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自发性高血压大鼠的肾激肽释放酶活性

Renal kallikrein activity in rats developing spontaneous hypertension.

作者信息

Praddaude F, Tran-Van T, Ader J L

机构信息

Laboratory of Physiology, Medical School, Paul Sabatier University, Toulouse, France.

出版信息

Clin Sci (Lond). 1989 Mar;76(3):311-5. doi: 10.1042/cs0760311.

Abstract
  1. Spontaneously hypertensive rats (SHR) excrete less kallikrein in urine than Wistar-Kyoto rats (WKY) during the developmental phase of hypertension. The present study was designed to examine whether the urinary defect is related to abnormalities in the renal kallikrein content in this hypertensive model. 2. Active and total kallikrein were measured (amidolytic assay) in the renal cortex of newborn and 4-, 8- and 12-week-old SHR and age-matched WKY. Active and total kallikrein were also measured in urine at the same ages, except at birth. 3. Tissue active kallikrein was significantly lower in SHR at birth, representing on average 53% of the values in WKY expressed as content per total cortex weight. Tissue total kallikrein did not differ between newborn SHR and WKY. 4. SHR at 4, 8 and 12 weeks of age had lower urinary active and total kallikrein excretion. Tissue active akllikrein, but not total kallikrein, was higher than in age-matched WKY per g of cortex weight or per mg of protein, whereas both tissue active and total kallikrein were lower in SHR when expressed as content per total cortex weight. At these three ages, active kallikrein represented, on average 86%, while total kallikrein represented 77%, of the values in age-matched WKY. 5. Our results indicate a defect in prokallikrein activation rather than in kallikrein synthesis in the renal cortex of SHR at birth. The reduction in urinary kallikrein excretion during the developmental phase of hypertension in young SHR is similar to the reduction observed in the renal tissue.
摘要
  1. 在高血压发展阶段,自发性高血压大鼠(SHR)尿中激肽释放酶的排泄量比Wistar-Kyoto大鼠(WKY)少。本研究旨在探讨在该高血压模型中,尿缺陷是否与肾激肽释放酶含量异常有关。2. 采用酰胺水解法测定新生及4周、8周和12周龄SHR以及年龄匹配的WKY肾皮质中的活性和总激肽释放酶。除出生时外,还在相同年龄的尿中测定活性和总激肽释放酶。3. SHR出生时组织活性激肽释放酶显著降低,以每总皮质重量的含量表示,平均为WKY值的53%。新生SHR和WKY的组织总激肽释放酶无差异。4. 4周、8周和12周龄的SHR尿中活性和总激肽释放酶排泄量较低。每克皮质重量或每毫克蛋白质计算,组织活性激肽释放酶(而非总激肽释放酶)高于年龄匹配的WKY,而以每总皮质重量的含量表示时,SHR的组织活性和总激肽释放酶均较低。在这三个年龄,活性激肽释放酶平均占年龄匹配WKY值的86%,而总激肽释放酶占77%。5. 我们的结果表明,SHR出生时肾皮质中存在前激肽释放酶激活缺陷而非激肽释放酶合成缺陷。年轻SHR高血压发展阶段尿激肽释放酶排泄量的减少与肾组织中观察到的减少相似。

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