蓝光(420- 453nm)诱导的非酶促一氧化氮生成的机制和生物学相关性在体外和体内人体皮肤中由光稳定的一氧化氮衍生物产生。

Free radical biology & medicine Pub Date : 2013-12-01 Epub Date: 2013-10-09 DOI:10.1016/j.freeradbiomed.2013.09.022
Christian Opländer, Annika Deck, Christine M Volkmar, Michael Kirsch, Jörg Liebmann, Matthias Born, Frank van Abeelen, Ernst E van Faassen, Klaus-Dietrich Kröncke, Joachim Windolf, Christoph V Suschek
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引用次数: 83

摘要

人体皮肤含有光敏性一氧化氮(NO)衍生物,如亚硝酸盐和s -亚硝基硫醇,它们在UVA辐射下分解成高输出NO,并产生NO特异性生物反应,如局部血流量增加或血压降低。为了避免UVA辐射的伤害效应,我们在体外和体内研究了蓝光(420- 453nm)诱导的非酶促一氧化氮衍生物在人体皮肤中生成NO的机制和生物学相关性。通过化学发光检测(CLD),在420或453nm的生理pH下,蓝光诱导s -亚硝基白蛋白和亚硝酸盐水溶液形成一氧化氮,其形成机制迄今尚未完全确定。体外电子顺磁共振光谱法检测人体皮肤标本,蓝光照射可显著提高皮内游离NO水平。CLD在健康志愿者体内检测到,蓝光照射人体皮肤可诱导NO从被照射皮肤区域大量释放,并导致NO从皮肤表面大量转运至皮下组织。与此同时,蓝光照射引起局部皮肤血流量的快速和显著上升,这是用微光导分光光度法无创检测到的。用中等剂量的蓝光照射人体皮肤,可显著增加不依赖酶的皮肤NO形成以及NO依赖的局部生物反应,即血流量增加。该效应归因于蓝光诱导的皮肤光敏性NO衍生物释放的NO。因此,与UVA相反,蓝光诱导的NO生成可能用于治疗基于生理NO生成或生物利用度受损的全身和局部血液动力学疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mechanism and biological relevance of blue-light (420-453 nm)-induced nonenzymatic nitric oxide generation from photolabile nitric oxide derivates in human skin in vitro and in vivo.

Human skin contains photolabile nitric oxide (NO) derivates such as nitrite and S-nitrosothiols, which upon UVA radiation decompose under high-output NO formation and exert NO-specific biological responses such as increased local blood flow or reduced blood pressure. To avoid the injurious effects of UVA radiation, we here investigated the mechanism and biological relevance of blue-light (420-453 nm)-induced nonenzymatic NO generation from photolabile nitric oxide derivates in human skin in vitro and in vivo. As quantified by chemiluminescence detection (CLD), at physiological pH blue light at 420 or 453 nm induced a significant NO formation from S-nitrosoalbumin and also from aqueous nitrite solutions by a to-date not entirely identified Cu(1+)-dependent mechanism. As detected by electron paramagnetic resonance spectrometry in vitro with human skin specimens, blue light irradiation significantly increased the intradermal levels of free NO. As detected by CLD in vivo in healthy volunteers, irradiation of human skin with blue light induced a significant emanation of NO from the irradiated skin area as well as a significant translocation of NO from the skin surface into the underlying tissue. In parallel, blue light irradiation caused a rapid and significant rise in local cutaneous blood flow as detected noninvasively by using micro-light-guide spectrophotometry. Irradiation of human skin with moderate doses of blue light caused a significant increase in enzyme-independent cutaneous NO formation as well as NO-dependent local biological responses, i.e., increased blood flow. The effects were attributed to blue-light-induced release of NO from cutaneous photolabile NO derivates. Thus, in contrast to UVA, blue-light-induced NO generation might be therapeutically used in the treatment of systemic and local hemodynamic disorders that are based on impaired physiological NO production or bioavailability.

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