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Diagnostic and therapeutic challenges.

机译:诊断和治疗挑战。

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Transient receptor potential ankyrin 1 (TRPA1) is a member of the large TRP super family of ion channels and functions as a Ca(2+)-permeable nonselective cation channel that is activated by various noxious stimuli. TRPA1 was initially identified as a potential mediator of noxious cold stimuli in mammalian nociceptive sensory neurons, while TRPA1s from nonmammalian vertebrates (snakes, green anole lizards, and frogs) were recently reported to be activated by heat, but not cold stimulus. In this study, we examined detailed properties of the green anole TRPA1 channel (gaTRPA1) related to thermal and chemical stimulation in whole-cell and single-channel recordings. Heat activates gaTRPA1 with a temperature threshold for activation of 35.8?°C, while heat together with allyl isothiocyanate (AITC), a chemical agonist, had synergistic effects on gaTRPA1 channel activation in that either the temperature threshold or activating AITC concentration was reduced in the presence of the other stimulus. Significant heat-evoked gaTRPA1 activation was observed in the presence but not absence of extracellular Ca(2+). gaTRPA1 channels were also activated by heat and AITC in excised membrane patches with an inside-out configuration. By comparing the kinetics of heat- and AITC-evoked single-channel currents, we defined similarities and differences of gaTRPA1 channel responses to heat and AITC. We observed similar current-voltage relationship and unitary amplitudes for heat- and AITC-evoked currents and found that heat-activated currents showed shorter durations of both open and closed times. Our results suggest that the gaTRPA1 channel is directly activated by heat and chemical stimuli.
机译:瞬态受体潜在的Ankyrin 1(TRPA1)是大型TRP超级离子通道的成员,其用作通过各种有害刺激激活的Ca(2 +) - 可渗透的非选择性阳离子通道。最初被鉴定为哺乳动物伤害感觉神经元有害冷刺激的潜在介质,而最近据报道,来自非含有脊椎动物(蛇,绿牛蜥蜴和青蛙)的TRPA1s被热量激活,但不是冷刺激。在本研究中,我们检查了与全池和单通道录制中的热和化学刺激相关的绿色anole TRPA1通道(GATRPA1)的详细性质。热激活GATRPA1,温度阈值以激活35.8Ω·℃,同时与烯丙基异硫氰酸酯(AITC)一起加热,化学激动剂对GATRPA1通道激活具有协同作用,因为温度阈值或激活AITC浓度降低存在其他刺激。在存在但不存在细胞外Ca(2+)的情况下观察到显着的热诱发GATRPA1活化。 GatrPA1通道也通过热量和AITC在切除的膜贴片中激活,其中内外配置。通过比较热量和AITC诱发的单通道电流的动力学,我们定义了GATRPA1通道响应对热量和AITC的相似之处和差异。我们观察了用于热和AITC诱发电流的类似电流 - 电压关系和单一振幅,发现热激活电流显示出开放和关闭时间的较短持续时间。我们的结果表明,GatrPA1通道通过热化和化学刺激直接激活。

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