一氧化氮合酶和环氧化酶调节年轻男性皮肤的β-肾上腺素能血管舒张和出汗。

Nitric oxide synthase and cyclooxygenase modulate β-adrenergic cutaneous vasodilatation and sweating in young men.

作者信息

Fujii Naoto, McNeely Brendan D, Kenny Glen P

机构信息

Human and Environmental Physiology Research Unit, University of Ottawa, Ottawa, Canada.

出版信息

J Physiol. 2017 Feb 15;595(4):1173-1184. doi: 10.1113/JP273502. Epub 2016 Dec 12.

DOI:10.1113/JP273502

PMID:27779753

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5309368/

Abstract

KEY POINTS

β-Adrenergic receptor agonists such as isoproterenol induce cutaneous vasodilatation and sweating in humans, but the mechanisms underpinning this response remain unresolved. Using intradermal microdialysis, we evaluated the roles of nitric oxide synthase (NOS) and cyclooxygenase (COX) in β-adrenergic cutaneous vasodilatation and sweating elicited by administration of isoproterenol. We show that while NOS contributes to β-adrenergic cutaneous vasodilatation, COX restricts cutaneous vasodilatation. We also show that combined inhibition of NOS and COX augments β-adrenergic sweating These new findings advance our basic knowledge regarding the physiological control of cutaneous blood flow and sweating, and provide important and new information to better understand the physiological significance of β-adrenergic receptors in the skin.

ABSTRACT

β-Adrenergic receptor agonists such as isoproterenol can induce cutaneous vasodilatation and sweating in humans, but the mechanisms underpinning this response remain unresolved. We evaluated the hypotheses that (1) nitric oxide synthase (NOS) contributes to β-adrenergic cutaneous vasodilatation, whereas cyclooxygenase (COX) limits the vasodilatation, and (2) COX contributes to β-adrenergic sweating. In 10 young males (25 ± 5 years), cutaneous vascular conductance (CVC) and sweat rate were evaluated at four intradermal forearm skin sites infused with (1) lactated Ringer solution (control), (2) 10 mm N -nitro-l-arginine (l-NNA), a non-specific NOS inhibitor, (3) 10 mm ketorolac, a non-specific COX inhibitor, or (4) a combination of l-NNA and ketorolac. All sites were co-administered with a high dose of isoproterenol (100 μm) for 3 min to maximally induce β-adrenergic sweating (β-adrenergic sweating is significantly blunted by subsequent activations). Approximately 60 min after the washout period, three incremental doses of isoproterenol were co-administered (1, 10 and 100 μm each for 25 min). Increases in CVC induced by the first and second 100 μm isoproterenol were attenuated by l-NNA alone, and those in response to all doses of isoproterenol were reduced by l-NNA with co-infusion of ketorolac (all P ≤ 0.05). Ketorolac alone augmented increases in CVC induced by 10 μm and by the second 100 μm isoproterenol (both P ≤ 0.05). While isoproterenol-induced sweating was not affected by the separate administration of l-NNA or ketorolac (all P > 0.05), their combined administration augmented sweating elicited by the first 3 min of 100 μm isoproterenol (P = 0.05). We show that while NOS contributes to β-adrenergic cutaneous vasodilatation, COX restrains the vasodilatation. Finally, combined inhibition of NOS and COX augments β-adrenergic sweating.

摘要

关键点

诸如异丙肾上腺素之类的β-肾上腺素能受体激动剂可诱导人体皮肤血管舒张和出汗，但其背后的机制仍未明确。我们采用皮内微透析技术，评估了一氧化氮合酶（NOS）和环氧化酶（COX）在异丙肾上腺素引发的β-肾上腺素能皮肤血管舒张和出汗中的作用。我们发现，虽然NOS有助于β-肾上腺素能皮肤血管舒张，但COX会限制皮肤血管舒张。我们还发现，联合抑制NOS和COX可增强β-肾上腺素能出汗。这些新发现增进了我们对皮肤血流和出汗生理控制的基础知识，并为更好地理解β-肾上腺素能受体在皮肤中的生理意义提供了重要的新信息。

摘要

诸如异丙肾上腺素之类的β-肾上腺素能受体激动剂可诱导人体皮肤血管舒张和出汗，但其背后的机制仍未明确。我们评估了以下假设：（1）一氧化氮合酶（NOS）有助于β-肾上腺素能皮肤血管舒张，而环氧化酶（COX）会限制血管舒张；（2）COX有助于β-肾上腺素能出汗。在10名年轻男性（25±5岁）中，于前臂皮内四个皮肤部位注入（1）乳酸林格溶液（对照）、（2）10 mM N-硝基-L-精氨酸（L-NNA），一种非特异性NOS抑制剂、（3）10 mM酮咯酸，一种非特异性COX抑制剂，或（4）L-NNA与酮咯酸的组合，以此评估皮肤血管传导性（CVC）和出汗率。所有部位均联合给予高剂量异丙肾上腺素（100 μM）3分钟，以最大程度诱导β-肾上腺素能出汗（后续激活会使β-肾上腺素能出汗明显减弱）。洗脱期约60分钟后，联合给予三次递增剂量的异丙肾上腺素（每次1、10和100 μM，各持续25分钟）。单独使用L-NNA可减弱首次和第二次100 μM异丙肾上腺素诱导的CVC增加，而联合注入酮咯酸时，L-NNA可降低对所有剂量异丙肾上腺素的反应（所有P≤0.05）。单独使用酮咯酸可增强10 μM及第二次100 μM异丙肾上腺素诱导的CVC增加（两者P≤0.05）。虽然异丙肾上腺素诱导的出汗不受单独给予L-NNA或酮咯酸的影响（所有P>0.05），但它们联合使用可增强100 μM异丙肾上腺素最初3分钟引发的出汗（P = 0.05）。我们发现，虽然NOS有助于β-肾上腺素能皮肤血管舒张，但COX会抑制血管舒张。最后，联合抑制NOS和COX可增强β-肾上腺素能出汗。

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