首页> 美国卫生研究院文献>American Journal of Physiology - Regulatory Integrative and Comparative Physiology >Role of 20-HETE in the antihypertensive effect of transfer of chromosome 5 from Brown Norway to Dahl salt-sensitive rats
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Role of 20-HETE in the antihypertensive effect of transfer of chromosome 5 from Brown Norway to Dahl salt-sensitive rats

机译:20-HETE在5号染色体从布朗挪威转移到达尔盐敏感性大鼠中的降压作用

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摘要

This study examined whether substitution of chromosome 5 containing the CYP4A genes from Brown Norway rat onto the Dahl S salt-sensitive (SS) genetic background upregulates the renal production of 20-HETE and attenuates the development of hypertension. The expression of CYP4A protein and the production of 20-HETE were significantly higher in the renal cortex and outer medulla of SS.5BN (chromosome 5-substituted Brown Norway rat) consomic rats fed either a low-salt (LS) or high-salt (HS) diet than that seen in SS rats. The increase in the renal production of 20-HETE in SS.5BN rats was associated with elevated expression of CYP4A2 mRNA. MAP measured by telemetry rose from 117 ± 1 to 183 ± 5 mmHg in SS rats fed a HS diet for 21 days, but only increased to 151 ± 5 mmHg in SS.5BN rats. The pressure-natriuretic and diuretic responses were twofold higher in SS.5BN rats compared with SS rats. Protein excretion rose to 354 ± 17 mg/day in SS rats fed a HS diet for 21 days compared with 205 ± 13 mg/day in the SS.5BN rats, and the degree of glomerular injury was reduced. Baseline glomerular capillary pressure (Pgc) was similar in SS.5BN rats (43 ± 1 mmHg) and Dahl S (44 ± 2 mmHg) rats. However, Pgc increased to 59 ± 3 mmHg in SS rats fed a HS diet for 7 days, while it remained unaltered in SS.5BN rats (43 ± 2 mmHg). Chronic administration of an inhibitor of the synthesis of 20-HETE (HET0016, 10 mg·kg−1·day−1 iv) reversed the antihypertensive phenotype seen in the SS.5BN rats. These findings indicate that the transfer of chromosome 5 from the BN rat onto the SS genetic background increases the renal expression of CYP4A protein and the production of 20-HETE and that 20-HETE contributes to the antihypertensive and renoprotective effects seen in the SS.5BN consomic strain.
机译:这项研究检查了将含有来自挪威褐鼠的CYP4A基因的5号染色体替换为Dahl S盐敏感(SS)遗传背景是否能上调肾脏20-HETE的产生并减轻高血压的发展。 CYP4A蛋白的表达和20-HETE的产生在SS.5 BN (5染色体取代的布朗挪威大鼠)低剂量饲喂的SS。盐(LS)或高盐(HS)饮食要比SS大鼠所见。 SS.5 BN 大鼠肾脏20-HETE产量增加与CYP4A2 mRNA表达升高有关。用遥测技术测得的MAP在21天喂食HS饮食的SS大鼠从117±1升至183±5mmHg,而在SS.5 BN 大鼠中仅升高至151±5mmHg。与SS大鼠相比,SS.5 BN 大鼠的压力利钠尿和利尿反应高出两倍。喂食HS饮食21天的SS大鼠的蛋白排泄上升至354±17 mg / day,而SS.5 BN 大鼠的蛋白排泄增加至205±13 mg / day,肾小球损伤程度为减少。 SS.5 BN 大鼠(43±1 mmHg)和Dahl S(44±2 mmHg)大鼠的基线肾小球毛细血管压(Pgc)相似。然而,喂食HS饲料7天的SS大鼠的Pgc升高至59±3 mmHg,而SS.5 BN 大鼠(43±2 mmHg)的Pgc保持不变。长期给予20-HETE合成抑制剂(HET0016,10 mg·kg -1 ·day -1 iv)可逆转SS中出现的降压表型。 5只 BN 大鼠。这些发现表明5号染色体从BN大鼠转移到SS遗传背景上会增加CYP4A蛋白的肾脏表达和20-HETE的产生,而20-HETE有助于SS中的降压和肾保护作用.5 BN 纯系。

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