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紫外线B照射的人体皮肤中对缓激肽B1和B2受体激活的致敏作用。

Sensitization to bradykinin B1 and B2 receptor activation in UV-B irradiated human skin.

作者信息

Eisenbarth Harald, Rukwied Roman, Petersen Marlen, Schmelz Martin

机构信息

Department of Physiology and Experimental Pathophysiology, University of Erlangen, Erlangen, Germany.

出版信息

Pain. 2004 Jul;110(1-2):197-204. doi: 10.1016/j.pain.2004.03.031.

Abstract

Bradykinin B1 and B2 receptors contribute to nociceptor sensitization under inflammatory conditions. Here, we examined the vascular inflammatory responses and nociceptive effects resulting from activation of B1 and B2 receptors in healthy and UV-B irradiated skin in human volunteers. The B1 receptor agonist des-Arg(10)-Kallidin (10(-6)-10(-3)M) and the B2 receptor agonist bradykinin (10(-9)-10(-4)M) were administered by dermal microdialysis to the ventral thigh. UV-B irradiation was performed 24 h prior to the experiment with the threefold minimum erythemal dose. Pain sensation perceived during the stimulation with the bradykinin receptor agonists was estimated on a numeric scale. Local and axon reflex-induced vasodilations were recorded by laser Doppler imaging. For protein extravasation, total protein content in the dialysate was assessed as a measure of increased endothelial permeability. In normal skin, both B1 and B2 receptor activation dose-dependently evoked pain, vasodilatation and protein extravasation. In UV-B irradiated skin, pain sensation and axon reflex vasodilatation were enhanced by both B1 and B2 agonists, whereas local vasodilatation was increased only following B1 receptor activation. The UV-B irradiation did not enhance B1 and B2 receptor-induced protein extravasation indicating a differential sensitization of the neuronal, but not the vascular response.

摘要

缓激肽B1和B2受体在炎症条件下会导致伤害感受器致敏。在此,我们研究了人类志愿者健康皮肤和紫外线B(UV-B)照射皮肤中B1和B2受体激活所引起的血管炎症反应和伤害感受效应。通过真皮微透析将B1受体激动剂去-Arg(10)-缓激肽(10⁻⁶ - 10⁻³M)和B2受体激动剂缓激肽(10⁻⁹ - 10⁻⁴M)注射到大腿腹侧。在实验前24小时用三倍最小红斑量进行UV-B照射。用数字评分法评估缓激肽受体激动剂刺激期间所感知到的疼痛感觉。通过激光多普勒成像记录局部和轴突反射诱导的血管舒张。对于蛋白外渗,评估透析液中的总蛋白含量作为内皮通透性增加的指标。在正常皮肤中,B1和B2受体激活均剂量依赖性地引起疼痛、血管舒张和蛋白外渗。在UV-B照射的皮肤中,B1和B2激动剂均增强了疼痛感觉和轴突反射血管舒张,而仅在B1受体激活后局部血管舒张增加。UV-B照射并未增强B1和B2受体诱导的蛋白外渗,表明神经元反应存在差异致敏,但血管反应不存在差异致敏。

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