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通过钙敏感受体的新型生理和药理激活剂激活肾脏钙和水排泄。

Activation of renal calcium and water excretion by novel physiological and pharmacological activators of the calcium-sensing receptor.

作者信息

Conigrave Arthur D, Lok Hiu Chuen

机构信息

School of Molecular and Microbial Biosciences, University of Sydney, Sydney, New South Wales, Australia.

出版信息

Clin Exp Pharmacol Physiol. 2004 May-Jun;31(5-6):368-71. doi: 10.1111/j.1440-1681.2004.04000.x.

Abstract

Activated Ca(2+)-sensing receptors (CaR) play key roles in the regulation of whole-body calcium metabolism by inhibiting the secretion of the key calcitropic hormone parathyroid hormone and promoting urinary calcium excretion. We have now examined the effects of intravenous administration of novel calcium receptor activators on renal function in anaesthetized female Wistar rats. The type II calcimimetic NPS R-467 and the CaR-active amino acids l-Phe and l-Ala, which act at distinct binding sites on the receptor, all activated urinary flow rate, calcium and osmolar excretion and suppressed urinary osmolality. The effects of l-Phe and NPS R-467 on urine flow rate and calcium excretion were stereoselective, consistent with the idea that these effects were mediated by calcium-sensing receptors. However, d-Phe also suppressed urinary osmolality and promoted osmolar excretion, possibly by exceeding the transport maximum in the proximal tubule. The data indicate that novel activators of CaR, including l-amino acids at physiologically relevant serum concentrations, play a significant role in the regulation of urinary calcium and water excretion.

摘要

激活的钙敏感受体(CaR)通过抑制关键的促钙激素甲状旁腺激素的分泌和促进尿钙排泄,在全身钙代谢调节中发挥关键作用。我们现在研究了静脉注射新型钙受体激活剂对麻醉的雌性Wistar大鼠肾功能的影响。II型钙敏感受体激动剂NPS R-467以及作用于受体不同结合位点的CaR活性氨基酸L-苯丙氨酸和L-丙氨酸,均能激活尿流率、钙和渗透压排泄,并抑制尿渗透压。L-苯丙氨酸和NPS R-467对尿流率和钙排泄的影响具有立体选择性,这与这些作用是由钙敏感受体介导的观点一致。然而,D-苯丙氨酸也抑制尿渗透压并促进渗透压排泄,可能是通过超过近端小管的转运极限。数据表明,新型CaR激活剂,包括生理相关血清浓度的L-氨基酸,在尿钙和水排泄调节中起重要作用。

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