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一种假定的微血管氧传感器的鉴定。

Identification of a putative microvascular oxygen sensor.

作者信息

Harder D R, Narayanan J, Birks E K, Liard J F, Imig J D, Lombard J H, Lange A R, Roman R J

机构信息

Department of Physiology, Medical College of Wisconsin, Milwaukee 53226, USA.

出版信息

Circ Res. 1996 Jul;79(1):54-61. doi: 10.1161/01.res.79.1.54.

Abstract

The vascular response to changes in oxygen levels in the blood and tissue is a highly adaptive physiological response that functions to match tissue oxygen supply to metabolic demand. Defining the cellular mechanisms that can sense physiologically relevant changes in PO2 and adjust vascular diameter are vital to our understanding of this process. A cytochrome P450 (P450) enzyme of the 4A family of omega-hydroxylases was localized in renal microvessels, renal cortex, and a striated muscle microvascular bed (cremaster) of the rat. In the presence of molecular oxygen, this P450 enzyme catalyzes formation of 20-HETE from arachidonic acid (AA). Prior studies have shown that 20-HETE potently contracts renal and cerebral arteries and arterioles. The present study demonstrates that 20-HETE constricts striated muscle arterioles as well. In both intact renal microvessels and enriched renal cortical microsomal enzyme preparations, the formation of 20-HETE was linearly dependent on PO2 between 20 and 140 mm Hg. Homogenates of cremaster tissue produced 20-oxygen HETE when incubated with AA. They also expressed message for P450 4A enzyme, as determined by Southern and Western blots. Administration of 17-octadecynoic acid (17-ODYA), which is a P450 4A inhibitor, attenuated the constriction of third-order cremasteric arterioles in response to elevation of superfusion solution PO2 from approximately equal to 3 to 5 mm Hg to approximately equal to 35 mm Hg. 17-ODYA had no effect on basal vascular tone or response of cremaster arterioles to vasoactive compounds. These results demonstrate the existence of P450 omega-hydroxylase activity and 20-HETE formation in the vasculature and parenchyma of at least two microvascular beds. Our data suggest that a P450 enzyme of the 4A family has the potential to function as an oxygen sensor in mammalian microcirculatory beds and to regulate arteriolar caliber by generating 20-HETE in an oxygen-dependent manner.

摘要

血管对血液和组织中氧水平变化的反应是一种高度适应性的生理反应,其作用是使组织氧供应与代谢需求相匹配。确定能够感知生理相关的PO2变化并调节血管直径的细胞机制,对于我们理解这一过程至关重要。一种ω-羟化酶4A家族的细胞色素P450(P450)酶定位于大鼠的肾微血管、肾皮质和横纹肌微血管床(提睾肌)。在分子氧存在的情况下,这种P450酶催化花生四烯酸(AA)形成20-羟基二十碳四烯酸(20-HETE)。先前的研究表明,20-HETE能强烈收缩肾动脉和脑动脉及小动脉。本研究表明,20-HETE也能收缩横纹肌小动脉。在完整的肾微血管和富集的肾皮质微粒体酶制剂中,20-HETE的形成在20至140 mmHg之间与PO2呈线性相关。提睾肌组织匀浆与AA孵育时产生20-氧代HETE。通过Southern和Western印迹法测定,它们也表达P450 4A酶的信息。给予P450 4A抑制剂17-十八炔酸(17-ODYA),可减弱当灌注液PO2从约等于3至5 mmHg升高到约等于35 mmHg时三级提睾肌小动脉的收缩。17-ODYA对基础血管张力或提睾肌小动脉对血管活性化合物的反应无影响。这些结果证明了至少两个微血管床的血管系统和实质中存在P450 ω-羟化酶活性和20-HETE形成。我们的数据表明,4A家族的一种P450酶有可能在哺乳动物微循环床中作为氧传感器发挥作用,并通过以氧依赖的方式生成20-HETE来调节小动脉口径。

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