋白激酶 (AMPK) 的活性与管状 Na 重吸收的变化有关。我们的数据表明,根据饮食钠摄入的不同,分数性钠重吸收分布不同,并引起管状 O 消耗和钠转运效率的变化。
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