Atrial natriuretic peptide and dopamine in established acute renal failure in the rat. Recent studies have shown that atrial natriuretic peptide (ANP) alone or combined with dopamine (D) markedly improved renal function when given immediately after an ischemic insult. However, the potential beneficial effect of ANP or ANP-D in the established phase of acute renal failure (ARF) and the duration of this effect have not been examined. In the present study atriopeptin III (APIII) and D, sufficient to maintain mean arterial pressure between 100 and 110 mm Hg, or normal saline were given i.v. for four hours to awake Munich-Wistar rats(N = 6 each group) two days after ARF induction with intrarenal norepinephrine (NE). Renal function and morphology were then examined two days after treatment (Day 4). Serum creatinine (SCr) was similarly increased in both groups at the time of APIII-D or saline infusion (Day 2). By Day 4 SCr had decreased to the pre-ARF induction level in APIII-D-treated rats(P < 0.005), but continued to rise in saline-treated animals(P < 0.025). Day 4 renal blood flow and glomerular filtration rate (GFR) were higher in APIII-D-compared to the saline-treated group (9.13 1.14 vs. 4.41 2.25 ml/min and 0.787 0.066 vs. 0.370 0.185 ml/min, respectively, bothP < 0.005). Single nephron GFR was higher in APIII-D-treated rats (96 47 vs. 37 28 ml/min, P < 0.025) primarily due to an increase in glomerular capillary pressure (51 4 vs. 43 5 mm Hg, P < 0.02). Urine flow rate and fractional excretion of sodium were less in APIII-D-treated rats(P < 0.05). While comparison of percent abnormal tubular profiles for specific kidney zones showed little difference between the two groups, the overall sums of percent abnormal profiles for all zones demonstrated significantly less tubular necrosis(P < 0.001) and tubular regeneration(P < 0.025) and fewer tubular casts(P < 0.01) in the kidneys of APIII-D-treated rats. It is concluded that APIII-D not only increases GFR in the established phase of ARF, but the effect is sustained. While the major effect of APIII-D may be to increase SNGFR in at least a sufficient number of nephrons to impact on whole kidney filtration rate, there also appears to be an effect on restoration of tubular function and morphology.
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机译:心钠素和多巴胺可在大鼠中确立急性肾功能衰竭。最近的研究表明,缺血性损伤后立即给予时,单独的心房利钠肽(ANP)或与多巴胺(D)组合可显着改善肾脏功能。但是,尚未检查ANP或ANP-D在急性肾衰竭(ARF)确立阶段的潜在有益作用及其持续时间。在本研究中,静脉内给予足以维持平均动脉压在100至110 mm Hg之间的Atriopeptin III(APIII)和D。肾内去甲肾上腺素(NE)诱导ARF后两天,醒来四小时以唤醒慕尼黑-维斯塔(N = 6)。治疗后两天(第4天)检查肾功能和形态。在APIII-D或生理盐水输注时(第2天),两组的血清肌酐(SCr)类似地增加。到第4天,在用APIII-D处理的大鼠中,SCr降低至ARF诱导前水平(P <0.005),而在用盐水处理的动物中则继续升高(P <0.025)。与盐水治疗组相比,APIII-D的第4天肾血流量和肾小球滤过率(GFR)更高(分别为9.13 1.14 vs. 4.41 2.25 ml / min和0.787 0.066 vs. 0.370 0.185 ml / min,P <0.005)。在APIII-D治疗的大鼠中,单个肾单位GFR较高(96 47 vs. 37 28 ml / min,P <0.025),这主要是由于肾小球毛细血管压力增加(51 4 vs. 43 5 mm Hg,P <0.02) 。 APIII-D处理的大鼠尿液流速和钠的分数排泄较少(P <0.05)。虽然对特定肾脏区域的异常肾小管百分比百分比的比较显示两组之间几乎没有差异,但所有区域的异常档案百分数的总和显示出肾小管坏死(P <0.001)和肾小管再生(P <0.025)明显更少在用APIII-D治疗的大鼠的肾脏中铸型(P <0.01)。结论是,APIII-D不仅在ARF的确立阶段增加了GFR,而且效果持续。尽管APIII-D的主要作用可能是增加至少足够数量的肾单位中的SNGFR,以影响全肾滤过率,但似乎也对肾小管功能和形态的恢复产生影响。
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