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Central inhibition of salt appetite by oxytocin in rats.

机译:催产素对大鼠食盐的中枢抑制作用。

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Considerable evidence indicates an important role of hormones in the stimulation of fluid consumption. For example, angiotensin II (Ang II), together with afferent neural input from cardiovascular baroreceptors, is well known to stimulate thirst and NaCl intake in rats. Conversely, numerous studies have demonstrated that central oxytocin (OT) provides a stimulus for inhibition of salt appetite. The latter conclusion is supported by the following observations in rats: (a) intracerebroventricular (i.c.v.) injection of OT inhibits salt appetite stimulated by subcutaneous colloid; (b) treatments that inhibit NaCl intake, such as acute hyperosmolality, stimulate pituitary secretion of OT (which is correlated with central release of OT in these studies), whereas treatments that decrease OT secretion, such as systemic injection of deoxycorticosterone and dietary sodium deprivation, potentiate Ang-II-induced NaCl intake; (c) systemic ethanol administration inhibits OT secretion and enhances Ang-II-induced saltappetite; (d) naloxone, which augments stimulated OT secretion, inhibits NaCl appetite induced by colloid treatment, an effect that is abolished by i.c.v. pretreatment with an OT receptor antagonist; and (e) destruction of central neurons bearing OT receptors increases Ang II-induced salt appetite. By mediating the inhibition of NaCl intake in rats, central OT complements the known peripheral effects of OT to facilitate renal sodium excretion.
机译:大量证据表明激素在刺激体液消耗中起重要作用。例如,众所周知,血管紧张素II(Ang II)与心血管压力感受器的传入神经输入一起刺激大鼠的口渴和NaCl摄入。相反,许多研究表明,中央催产素(OT)可以刺激食欲。在大鼠中的以下观察结果支持了后一个结论:(a)脑室内(i.c.v.)注射OT抑制皮下胶体刺激的食欲。 (b)抑制NaCl摄入的治疗(例如急性高渗性)会刺激OT的垂体分泌(在这些研究中与OT的中央释放有关),而降低OT分泌的治疗(例如全身注射脱氧皮质酮和饮食中的钠缺乏) ,增强Ang-II诱导的NaCl摄入; (c)全身性乙醇给药抑制OT分泌并增强Ang-II诱导的食欲; (d)纳洛酮,其增加刺激的OT分泌,抑制由胶体处理诱导的NaCl食欲,这种作用被静脉内消除。用OT受体拮抗剂预处理; (e)破坏带有OT受体的中枢神经元会增加Ang II诱导的食欲。通过介导大鼠对NaCl摄入的抑制,中枢性OT补充了OT的已知外周效应,以促进肾脏钠排泄。

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