首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Recombinant human insulin-like growth factor-I accelerates recovery and reduces catabolism in rats with ischemic acute renal failure.
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Recombinant human insulin-like growth factor-I accelerates recovery and reduces catabolism in rats with ischemic acute renal failure.

机译:重组人胰岛素样生长因子-I促进缺血性急性肾衰竭大鼠的恢复并减少其分解代谢。

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摘要

This study evaluated whether recombinant human insulin-like growth factor-I (rhIGF-I) enhances recovery of renal function and reduces catabolism in rats with ischemic acute renal failure (ARF). ARF and sham rats received subcutaneous injections of either rhIGF-I or vehicle three times daily starting 5 h after surgery. Serum creatinine and urea, which initially rose similarly in the ARF+vehicle and ARF+rhIGF-I rats, increased more slowly after commencing the rhIGF-I injections. 72 h after surgery, the ARF+rhIGF-I rats, in comparison with ARF+vehicle animals, showed significantly greater renal plasma flow and filtration fraction, a fivefold higher glomerular filtration rate, greater renal cortical IGF-I levels, increased proliferating cell nuclear antigen expression in proximal tubule nuclei and enhanced DNA synthesis in the renal cortex, corticomedullary junction, glomeruli, and tubules as demonstrated by [3H]thymidine incorporation and in corticomedullary junction tubules as determined by autoradiography. Estimated total nitrogen output (ETNO) was greater in ARF+vehicle than in ARF+rhIGF-I or sham rats throughout the study. ETNO in ARF+rhIGF-I rats returned to sham values by the second day after surgery. 72 h after surgery, protein degradation was increased and protein synthesis reduced in the epitrochlearis muscle of ARF+vehicle as compared with ARF+rhIGF-I or sham+vehicle rats. Thus, treatment with rhIGF-I starting 5 h after inducing ischemic ARF in rats increases recovery of renal function, enhances formation of new renal tubular cells, lowers protein degradation, and increases protein synthesis in skeletal muscle and reduces net catabolism.
机译:这项研究评估了重组人胰岛素样生长因子-I(rhIGF-I)是否能增强缺血性急性肾衰竭(ARF)大鼠的肾功能恢复并降低其分解代谢。从手术后5小时开始,ARF和假手术大鼠每天皮下注射rhIGF-I或媒介物3次。开始注射rhIGF-1后,血清肌酐和尿素最初在ARF +载体和ARF + rhIGF-I大鼠中相似地上升,但增加较慢。手术后72小时,与ARF +车辆动物相比,ARF + rhIGF-I大鼠显示出明显更高的肾血浆流量和滤过分数,肾小球滤过率高五倍,肾皮质IGF-I水平更高,增殖细胞核增加如[3 H]胸苷掺入所证实的,在肾小管近端细胞核中的抗原表达和在肾皮质,皮质肾小管连接处,肾小球和肾小管中的DNA合成增强以及由放射自显影确定的在皮质肾小管连接中。在整个研究过程中,ARF +车辆的估计总氮产量(ETNO)大于ARF + rhIGF-1或假大鼠。手术后第二天,ARF + rhIGF-I大鼠的ETNO恢复至假值。与ARF + rhIGF-1或假手术+载体大鼠相比,ARF +载体的棘上肌中的蛋白质降解在手术后72小时增加,蛋白质合成减少。因此,在大鼠中诱导缺血性ARF后5小时开始用rhIGF-1治疗增加了肾功能的恢复,增强了新的肾小管细胞的形成,降低了蛋白质的降解,并增加了骨骼肌中蛋白质的合成并减少了净分解代谢。

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