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大鼠实验性高血压及对18-羟基脱氧皮质酮治疗的其他反应

Experimental hypertension and other responses to 18-hydroxy-deoxycorticosterone treatment in the rat.

作者信息

Hall C E, Gomez-Sanchez C E, Holland O B, Nasseth D, Hall O

出版信息

Endocrinology. 1978 Jul;103(1):133-40. doi: 10.1210/endo-103-1-133.

Abstract

Young female unilaterally nephrectomized, salt-loaded, Sprague-Dawley rats were treated with 200 microgram or 1 mg 18-hydroxy-deoxycorticosterone-21-acetate (18-OH-DOCA) in oil daily, and a group of kidney-intact animals on a normal salt intake was given 2 mg/day. The hormone was not found to increase saline consumption, increase urinary potassium or kallikrein excretion, or depress serum renin activity or potassium concentration. Slight hypertension did develop at 3 weeks in salt-loaded rats on the lowest dose, but this was neither increased by higher dosage or longer treatment, nor reflected by increased heart or kidney weight. The effect of 40-mg pellet implantation of DOCA and 18-OH-DOCA was then compared in unilaterally nephrectomized, salt-loaded, female Fischer 344 rats. The former caused increased saline consumption, hypertension, hypokalemia, and heart and kidney enlargement, whereas 18-OH-DOCA did not. Thus, the hypertensogenic potency of 18-OH-DOCA is, at best, a reflection of its known, very weak, mineralocorticoid activity.

摘要

对年轻的单侧肾切除、盐负荷的雌性斯普拉格-道利大鼠,每日用油剂给予200微克或1毫克18-羟基脱氧皮质酮-21-乙酸酯(18-OH-DOCA),并对一组正常盐摄入的肾脏完整动物给予2毫克/天。未发现该激素增加盐水消耗、增加尿钾或激肽释放酶排泄,或降低血清肾素活性或钾浓度。在最低剂量下,盐负荷大鼠在3周时确实出现了轻微高血压,但更高剂量或更长疗程并未使其加重,心脏或肾脏重量增加也未反映出这一点。然后在单侧肾切除、盐负荷的雌性费希尔344大鼠中比较了40毫克DOCA和18-OH-DOCA丸剂植入的效果。前者导致盐水消耗增加、高血压、低钾血症以及心脏和肾脏增大,而18-OH-DOCA则没有。因此,18-OH-DOCA的致高血压效力充其量反映了其已知的非常微弱的盐皮质激素活性。

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