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血管紧张素II诱导的肾血流改变对离体灌注大鼠肾脏中头孢尼西排泄的影响。

Influence of angiotensin II-induced alterations in renal flow on excretion of cefonicid in isolated perfused rat kidneys.

作者信息

Rodríguez C A, Smith D E

机构信息

College of Pharmacy, University of Michigan, Ann Arbor 48109-1065.

出版信息

Antimicrob Agents Chemother. 1992 Mar;36(3):616-9. doi: 10.1128/AAC.36.3.616.

Abstract

The effects of variations in renal perfusate flow on the excretion of cefonicid was examined in isolated perfused rat kidneys. Cefonicid, an expanded-spectrum cephalosporin, is primarily eliminated by active tubular secretion and is neither metabolized nor reabsorbed in the isolated kidney. We used angiotensin II (AII), a strong vasoconstrictor hormone of the afferent and the efferent arterioles in the kidney, to determine whether the renal and secretion clearances, as well as the excretion ratio (ER = CLR/[fu x GFR], where CLR is renal clearance, fu is the unbound fraction, and GFR is glomerular filtration rate), of this low-extraction compound can be altered by a decreased perfusion flow. Control studies were performed in the absence (n = 5) and presence (n = 4) of AII; cefonicid studies were performed in the absence (n = 4) and presence (n = 5) of AII. AII (1 to 4 ng/min) and cefonicid (5 to 10 micrograms/min) were infused into the perfusate. Cefonicid was assayed by high-performance liquid chromatography, and its protein binding was determined by ultrafiltration. AII decreased the perfusate flow rate and increased the renal vascular resistance and filtration fraction of the isolated kidney in the presence and absence of cefonicid. The glomerular filtration rate remained unchanged among the groups. The fractional excretion of glucose was low and steady, indicating a well-preserved tubular function. Although the unbound fraction was unchanged between treatments, the renal and secretion clearances and the excretion ratio of cefonicid were reduced by about 40% in the presence of AII (excretion ratios, 10.3 without AII versus 6.03 with AII). These results suggest that the altered clearance parameters of cefonicid are the result of a flow-induced change in the intrinsic secretory transport of the drug.

摘要

在离体灌注大鼠肾脏中研究了肾灌注液流量变化对头孢尼西排泄的影响。头孢尼西是一种广谱头孢菌素,主要通过肾小管主动分泌消除,在离体肾脏中既不代谢也不重吸收。我们使用血管紧张素II(AII),一种肾脏入球小动脉和出球小动脉的强血管收缩激素,来确定这种低摄取化合物的肾清除率和分泌清除率以及排泄率(ER = CLR/[fu×GFR],其中CLR是肾清除率,fu是未结合分数,GFR是肾小球滤过率)是否会因灌注流量降低而改变。在无AII(n = 5)和有AII(n = 4)的情况下进行对照研究;在无AII(n = 4)和有AII(n = 5)的情况下进行头孢尼西研究。将AII(1至4 ng/分钟)和头孢尼西(5至10微克/分钟)注入灌注液中。通过高效液相色谱法测定头孢尼西,并通过超滤法测定其蛋白结合率。无论有无头孢尼西,AII均降低了灌注液流速,增加了离体肾脏的肾血管阻力和滤过分数。各组间肾小球滤过率保持不变。葡萄糖的分数排泄率低且稳定,表明肾小管功能良好。尽管不同处理之间未结合分数未变,但在有AII的情况下,头孢尼西的肾清除率、分泌清除率和排泄率降低了约40%(排泄率,无AII时为10.3,有AII时为6.03)。这些结果表明,头孢尼西清除参数的改变是药物内在分泌转运中流量诱导变化的结果。

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