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出生后发育过程中皮质类固醇对大鼠远端结肠钠钾转运的调节作用

Corticosteroid regulation of Na+ and K+ transport in the rat distal colon during postnatal development.

作者信息

Pácha J, Popp M, Capek K

机构信息

Czechoslovak Academy of Sciences, Institute of Physiology, Videnska.

出版信息

J Dev Physiol. 1988 Dec;10(6):531-40.

PMID:3246545
Abstract

To study the role of corticosteroids in the regulation of colonic electrogenic amiloride-sensitive Na+ absorption (ISCNa) and barium-sensitive K+ secretion (ISCK) during development, we investigated suckling (10-day old), weanling (25-day old) and adult (90-day old) adrenalectomized rats after they had received aldosterone, dexamethasone or corticosterone. Adrenalectomy reduced markedly ISCNa in suckling rats and completely inhibited ISCNa in weanling animals; the ISCNa was absent in intact adult rats. The doses of aldosterone, corticosterone and dexamethasone estimated to be equivalent to the endogenous production rate of aldosterone and corticosterone restored ISCNa after 1 day in both suckling and weanling rats. Compared with aldosterone, glucocorticoids produced a greater increase in ISCNa. Concurrent spironolactone treatment (a mineralocorticoid antagonist) completely prevented the effect of aldosterone but had no effect in dexamethasone-treated rats. The glucocorticoid antagonist RU 38 486 inhibited the dexamethasone-induction of ISCNa but had no effect on aldosterone. The response to corticosteroids, measured as the increase of ISCNa, declined from suckling to adult rats. In contrast to ISCNa, the same time of treatment and the same doses of corticosteroids did not influence ISCK. ISCK was stimulated only after chronic treatment (4 days). These findings suggest that, in the distal colon of young rats, (1) both corticosteroids may regulate amiloride-sensitive Na+ absorption and barium-sensitive K+ secretion, (2) different receptors mediate the colonic effects of glucocorticoids and mineralocorticoids, (3) immature rats are more sensitive to corticosteroids than adult animals, and (4) the acute effect of corticosteroids is an increase in Na+ absorption which is followed by delayed stimulation of K+ secretion.

摘要

为研究皮质类固醇在发育过程中对结肠电生性氨氯地平敏感的Na⁺吸收(ISCNa)和钡敏感的K⁺分泌(ISCK)的调节作用,我们对10日龄哺乳、25日龄断奶和90日龄成年的肾上腺切除大鼠给予醛固酮、地塞米松或皮质酮后进行了研究。肾上腺切除显著降低了哺乳大鼠的ISCNa,并完全抑制了断奶动物的ISCNa;成年大鼠完整时不存在ISCNa。估计相当于醛固酮和皮质酮内源性产生速率的醛固酮、皮质酮和地塞米松剂量,在哺乳和断奶大鼠中1天后恢复了ISCNa。与醛固酮相比,糖皮质激素使ISCNa增加得更多。同时给予螺内酯治疗(一种盐皮质激素拮抗剂)完全阻止了醛固酮的作用,但对地塞米松治疗的大鼠没有影响。糖皮质激素拮抗剂RU 38 486抑制地塞米松诱导的ISCNa,但对醛固酮没有影响。以ISCNa增加来衡量的对皮质类固醇的反应,从哺乳大鼠到成年大鼠逐渐下降。与ISCNa相反,相同的治疗时间和相同剂量的皮质类固醇不影响ISCK。仅在慢性治疗(4天)后ISCK才受到刺激。这些发现表明,在幼鼠的远端结肠中,(1)两种皮质类固醇可能调节氨氯地平敏感的Na⁺吸收和钡敏感的K⁺分泌,(2)不同的受体介导糖皮质激素和盐皮质激素对结肠的作用,(3)未成熟大鼠比成年动物对皮质类固醇更敏感,(4)皮质类固醇的急性作用是增加Na⁺吸收,随后是延迟的K⁺分泌刺激。

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