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松弛素介导的清醒大鼠肾血管舒张、超滤及血浆渗透压变化的时间进程和剂量反应。

Time course and dose response of relaxin-mediated renal vasodilation, hyperfiltration, and changes in plasma osmolality in conscious rats.

作者信息

Danielson Lee A, Conrad Kirk P

机构信息

Magee-Womens Research Institute, 204 Craft Ave., Pittsburgh, PA 15213, USA.

出版信息

J Appl Physiol (1985). 2003 Oct;95(4):1509-14. doi: 10.1152/japplphysiol.00545.2003. Epub 2003 Jun 20.

DOI:10.1152/japplphysiol.00545.2003
PMID:12819218
Abstract

The pregnancy hormone relaxin elicits renal vasodilation, hyperfiltration, and osmoregulatory changes when chronically administered to conscious, nonpregnant rats. The objective in this study was to determine the dose response and time course of hormone action, as well as the time required for recovery on stopping its administration. The threshold dose of recombinant human relaxin (rhRLX) for renal vasodilation and reduction in plasma osmolality was 0.15 microg/h when given by subcutaneous osmotic minipump for 2 days (an infusion rate that achieved circulating levels of approximately 6 ng/ml). The peak response was observed during the 0.4 microg/h infusion rate (serum rhRLX of approximately 11 ng/ml), which was comparable to our previous work using a 4.0 microg/h (serum rhRLX of approximately 20 ng/ml). In contrast, a dose of 40 microg/h was ineffective (serum rhRLX of approximately 80 ng/ml). When 4.0 microg/h rhRLX was administered by osmotic minipump for shorter periods (</=24 h), renal circulatory and osmoregulatory changes were observed by </=6 h. After removal of the osmotic minipump, these changes persisted for at least 12 h, but they were fully restored by 24 h. Even briefer administration of 4.0 microg/h rhRLX by intravenous infusion showed an onset of action in the kidney by 1-2 h. In contrast, the 40 microg/h dose of rhRLX elicited minimal effects, and comparable to our earlier report, 4.0 microg/h purified porcine relaxin was also relatively ineffective during short-term intravenous administration. In conclusion, the effect of relaxin on the renal circulation and osmoregulation is biphasic, insofar as high doses are relatively inactive, and the onset of action is more rapid than previously believed. These findings may be important to consider when evaluating relaxin in the treatment of renal disease.

摘要

当长期给清醒的非妊娠大鼠注射妊娠激素松弛素时,会引起肾血管舒张、肾小球超滤及渗透调节变化。本研究的目的是确定激素作用的剂量反应和时间进程,以及停止给药后恢复所需的时间。通过皮下渗透微型泵给药2天,肾血管舒张和血浆渗透压降低的重组人松弛素(rhRLX)阈值剂量为0.15微克/小时(该输注速率可使循环水平达到约6纳克/毫升)。在0.4微克/小时的输注速率下观察到峰值反应(血清rhRLX约为11纳克/毫升),这与我们之前使用4.0微克/小时(血清rhRLX约为20纳克/毫升)的研究结果相当。相比之下,40微克/小时的剂量无效(血清rhRLX约为80纳克/毫升)。当通过渗透微型泵以较短时间(≤24小时)给予4.0微克/小时的rhRLX时,在≤6小时时观察到肾循环和渗透调节变化。移除渗透微型泵后,这些变化持续至少12小时,但在24小时时完全恢复。即使通过静脉输注更短时间给予4.0微克/小时的rhRLX,在1 - 2小时时肾脏也出现了作用起效。相比之下,40微克/小时的rhRLX剂量产生的影响最小,并且与我们早期的报告一致,4.0微克/小时的纯化猪松弛素在短期静脉给药期间也相对无效。总之,松弛素对肾循环和渗透调节的作用是双相的,因为高剂量相对无活性,并且作用起效比之前认为的更快。在评估松弛素治疗肾脏疾病时,这些发现可能具有重要的参考价值。

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Time course and dose response of relaxin-mediated renal vasodilation, hyperfiltration, and changes in plasma osmolality in conscious rats.松弛素介导的清醒大鼠肾血管舒张、超滤及血浆渗透压变化的时间进程和剂量反应。
J Appl Physiol (1985). 2003 Oct;95(4):1509-14. doi: 10.1152/japplphysiol.00545.2003. Epub 2003 Jun 20.
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