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肾上腺髓质素在缺氧缺血性大鼠肾脏及动脉狭窄的人肾脏中的表达

Expression of adrenomedullin in hypoxic and ischemic rat kidneys and human kidneys with arterial stenosis.

作者信息

Sandner Peter, Hofbauer Karl Heinz, Tinel Hanna, Kurtz Armin, Thiesson Helle C, Ottosen Peter D, Walter Steen, Skøtt Ole, Jensen Boye L

机构信息

Dept. of Physiology and Pharmacology, University of Southern Denmark, Winsløwparken 21, No. 3, DK-5000 Odense, Denmark.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2004 May;286(5):R942-51. doi: 10.1152/ajpregu.00274.2003. Epub 2004 Jan 8.

Abstract

To investigate regional aspects of hypoxic regulation of adrenomedullin (AM) in kidneys, we mapped the distribution of AM in the rat kidney after hypoxia (normobaric hypoxic hypoxia, carbon monoxide, and CoCl(2) for 6 h), anemia (hematocrit lowered by bleeding) and after global transient ischemia for 1 h (unilateral renal artery occlusion and reperfusion for 6 and 24 h) and segmental infarct (6 and 24 h). AM expression and localization was determined in normal human kidneys and in kidneys with arterial stenosis. Hypoxia stimulated AM mRNA expression significantly in rat inner medulla (CO 13 times, 8% O(2) 6 times, and CoCl(2) 8 times), followed by the outer medulla and cortex. AM mRNA level was significantly elevated in response to anemia and occlusion-reperfusion. Immunoreactive AM was associated with the thin limbs of Henle's loop, distal convoluted tubule, collecting ducts, papilla surface epithelium, and urothelium. AM labeling was prominent in the inner medulla after CO and in the outer medulla after occlusion-reperfusion. The infarct border zone was strongly labeled for AM. In cultured inner medullary collecting duct cells, AM mRNA was significantly increased by hypoxia. AM mRNA was equally distributed in human kidney and AM was localized as in the rat kidney. In human kidneys with artery stenosis, AM mRNA was not significantly enhanced compared with controls, but AM immunoreactivity was observed in tubules, vessels, and glomerular cells. In summary, AM expression was increased in the rat kidney in response to hypoxic and ischemic hypoxia in keeping with oxygen gradients. AM was widely distributed in the human kidney with arterial stenosis. AM may play a significant role to counteract hypoxia in the kidney.

摘要

为研究肾脏中肾上腺髓质素(AM)缺氧调节的区域特征,我们绘制了大鼠肾脏在缺氧(常压低氧、一氧化碳和氯化钴处理6小时)、贫血(放血降低血细胞比容)以及全肾短暂缺血1小时(单侧肾动脉阻断并再灌注6和24小时)和节段性梗死(6和24小时)后AM的分布情况。在正常人类肾脏和有动脉狭窄的肾脏中测定了AM的表达和定位。缺氧显著刺激大鼠肾内髓质中AM mRNA的表达(一氧化碳处理后增加13倍,8%氧气处理后增加6倍,氯化钴处理后增加8倍),其次是外髓质和皮质。贫血和阻断 - 再灌注后,AM mRNA水平显著升高。免疫反应性AM与亨氏袢细段、远曲小管、集合管、乳头表面上皮和尿路上皮相关。一氧化碳处理后,AM标记在内髓质中突出,阻断 - 再灌注后在外髓质中突出。梗死边缘区AM标记强烈。在培养的肾内髓集合管细胞中,缺氧显著增加AM mRNA。AM mRNA在人类肾脏中分布均匀,且AM的定位与大鼠肾脏相同。在有动脉狭窄的人类肾脏中,与对照组相比,AM mRNA没有显著增强,但在肾小管、血管和肾小球细胞中观察到AM免疫反应性。总之,大鼠肾脏中AM的表达因缺氧和缺血性缺氧而增加,与氧梯度一致。AM在有动脉狭窄的人类肾脏中广泛分布。AM可能在对抗肾脏缺氧中发挥重要作用。

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