Department of Anesthesiology, Vanderbilt University School of Medicine, Nashville, Tennessee, United States.
Division of Nephrology, Department of Medicine, Vanderbilt University School of Medicine, Nashville, Tennessee, United States.
Am J Physiol Renal Physiol. 2024 Sep 1;327(3):F373-F385. doi: 10.1152/ajprenal.00101.2024. Epub 2024 Jul 4.
Dietary potassium deficiency causes stimulation of sodium reabsorption leading to an increased risk in blood pressure elevation. The distal convoluted tubule (DCT) is the main rheostat linking plasma K levels to the activity of the Na-Cl cotransporter (NCC). This occurs through basolateral membrane potential sensing by inwardly rectifying K channels (Kir4.1/5.1); decrease in intracellular Cl; activation of WNK4 and interaction and phosphorylation of STE20/SPS1-related proline/alanine-rich kinase (SPAK); binding of calcium-binding protein 39 (cab39) adaptor protein to SPAK, leading to its trafficking to the apical membrane; and SPAK binding, phosphorylation, and activation of NCC. As kidney-specific with-no-lysine kinase 1 (WNK1) isoform (KS-WNK1) is another participant in this pathway, we examined its function in NCC regulation. We eliminated KS-WNK1 specifically in the DCT and demonstrated increased expression of WNK4 and long WNK1 (L-WNK1) and increased phosphorylation of NCC. As in other KS-WNK1 models, the mice were not hyperkalemic. Although wild-type mice under low-dietary K conditions demonstrated increased NCC phosphorylation, the phosphorylation levels of the transporter, already high in KS-WNK1, did not change under the low-K diet. Thus, in the absence of KS-WNK1, the transporter lost its sensitivity to low plasma K. We also show that under low K conditions, in the absence of KS-WNK1, there was no formation of WNK bodies. These bodies were observed in adjacent segments, not affected by the targeting of KS-WNK1. As our data are overall consistent with those of the global KS-WNK1 knockout, they indicate that the DCT is the predominant segment affecting the salt transport regulated by KS-WNK1. In this paper, we show that KS-WNK1 is a critical component of the distal convoluted tubule (DCT) K switch pathway. Its deletion results in an inability of the DCT to sense changes in plasma potassium. Absence of KS-WNK1 leads to abnormally high levels of WNK4 and L-WNK1 in the DCT, resulting in increased Na-Cl phosphorylation and function. Our data are consistent with KS-WNK1 targeting WNK4 and L-WNK1 to degradation.
饮食钾缺乏会刺激钠重吸收,导致血压升高的风险增加。远曲小管(DCT)是将血浆 K 水平与 Na-Cl 共转运蛋白(NCC)活性联系起来的主要变阻器。这是通过内向整流钾通道(Kir4.1/5.1)感应基底外侧膜电位来实现的;细胞内 Cl 减少;WNK4 激活以及 STE20/SPS1 相关脯氨酸/丙氨酸丰富激酶(SPAK)的相互作用和磷酸化;钙结合蛋白 39(cab39)衔接蛋白与 SPAK 的结合,导致其转运到顶膜;以及 SPAK 结合、磷酸化和 NCC 的激活。由于肾特异性无赖氨酸激酶 1(WNK1)同工型(KS-WNK1)也是该途径的参与者,我们研究了其在 NCC 调节中的作用。我们特异性地在 DCT 中消除了 KS-WNK1,并证实 WNK4 和长 WNK1(L-WNK1)的表达增加,并且 NCC 的磷酸化增加。与其他 KS-WNK1 模型一样,这些小鼠没有高钾血症。尽管在低钾饮食条件下,野生型小鼠表现出 NCC 磷酸化增加,但在低钾饮食条件下,已经处于高 KS-WNK1 的转运体的磷酸化水平没有变化。因此,在没有 KS-WNK1 的情况下,转运体失去了对低血浆 K 的敏感性。我们还表明,在低钾条件下,在没有 KS-WNK1 的情况下,没有形成 WNK 体。这些体现在相邻的节段中观察到,不受 KS-WNK1 靶向的影响。由于我们的数据总体上与全球 KS-WNK1 敲除的结果一致,因此它们表明 DCT 是影响 KS-WNK1 调节的盐转运的主要节段。在本文中,我们表明 KS-WNK1 是远曲小管(DCT)K 开关途径的关键组成部分。其缺失导致 DCT 无法感知血浆钾的变化。KS-WNK1 的缺失导致 DCT 中 WNK4 和 L-WNK1 的水平异常升高,导致 Na-Cl 磷酸化和功能增加。我们的数据与 KS-WNK1 靶向 WNK4 和 L-WNK1 进行降解的结果一致。
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