膳食阴离子控制钾的排泄:它不仅仅是一种吸收不良的阴离子效应。

IF 3.7 2区 医学 Q1 PHYSIOLOGY American Journal of Physiology-renal Physiology Pub Date : 2023-09-01 Epub Date: 2023-07-27 DOI:10.1152/ajprenal.00193.2023
Lama Al-Qusairi, Mohammed Z Ferdaus, Truyen D Pham, Dimin Li, P Richard Grimm, Ava M Zapf, Delaney C Abood, Ebrahim Tahaei, Eric Delpire, Susan M Wall, Paul A Welling
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引用次数: 0

摘要

尿钾(K+)排泄机制随着膳食K+的增加而上调,但伴随的膳食阴离子的作用仍不充分。可吸收性差的阴离子,包括[公式:见正文],被认为通过跨上皮电压效应增加K+分泌。在这里,我们测试了它们是否也影响K+分泌机制。将野生型小鼠、醛固酮合成酶(AS)敲除(KO)小鼠或pendrin KO小鼠随机分为对照、高KCl或高KHCO3饮食。在平衡实验中评估K+分泌能力。通过蛋白质印迹分析和共聚焦显微镜评估K+分泌转运蛋白的蛋白质丰度、修饰和定位。与高KCl饮食相比,喂食高KHCO3饮食显著增加了尿K+排泄和肾小管K+梯度,与上皮Na+通道(ENaC)和肾髓质外K+通道(ROMK)的更显著上调以及远端肾单位的顶端定位一致。在AS KO小鼠中进行的实验表明,[配方:见正文]的增强作用与醛固酮无关。高KHCO3饮食还独特地增加了大电导Ca2+激活的K+(BK)通道β4-亚单位,稳定了顶端膜上的BKα、Cl-/[公式:见正文]交换体、pendrin和顶端KCl协同转运蛋白(KCC3a),所有这些都在pendrin阳性插入细胞中特异性表达。在pendrin KO小鼠中的实验表明,高KHCO3饮食需要pendrin来增加K+排泄。总之,[公式:见正文]刺激K+排泄,超过吸收不良的阴离子效应,上调主细胞中的ENaC和ROMK,上调pendrin阳性插入细胞中的BK、pendrin和KCC3a。该适应机制通过食用富含碱性灰分的饮食来预防高钾血症和碱中毒,但可能会导致碱中毒中的K+消耗和低钾血症。新的和值得注意的膳食阴离子深刻影响K+稳态。在这里,我们发现富含K+的饮食,含有[公式:见正文]作为抗衡离子,比高KCl饮食更能增强发电K+排泄机制、上皮Na+通道和肾髓质外K+通道。它还在B插入细胞中独特地诱导KCC3a和pendrin,提供电中性KHCO3分泌途径。这些发现揭示了新的K+平衡机制,驱动对碱性和富含K+的食物的适应,这应该指导K+疾病的新治疗策略。
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Dietary anions control potassium excretion: it is more than a poorly absorbable anion effect.

The urinary potassium (K+) excretion machinery is upregulated with increasing dietary K+, but the role of accompanying dietary anions remains inadequately characterized. Poorly absorbable anions, including [Formula: see text], are thought to increase K+ secretion through a transepithelial voltage effect. Here, we tested if they also influence the K+ secretion machinery. Wild-type mice, aldosterone synthase (AS) knockout (KO) mice, or pendrin KO mice were randomized to control, high-KCl, or high-KHCO3 diets. The K+ secretory capacity was assessed in balance experiments. Protein abundance, modification, and localization of K+-secretory transporters were evaluated by Western blot analysis and confocal microscopy. Feeding the high-KHCO3 diet increased urinary K+ excretion and the transtubular K+ gradient significantly more than the high-KCl diet, coincident with more pronounced upregulation of epithelial Na+ channels (ENaC) and renal outer medullary K+ (ROMK) channels and apical localization in the distal nephron. Experiments in AS KO mice revealed that the enhanced effects of [Formula: see text] were aldosterone independent. The high-KHCO3 diet also uniquely increased the large-conductance Ca2+-activated K+ (BK) channel β4-subunit, stabilizing BKα on the apical membrane, the Cl-/[Formula: see text] exchanger, pendrin, and the apical KCl cotransporter (KCC3a), all of which are expressed specifically in pendrin-positive intercalated cells. Experiments in pendrin KO mice revealed that pendrin was required to increase K+ excretion with the high-KHCO3 diet. In summary, [Formula: see text] stimulates K+ excretion beyond a poorly absorbable anion effect, upregulating ENaC and ROMK in principal cells and BK, pendrin, and KCC3a in pendrin-positive intercalated cells. The adaptive mechanism prevents hyperkalemia and alkalosis with the consumption of alkaline ash-rich diets but may drive K+ wasting and hypokalemia in alkalosis.NEW & NOTEWORTHY Dietary anions profoundly impact K+ homeostasis. Here, we found that a K+-rich diet, containing [Formula: see text] as the counteranion, enhances the electrogenic K+ excretory machinery, epithelial Na+ channels, and renal outer medullary K+ channels, much more than a high-KCl diet. It also uniquely induces KCC3a and pendrin, in B-intercalated cells, providing an electroneutral KHCO3 secretion pathway. These findings reveal new K+ balance mechanisms that drive adaption to alkaline and K+-rich foods, which should guide new treatment strategies for K+ disorders.

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来源期刊
CiteScore
8.40
自引率
7.10%
发文量
154
审稿时长
2-4 weeks
期刊介绍: The American Journal of Physiology - Renal Physiology publishes original manuscripts on timely topics in both basic science and clinical research. Published articles address a broad range of subjects relating to the kidney and urinary tract, and may involve human or animal models, individual cell types, and isolated membrane systems. Also covered are the pathophysiological basis of renal disease processes, regulation of body fluids, and clinical research that provides mechanistic insights. Studies of renal function may be conducted using a wide range of approaches, such as biochemistry, immunology, genetics, mathematical modeling, molecular biology, as well as physiological and clinical methodologies.
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