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布拉格高血压大鼠(一种自发性高血压新模型)的肾脏内皮素系统

The renal endothelin system in the Prague hypertensive rat, a new model of spontaneous hypertension.

作者信息

Vogel V, Bäcker A, Heller J, Kramer H J

机构信息

Renal Section, Medical Policlinic, University of Bonn, Wilhelmstrasse 35-37, 53111 Bonn, Germany.

出版信息

Clin Sci (Lond). 1999 Jul;97(1):91-8.

Abstract

In a new model of spontaneous hypertension, namely the Prague hypertensive rat (PHR), hypertension is transferred with a kidney transplanted from the PHR to its normotensive counterpart (PNR) by an as yet unknown mechanism. One candidate may be endothelin (ET), since this potent vasoconstrictor affects vascular tone, renal haemodynamics and renal excretory function, and all members of this peptide family are located within the kidney and act in an autocrine/paracrine fashion. In the present study we investigated, in the renal tissue of PHRs and PNRs: (1) preproET-1 and preproET-3 mRNAs as well as ET-1 and ET-3 peptide distribution, (2) endothelin-converting enzyme (ECE)-1 mRNA expression, and (3) ET receptors and their characteristics in membranes of glomeruli and papillae. In addition, plasma ET concentration and urinary ET excretion were determined. Quantitative measurements by competitive reverse transcription-polymerase chain reaction revealed ET-1 mRNA levels in the renal cortex from PHRs and PNRs of 1.09+/-0.13 and 1. 29+/-0.18 amol/microgram of total RNA respectively, and in red medulla of 2.72+/-0.82 and 3.30+/-0.68 amol/microgram respectively. In contrast, renal papilla from PHRs showed significantly lower levels of preproET-1 mRNA (1.81+/-0.64 amol/microgram of total RNA, compared with 4.25+/-0.82 amol/microgram in PNRs; each n=5; P<0.05). The ET-1 peptide concentration in papillary tissue was also significantly lower in PHRs than in PNRs (120.2+/-30.8 and 491.3+/-53.4 fmol/mg of protein respectively; n=5; P<0.01), whereas it was similar in cortex and medulla from PHRs and PNRs. The preproET-3 mRNA content in renal tissue was much lower than that of preproET-1 mRNA. It was significantly higher in red medulla from PHRs compared with that from PNRs (0.25+/-0.05 and 0.13+/-0.02 amol/microgram of total RNA respectively; P<0.05), but was similar in papillae of PHRs and PNRs (0.04+/-0.02 and 0.05+/-0.01 amol/microgram respectively; n=5). Cortical preproET-3 mRNA was at the lower limit of detection. Similarly, the ET-3 peptide concentration was slightly but significantly higher in the red medulla of PHRs compared with PNRs (15.4+/-2.0 and 8.8+/-0.8 fmol/mg of protein respectively; n=5; P<0. 05), whereas no differences in ET-3 peptide concentration were found in papillae from PHRs and PNRs. ECE-1 mRNA levels were similar in the renal cortex, red medulla and papillae from PHRs and PNRs, ranging between 0.34+/-0.03 and 0.56+/-0.12 amol/microgram of total RNA. Of the total ET receptors in glomerular membranes, 39% were ETA receptors, whereas papillary membranes contained exclusively ETB receptors. PHRs and PNRs showed similar Bmax and Kd values for ET-1 in renal glomerular membranes (Bmax, 6.5+/-1.3 and 4.9+/-1.2 pmol/mg of protein respectively; Kd, 0.69+/-0.10 and 0.56+/-0.10 nM respectively) and papillary membranes (Bmax, 9.7+/-1.1 and 11.3+/-1. 6 pmol/mg of protein respectively; Kd, 0.30+/-0.04 and 0.42+/-0.07 nM respectively). Plasma ET-1/2 concentrations (10.4+/-1.3 and 12. 2+/-1.2 fmol/ml in PHRs and PNRs respectively) and urinary ET-1 excretion (3.1+/-0.3 and 3.0+/-0.2 pmol/24 h in PHRs and PNRs respectively) were similar in hypertensive and normotensive rats. In summary, although tissue levels of preproET-3 mRNA were very low in the kidney, significantly greater amounts of preproET-3 mRNA and ET-3 peptide were found in medullary tissue from PHRs compared with PNRs, a finding that awaits further investigation. In contrast, the preproET-1 mRNA content and ET-1 peptide concentration were significantly lower in papillary tissue from PHRs compared with PNRs. Decreased synthesis of ET-1, which normally antagonizes the action of [Arg8]vasopressin, may allow increased water (and sodium) reabsorption at the level of the inner medullary collecting duct. This intrinsic defect of the kidney in the PHR may contribute to hypertension in this model, and may transmit high blood pressure on transplantation of the 'hypertensive' kidney i

