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环磷酸腺苷是一种肝肾联系物,影响钠利尿,并促成大鼠体内胰高血糖素诱导的超滤过。

Cyclic AMP is a hepatorenal link influencing natriuresis and contributing to glucagon-induced hyperfiltration in rats.

作者信息

Ahloulay M, Déchaux M, Hassler C, Bouby N, Bankir L

机构信息

INSERM Unité 90, Hôpital Necker-Enfants Malades, Paris, France.

出版信息

J Clin Invest. 1996 Nov 15;98(10):2251-8. doi: 10.1172/JCI119035.

Abstract

The effects of glucagon (G) on proximal tubule reabsorption (PTR) and GFR seem to depend on a prior action of this hormone on the liver resulting in the liberation of a mediator and/or of a compound derived from amino acid metabolism. This study investigates in anesthetized rats the possible contribution of cAMP and urea, alone and in combination with a low dose of G, on phosphate excretion (known to depend mostly on PTR) and GFR. After a 60-min control period, cAMP (5 nmol/min x 100 grams of body weight [BW]) or urea (2.5 micromol/min x 100 grams BW) was infused intravenously for 200 min with or without G (1.2 ng/min x 100 grams BW, a physiological dose which, alone, does not influence PTR or GFR). cAMP increased markedly the excretion of phosphate and sodium (+303 and +221%, respectively, P < 0.01 for each) but did not alter GFR. Coinfusion of cAMP and G induced the same tubular effects but also induced a 20% rise in GFR (P < 0.05). Infusion of urea, with or without G, did not induce significant effects on PTR or GFR. After G infusion at increasing doses, the increase in fractional excretion of phosphate was correlated with a simultaneous rise in plasma cAMP concentration and reached a maximum for doubling of plasma cAMP. These results suggest that cAMP, normally released by the liver into the blood under the action of G, (a) is probably an essential hepatorenal link regulating the intensity of PTR, and (b) contributes, in conjunction with specific effects of G on the nephron, to the regulation of GFR.

摘要

胰高血糖素(G)对近端肾小管重吸收(PTR)和肾小球滤过率(GFR)的影响似乎取决于该激素先作用于肝脏,从而导致一种介质和/或一种源自氨基酸代谢的化合物的释放。本研究在麻醉大鼠中探究了单独及与低剂量G联合使用时,环磷酸腺苷(cAMP)和尿素对磷酸盐排泄(已知主要取决于PTR)和GFR的可能作用。在60分钟的对照期后,静脉输注cAMP(5纳摩尔/分钟×100克体重[BW])或尿素(2.5微摩尔/分钟×100克BW),持续200分钟,输注过程中有无G(1.2纳克/分钟×100克BW,这是一个生理剂量,单独使用时不影响PTR或GFR)。cAMP显著增加了磷酸盐和钠的排泄(分别增加303%和221%,P均<0.01),但未改变GFR。cAMP与G联合输注产生了相同的肾小管效应,同时还使GFR升高了20%(P<0.05)。输注尿素,无论有无G,对PTR或GFR均未产生显著影响。在以递增剂量输注G后,磷酸盐排泄分数的增加与血浆cAMP浓度的同时升高相关,并且在血浆cAMP加倍时达到最大值。这些结果表明,正常情况下在G作用下由肝脏释放到血液中的cAMP,(a)可能是调节PTR强度的重要肝肾联系,(b)与G对肾单位的特定作用一起,有助于调节GFR。

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