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抗利尿激素对锂作为近端小管输送标志物的影响。

Effect of antidiuretic hormone on lithium as a marker for proximal tubule delivery.

作者信息

Kirchner K A

机构信息

Department of Medicine, University of Mississippi Medical Center, Jackson 39216-4505.

出版信息

Am J Physiol. 1989 Nov;257(5 Pt 2):F899-906. doi: 10.1152/ajprenal.1989.257.5.F899.

Abstract

To determine whether acute changes in antidiuretic hormone (ADH) alter the ability of lithium to quantitatively reflect proximal delivery, fractional lithium excretion (CLi/CIn) and late proximal (TF/P)In determined by micropuncture were measured in sodium-loaded rats following administration of desamino-8-D-arginine vasopressin (dDAVP) at rates equivalent to approximately half-maximal (20 pg/min) and maximal (40 pg/min) plasma levels of endogenous hormone. dDAVP dissociated the linear correlation between CLi/CIn and 1/(TF/P)In (r = 0.05) usually observed in sodium-loaded rats. Proximal delivery determined by lithium clearance underestimated (P less than 0.001) values obtained by micropuncture. Amiloride restored the linear correlation between CLi/CIn and 1/(TF/P)In in sodium-loaded dDAVP-treated rats (r = 0.70) and quantitative estimates of proximal delivery by each technique became equivalent. Indomethacin also reduced (P less than 0.001) estimates of proximal delivery obtained by lithium techniques in sodium-loaded rats. Water loading in hydropenic rats restored concordance between estimates of proximal delivery obtained by lithium clearance and micropuncture methods. Thus changes in ADH markedly alter the ability of lithium to function as a quantitative marker for proximal delivery. Furthermore, ADH may increase lithium uptake at distal nephron sites by an amiloride-sensitive pathway.

摘要

为了确定抗利尿激素(ADH)的急性变化是否会改变锂定量反映近端输送的能力,在给予去氨基-8-D-精氨酸血管加压素(dDAVP)后,对钠负荷大鼠进行微穿刺测定其锂排泄分数(CLi/CIn)和晚期近端(TF/P)In,给药速率相当于内源性激素血浆水平的大约半数最大(20 pg/min)和最大(40 pg/min)。dDAVP使钠负荷大鼠中通常观察到的CLi/CIn与1/(TF/P)In之间的线性相关性解离(r = 0.05)。通过锂清除率测定的近端输送低估了(P小于0.001)微穿刺获得的值。氨氯地平恢复了钠负荷dDAVP处理大鼠中CLi/CIn与1/(TF/P)In之间的线性相关性(r = 0.70),并且每种技术对近端输送的定量估计变得等效。吲哚美辛也降低了(P小于0.001)钠负荷大鼠中锂技术获得的近端输送估计值。水负荷大鼠中的水负荷恢复了锂清除率和微穿刺方法获得的近端输送估计值之间的一致性。因此,ADH的变化显著改变了锂作为近端输送定量标志物的功能。此外,ADH可能通过氨氯地平敏感途径增加远端肾单位部位的锂摄取。

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