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前列腺素与肾脏

Prostaglandins and the kidney.

作者信息

Dunn M J, Hood V L

出版信息

Am J Physiol. 1977 Sep;233(3):169-84. doi: 10.1152/ajprenal.1977.233.3.F169.

Abstract

This review provides a summary and assessment of research involving renal prostaglandins. Arachidonic acid released from phospholipids is converted by prostaglandin cyclo-oxygenase in the kidney to PGF2, PGF2alpha, PGD2, and, possibly, to PGI2 and thromboxane A2. Production of PGE2 and PGF2alpha is predominately but not exclusively in the medulla, whereas degradative enzymes are present in both cortex and medulla. Prostaglandins enter the tubular lumen by facilitated transport and are partially reabsorbed from the urine in the distal nephron. Urine prostaglandins probably reflect renal synthesis. PGE2 and endoperoxides stimulate and PGF2alpha and indomethacin inhibit renal renin synthesis. In response to ischemia, vasoconstriction, or angiotensin II the kidney increases prostaglandin synthesis to modulate renal vascular resistance. In conscious animals or man no role has been established for prostaglandins in the maintenance of basal renal blood flow or renal sodium excretion. PGE influences renal water excretion by inhibiting the action vasopressin. Despite conflicting data there is evidence that renal prostaglandins are involved either primarily or secondarily in many types of hypertension. Inhibitors of prostaglandin cyclooxygenase have been used with success in Bartter's syndrome. Conflicting results in many areas of investigation may be resolved by the use of more accurate and reliable assays, careful handling of samples, and the use of urine to further investigate renal prostaglandin synthesis.

摘要

本综述对涉及肾前列腺素的研究进行了总结和评估。从磷脂释放的花生四烯酸在肾脏中被前列腺素环氧化酶转化为PGF2、PGF2α、PGD2,也可能转化为PGI2和血栓素A2。PGE2和PGF2α的产生主要但并非仅发生在髓质,而降解酶在皮质和髓质中均有存在。前列腺素通过易化转运进入肾小管腔,并在远端肾单位中部分从尿液中重吸收。尿前列腺素可能反映肾脏的合成情况。PGE2和内过氧化物刺激肾素合成,而PGF2α和吲哚美辛抑制肾素合成。对缺血、血管收缩或血管紧张素II的反应中,肾脏会增加前列腺素的合成以调节肾血管阻力。在清醒动物或人类中,尚未确定前列腺素在维持基础肾血流量或肾钠排泄中发挥作用。PGE通过抑制血管升压素的作用来影响肾水排泄。尽管数据存在矛盾,但有证据表明肾前列腺素主要或次要参与多种类型的高血压。前列腺素环氧化酶抑制剂已成功用于巴特综合征。通过使用更准确可靠的检测方法、小心处理样本以及利用尿液进一步研究肾前列腺素的合成,许多研究领域中相互矛盾的结果可能会得到解决。

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