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首页> 外文期刊>American Journal of Physiology >Functional role of NHE4 as a pH regulator in rat and human colonic crypts.
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Functional role of NHE4 as a pH regulator in rat and human colonic crypts.

机译:NHE4在大鼠和人类结肠隐窝中作为pH调节剂的功能作用。

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To regulate ionic and fluid homeostasis. the colon relies upon a series of Na~+-dependent transport proteins. Recent studies have identified a sodium/hydrogen exchanger (NHE) 4 (NHE4) protein in the gastrointestinal tract but to date there has been little description of its function. Additionally, we have previously shown that aldosterone can rapidly modulate Na~+-dependent proton excretion via NHE proteins. In this study we examined the role of NHE4 in rat and human colonic crypts, determined the effect of aldosterone on NHE4 specifically, and explored the intracellular pathways leading to activation. Colonic samples were dissected from Sprague-Dawley rats. Human specimens were obtained from patients undergoing elective colon resections. Crypts were isolated using ethylenediaminetetraacetic acid and intracellular pH (pHi) changes were monitored using 2'-7'-bis(carboxyethyl)-5(6)-carboxyfluorescein (BCECF). Crypts were exposed to 7 muM ethyl-isopropylamiloride or 400 muM amiloride, doses previously shown to inhibit NHE1 and NHE3 but allow NHE4 to remain active. Functional NHE4 activity was demonstrated in both rat and human colonic crypts. NHE4 activity was increased in the presence of 1 muM aldosterone. In the rat model, crypts were exposed to 100 muM 3-isobutyl-1-methylxanthine/1 muM forskolin and demonstrated a decrease in NHE4 activity with increased cAMP levels. No significant change in NHE4 activity was seen by increasing osmolarity. These results demonstrate functional NHE4 activity in the rat and human colon and an increase in activity by aldosterone. This novel exchanger is capable of modulating intracellular pH over a wide pH spectrum and may play an important role in maintaining cellular pH homeostasis.
机译:调节离子和流体稳态。结肠依赖于一系列Na +依赖性转运蛋白。最近的研究已经确定了胃肠道中的钠/氢交换剂(NHE)4(NHE4)蛋白,但迄今为止,对其功能的描述很少。另外,我们以前已经表明,醛固酮可以通过NHE蛋白快速调节Na〜+依赖的质子排泄。在这项研究中,我们检查了NHE4在大鼠和人类结肠隐窝中的作用,确定了醛固酮对NHE4的作用,并探讨了导致激活的细胞内途径。从Sprague-Dawley大鼠中解剖结肠样品。人体标本取自进行选择性结肠切除术的患者。使用乙二胺四乙酸分离地穴,并使用2'-7'-双(羧乙基)-5(6)-羧基荧光素(BCECF)监测细胞内pH(pHi)的变化。将地穴暴露于7μM乙基异丙基阿米洛利或400μM阿米洛利,这些剂量先前显示可抑制NHE1和NHE3,但允许NHE4保持活性。在大鼠和人类结肠隐窝中均证实了功能性NHE4活性。在1μM醛固酮存在下,NHE4活性增加。在大鼠模型中,隐窝暴露于100μM3-异丁基-1-甲基黄嘌呤/ 1μM毛喉素中,并显示出随着cAMP水平的升高,NHE4活性降低。通过增加渗透压,未观察到NHE4活性的显着变化。这些结果证明在大鼠和人结肠中功能性NHE4活性以及醛固酮的活性增加。这种新型的交换剂能够在很宽的pH谱范围内调节细胞内的pH值,并且在维持细胞的pH稳态中起着重要的作用。

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