摘要

在一种新的自发性高血压模型,即布拉格高血压大鼠(PHR)中,高血压可通过一种尚不清楚的机制,由PHR的肾脏移植到其血压正常的对应物(PNR)而传递。一种可能的因素是内皮素(ET),因为这种强效血管收缩剂会影响血管张力、肾血流动力学和肾脏排泄功能,且该肽家族的所有成员都位于肾脏内,并以自分泌/旁分泌方式发挥作用。在本研究中,我们在PHR和PNR的肾组织中研究了:(1)前体ET-1和前体ET-3 mRNA以及ET-1和ET-3肽的分布,(2)内皮素转换酶(ECE)-1 mRNA的表达,以及(3)肾小球和乳头膜中的ET受体及其特性。此外,还测定了血浆ET浓度和尿ET排泄量。通过竞争性逆转录-聚合酶链反应进行的定量测量显示,PHR和PNR肾皮质中ET-1 mRNA水平分别为1.09±0.13和1.29±0.18 amol/μg总RNA,红髓中分别为2.72±0.82和3.30±0.68 amol/μg。相比之下,PHR的肾乳头前体ET-1 mRNA水平显著较低(1.81±0.64 amol/μg总RNA,而PNR为4.25±0.82 amol/μg;每组n = 5;P<0.05)。PHR乳头组织中的ET-1肽浓度也显著低于PNR(分别为120.2±30.8和491.3±53.4 fmol/mg蛋白质;n = 5;P<0.01),而PHR和PNR的皮质和髓质中则相似。肾组织中的前体ET-3 mRNA含量远低于前体ET-1 mRNA。与PNR相比,PHR红髓中的前体ET-3 mRNA显著更高(分别为0.25±0.05和0.13±0.02 amol/μg总RNA;P<0.05),但PHR和PNR乳头中的前体ET-3 mRNA相似(分别为0.04±0.02和0.05±0.01 amol/μg;n = 5)。皮质前体ET-3 mRNA处于检测下限。同样,与PNR相比,PHR红髓中的ET-3肽浓度略高但显著更高(分别为15.4±2.0和8.8±0.8 fmol/mg蛋白质;n = 5;P<0.05),而PHR和PNR乳头中的ET-3肽浓度没有差异。PHR和PNR肾皮质、红髓和乳头中的ECE-1 mRNA水平相似,在0.34±0.03至0.56±0.12 amol/μg总RNA之间。在肾小球膜的总ET受体中,39%为ETA受体,而乳头膜仅含有ETB受体。PHR和PNR在肾小球膜(Bmax分别为6.5±1.3和4.9±1.2 pmol/mg蛋白质;Kd分别为0.69±0.10和0.56±0.10 nM)和乳头膜(Bmax分别为9.7±1.1和11.3±1.6 pmol/mg蛋白质;Kd分别为0.30±0.04和0.42±0.07 nM)中对ET-1的Bmax和Kd值相似。高血压大鼠和血压正常大鼠的血浆ET-1/2浓度(PHR和PNR分别为10.4±1.3和12.2±1.2 fmol/ml)和尿ET-1排泄量(PHR和PNR分别为3.1±0.3和3.0±0.2 pmol/24 h)相似。总之,尽管肾脏中前体ET-3 mRNA的组织水平非常低,但与PNR相比,PHR髓质组织中前体ET-3 mRNA和ET-3肽的含量显著更高,这一发现有待进一步研究。相比之下,PHR乳头组织中的前体ET-1 mRNA含量和ET-1肽浓度显著低于PNR。正常情况下拮抗[精氨酸8]加压素作用的ET-1合成减少,可能会使内髓集合管水平的水(和钠)重吸收增加。PHR肾脏的这种内在缺陷可能导致该模型中的高血压,并可能在“高血压”肾脏移植时传递高血压。

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