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首页> 外文期刊>American Journal of Physiology >Biphasic effects of ANP infusion in conscious, euvolumic rats: roles of AQP2 and ENaC trafficking.
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Biphasic effects of ANP infusion in conscious, euvolumic rats: roles of AQP2 and ENaC trafficking.

机译:ANP输注对有意识的,正常体质大鼠的双相影响:AQP2和ENaC贩运的作用。

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摘要

Atrial natriuretic peptide (ANP) acutely promotes water and sodium excretion, whereas subchronic effects involve water retention. Renal hemodynamics, water and sodium excretion, and aquaporin-2 (AQP2) and epithelial Na channel (ENaC) subcellular trafficking were determined in response to continuous ANP infusion in conscious rats, where body sodium and fluid balance was constantly maintained. ANP (0.5 microg x kg(-1) x min(-1)) evoked a transient (peak at 10 min) fivefold diuresis followed by reduced urine production to control levels (30- to 90-min period). The fractional distal water excretion was significantly increased initially and then decreased in response to ANP. There was no change in the subcellular localization of AQP2 and AQP2 phosphorylated in PKA consensus site S256 (p-AQP2) 10 min after ANP infusion. In contrast, after 90 min a marked increase in apical labeling of AQP2 and p-AQP2 was observed in the inner and outer medullary collecting ducts but not in cortical collecting ducts. In support of this, ANP induced plasma membrane targeting of AQP2 in transiently AQP2-transfected cells. ANP infusion evoked an instant increase in renal sodium excretion, which persisted for 90 min. Ten minutes of ANP infusion induced no changes in the subcellular localization of ENaC subunits, whereas a marked increase in apical targeting of alpha- and gamma-subunits was observed after 90 min. In conclusion, 1) ANP infusion induced a sustained natriuresis and transient diuresis; 2) there were no changes in the subcellular localization of AQP2 and ENaC subunits after 10 min of ANP infusion; and 3) there was a marked increase in apical targeting of AQP2, p-AQP2, and alpha- and gamma-ENaC after 90 min of ANP infusion. The increased targeting of ENaC and AQP2 likely represents direct or compensatory effects to increase sodium and water reabsorption and to prevent volume depletion in response to prolonged ANP infusion.
机译:心钠素(ANP)会迅速促进水和钠的排泄,而亚慢性影响则涉及保水。在有意识的大鼠中,通过持续的ANP输注来确定肾脏的血流动力学,水和钠的排泄以及aquaporin-2(AQP2)和上皮Na通道(ENaC)的亚细胞运输,并持续维持体内钠和液体的平衡。 ANP(0.5 microg x kg(-1)x min(-1))引起短暂的五倍利尿(在10分钟达到峰值),随后尿量减少到控制水平(30至90分钟)。响应ANP,远端远侧排泄分数最初显着增加,然后下降。 ANP输注后10分钟,在PKA共有位点S256(p-AQP2)中磷酸化的AQP2和AQP2的亚细胞定位没有变化。相反,在90分钟后,在内侧和外侧的髓收集管中观察到AQP2和p-AQP2的顶端标记显着增加,而在皮质收集管中则未观察到。支持这一点的是,ANP在瞬时AQP2转染的细胞中诱导了AQP2的质膜靶向。 ANP输注引起肾钠排泄立即增加,持续90分钟。十分钟的ANP输注不会引起ENaC亚基亚细胞定位的任何变化,而90分钟后观察到α-和gamma亚基的根尖靶向显着增加。结论:1)ANP输注引起持续性利尿和短暂性利尿。 2)ANP输注10分钟后,AQP2和ENaC亚基的亚细胞定位没有变化; 3)ANP输注90分钟后,AQP2,p-AQP2以及α-和γ-ENaC的根尖靶向明显增加。 ENaC和AQP2靶向性的提高可能代表直接或补偿性作用,以增加钠和水的重吸收并防止ANP长时间输注引起体液消耗。

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