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无毛和有毛皮肤传入神经中表达的酸敏感离子通道的质子敏感性、钙离子通透性及分子基础。

Proton sensitivity Ca2+ permeability and molecular basis of acid-sensing ion channels expressed in glabrous and hairy skin afferents.

作者信息

Jiang N, Rau K K, Johnson R D, Cooper B Y

机构信息

Department of Oral Surgery and Diagnostic Sciences, Division of Neuroscience, J.H. Miller Health Center, University of Florida College of Dentistry, Gainesville, FL 32610, USA.

出版信息

J Neurophysiol. 2006 Apr;95(4):2466-78. doi: 10.1152/jn.00861.2005. Epub 2006 Jan 11.

Abstract

We contrasted the physiology and peripheral targets of subclassified nociceptive and nonnociceptive afferents that express acid-sensing ion channel (ASIC)-like currents. The threshold for current activation was similar in eight distinct cell subclasses regardless of functional modality (pH 6.8). When potency was determined from concentration-response curves, nonnociceptors exhibited currents with significantly greater potency than that of all but one class of nociceptors (pH50 = 6.54 and 6.75 vs. 6.20-6.34). In nonnociceptive cells, acid transduction was also confined to a very narrow range (0.1-0.3 vs. 0.8-1.4 pH units for nociceptors). Simultaneous whole cell recording and ratiometric imaging of three peptidergic nociceptive classes were consistent with the expression of Ca2+ -permeable ASICs. Sensitivity to psalmotoxin and flurbiprofen indicated the presence of Ca2+ -permeable ASIC1a. Immunocytochemistry on these subclassified populations revealed a differential distribution of five ASIC proteins consistent with Ca2+ permeability and differential kinetics of proton-gated currents (type 5: ASIC1a, 1b, 2a, 2b, 3; type 8a: ASIC1a, 1b, 3; type 8b: ASIC1a, 1b, 2a, 2b, 3). Using DiI tracing, we found that nociceptive classes had discrete peripheral targets. ASIC-expressing types 8a and 9 projected to hairy skin, but only types 8a and 13 projected to glabrous skin. Non-ASIC-expressing types 2 and 4 were present only in hairy skin. We conclude that ASIC-expressing nociceptors differ from ASIC-expressing nonnociceptors mainly by range of proton reactivity. ASIC- as well as non-ASIC-expressing nociceptors have highly distinct cutaneous targets, and only one class was consistent with the existence of a generic C polymodal nociceptor (type 8a).

摘要

我们对比了表达酸敏感离子通道(ASIC)样电流的亚分类伤害性和非伤害性传入神经的生理学及外周靶点。无论功能模式如何(pH 6.8),在八个不同的细胞亚类中,电流激活阈值相似。当根据浓度-反应曲线确定效力时,除一类伤害性感受器外,非伤害性感受器的电流效力显著高于所有其他类别的伤害性感受器(pH50 = 6.54和6.75,而伤害性感受器为6.20 - 6.34)。在非伤害性细胞中,酸转导也局限于非常窄的范围(0.1 - 0.3个pH单位,而伤害性感受器为0.8 - 1.4个pH单位)。对三类肽能伤害性感受器进行的全细胞同步记录和比率成像与Ca2+通透型ASIC的表达一致。对Psalmotoxin和氟比洛芬的敏感性表明存在Ca2+通透型ASIC1a。对这些亚分类群体进行的免疫细胞化学显示,五种ASIC蛋白的分布不同,这与Ca2+通透性以及质子门控电流的不同动力学一致(5型:ASIC1a、1b、2a、2b、3;8a型:ASIC1a、1b、3;8b型:ASIC1a、1b、2a、2b、3)。使用DiI示踪法,我们发现伤害性感受器类别具有离散的外周靶点。表达ASIC的8a型和9型投射至有毛皮肤,但只有8a型和13型投射至无毛皮肤。不表达ASIC的2型和4型仅存在于有毛皮肤中。我们得出结论,表达ASIC的伤害性感受器与表达ASIC的非伤害性感受器的主要区别在于质子反应范围。表达ASIC以及不表达ASIC的伤害性感受器具有高度不同的皮肤靶点,并且只有一类与通用的C类多模式伤害性感受器(8a型)的存在一致。

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