Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion.

Sorensen MV; Matos JE; Sausbier M; Sausbier U; Ruth P; Praetorius HA; Leipziger J

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Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion.

机译：醛固酮增加KCa1.1（BK）通道介导的结肠K +分泌。

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Mammalian K(+) homeostasis results from highly regulated renal and intestinal absorption and secretion, which balances the unregulated K(+) intake. Aldosterone is known to enhance both renal and colonic K(+) secretion. In mouse distal colon K(+) secretion occurs exclusively via luminal K(Ca)1.1 (BK) channels. Here we investigate if aldosterone stimulates colonic K(+) secretion via BK channels. Luminal Ba(2+) and iberiotoxin (IBTX)-sensitive electrogenic K(+) secretion was measured in Ussing chambers. In vivo aldosterone was augmented via a high K(+) diet. High K(+) diet led to a 2-fold increase of luminal Ba(2+) and IBTX-sensitive short-circuit current in distal mouse colonic mucosa. This effect was absent in BK alpha-subunit-deficient (BK(-/-)) mice. The resting and diet-induced K(+) secretion was stimulated by luminal ionomycin. In BK(-/-) mice luminal ionomycin did not stimulate K(+) secretion. In vitro addition of aldosterone likewise triggered a 2-fold increase in K(+) secretion, which was inhibited by the mineralocorticoid receptor antagonist spironolactone and the BK channel blocker IBTX. Semi-quantification of mRNA from colonic crypts showed up-regulation of BK alpha- and beta(2)-subunits in high K(+) diet mice. The BK channel could be detected luminally in colonic crypt cells by immunohistochemistry. The expression level of the channel in the luminal membrane was strongly up-regulated in K(+)-loaded animals. Taken together, these data strongly suggest that aldosterone-induced K(+) secretion occurs via increased expression of luminal BK channels.

机译：哺乳动物的K（+）体内稳态是由高度调节的肾脏和肠道吸收与分泌引起的，从而平衡了不受调节的K（+）摄入量。已知醛固酮可以增强肾脏和结肠的K（+）分泌。在小鼠远端结肠K（+）分泌仅通过腔K（Ca）1.1（BK）通道发生。在这里，我们调查醛固酮是否通过BK通道刺激结肠K（+）分泌。在Ussing室中测量了发光Ba（2+）和纤维毒素（IBTX）敏感的电原性K（+）分泌。体内醛固酮通过高K（+）饮食增加。高K（+）饮食导致远端小鼠结肠粘膜中腔Ba（2+）和IBTX敏感的短路电流增加2倍。在BK alpha亚基缺陷（BK（-/-））小鼠中没有这种效果。腔离子霉素可刺激静息和饮食诱导的K（+）分泌。在BK（-/-）小鼠腔离子霉素不刺激K（+）分泌。体外添加醛固酮同样会引起K（+）分泌增加2倍，这被盐皮质激素受体拮抗剂螺内酯和BK通道阻滞剂IBTX抑制。从结肠隐窝的mRNA的半定量显示高K（+）饮食小鼠中BK alpha-和beta（2）-亚基的上调。 BK通道可以通过免疫组织化学在结肠隐窝细胞中进行发光检测。在K（+）负载的动物中，腔膜中通道的表达水平强烈上调。综上所述，这些数据强烈表明醛固酮诱导的K（+）分泌是通过增加腔BK通道的表达而发生的。

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《The Journal of Physiology》 |2008年第17期|共14页
作者
Sorensen MV; Matos JE; Sausbier M; Sausbier U; Ruth P; Praetorius HA; Leipziger J;
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正文语种 eng
中图分类人体生理学;
关键词
Process of secretion; Laboratory mice; large-conductance calcium-activated potassium channel; 膳食;

机译：分泌过程;实验室小鼠;大电导钙激活钾通道;代谢;

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专利

1. Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion. [J] . Sorensen MV, Matos JE, Sausbier M, The Journal of Physiology . 2008,第17期

机译：醛固酮增加KCa1.1（BK）通道介导的结肠K +分泌。
2. Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion. [J] . Sorensen MV, Matos JE, Sausbier M, The Journal of Physiology . 2008,第Pta17期

机译：醛固酮增加KCa1.1（BK）通道介导的结肠K +分泌。
3. Adrenaline-induced colonic K+ secretion is mediated by KCa1.1 (BK) channels. [J] . Sorensen MV, Sausbier M, Ruth P, The Journal of Physiology . 2010,第10期

机译：肾上腺素诱导的结肠K +分泌是由KCa1.1（BK）通道介导的。
4. Enhancing 802.11ac Dynamic Access method for Increasing the Throughput of Low Priority Access Categories BK and BE [C] . Souhila Mammeri, Mohand Yazid, Louiza Bouallouche-Medjkoune, International Symposium on Networks, Computers and Communications . 2018

机译：增强802.11ac动态访问方法以提高低优先级访问类别BK和BE的吞吐量
5. The colonic (HKalpha2) H+,K+ ATPase and the effects of aldosterone in the kidney. [D] . Gumz, Michelle L. 2004

机译：结肠中的（HKalpha2）H +，K + ATPase和醛固酮在肾脏中的作用。
6. Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion [O] . Mads V Sørensen, Joana E Matos, Matthias Sausbier, 2008

机译：醛固酮增加KCa1.1（BK）通道介导的结肠K +分泌
7. Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion [O] . Sørensen, Mads V, Matos, Joana E, Sausbier, Matthias, 2008

机译：醛固酮增加KCa1.1（BK）通道介导的结肠K +分泌

Aldosterone increases KCa1.1 (BK) channel-mediated colonic K+ secretion.

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