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低氧适应大鼠肺组织和肺外组织中血管紧张素转换酶的改变

Altered angiotensin-converting enzyme in lung and extrapulmonary tissues of hypoxia-adapted rats.

作者信息

Oparil S, Narkates A J, Jackson R M, Ann H S

机构信息

Department of Medicine, University of Alabama, Birmingham 35294.

出版信息

J Appl Physiol (1985). 1988 Jul;65(1):218-27. doi: 10.1152/jappl.1988.65.1.218.

Abstract

The effects of exposing rats to hypoxia (10% O2) at normal atmospheric pressure for periods of 14 or 28 days on angiotensin-converting enzyme (ACE) activity and stores of angiotensin I (ANG I) and angiotensin II (ANG II) in lung, kidney, brain, and testis were examined. ACE activity was measured by spectrophotometric assay, and active sites of ACE were estimated by measuring the binding of 125I-351A [N-(1-carbonyl-3-phenyl-propyl)-L-lysyl-L-proline], a highly specific active site-directed inhibitor of ACE, to tissue homogenates and perfused lungs. Hypoxia exposure produced progressive reductions in ACE activity in lung homogenates and in ACE inhibitor binding to perfused lungs. ANG II levels in lungs from hypoxia-adapted animals were significantly less than air controls, suggesting that the reduction in intrapulmonary ACE activity was associated with reduced local generation of ANG II. ACE activity was increased in kidney and unchanged in brain and testis of hypoxia-adapted rats compared with air controls. Thus the effects of chronic hypoxia on catalytically active ACE and ACE active sites in the intact animal were organ specific. Adaptation to chronic hypoxia did not significantly alter plasma renin activity or ANG I or ANG II levels or serum ACE content. The hypoxia-induced alterations in lung and kidney ACE were reversible after return to a normoxic environment.

摘要

研究了在正常大气压下将大鼠暴露于低氧环境(10%氧气)14天或28天对肺、肾、脑和睾丸中血管紧张素转换酶(ACE)活性以及血管紧张素I(ANG I)和血管紧张素II(ANG II)储存量的影响。通过分光光度法测定ACE活性,并通过测量125I-351A [N-(1-羰基-3-苯基丙基)-L-赖氨酰-L-脯氨酸](一种高度特异性的ACE活性位点导向抑制剂)与组织匀浆和灌注肺的结合来估计ACE的活性位点。暴露于低氧环境导致肺匀浆中ACE活性以及ACE抑制剂与灌注肺的结合逐渐降低。低氧适应动物肺中的ANG II水平显著低于空气对照组,这表明肺内ACE活性的降低与ANG II的局部生成减少有关。与空气对照组相比,低氧适应大鼠的肾中ACE活性增加,脑和睾丸中的ACE活性未发生变化。因此,慢性低氧对完整动物中具有催化活性的ACE和ACE活性位点的影响具有器官特异性。适应慢性低氧并未显著改变血浆肾素活性、ANG I或ANG II水平或血清ACE含量。回到常氧环境后,低氧诱导的肺和肾ACE变化是可逆的。

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