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首页> 外文期刊>Journal of Neurophysiology >Acid-sensitive two-pore domain potassium (K2P) channels in mouse taste buds.
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Acid-sensitive two-pore domain potassium (K2P) channels in mouse taste buds.

机译:小鼠味蕾中的酸敏感性两孔结构域钾(K2P)通道。

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摘要

Sour (acid) taste is postulated to result from intracellular acidification that modulates one or more acid-sensitive ion channels in taste receptor cells. The identity of such channel(s) remains uncertain. Potassium channels, by regulating the excitability of taste cells, are candidates for acid transducers. Several 2-pore domain potassium leak conductance channels (K(2)P family) are sensitive to intracellular acidification. We examined their expression in mouse vallate and foliate taste buds using RT-PCR, and detected TWIK-1 and -2, TREK-1 and -2, and TASK-1. Of these, TWIK-1 and TASK-1 were preferentially expressed in taste cells relative to surrounding nonsensory epithelium. The related TRESK channel was not detected, whereas the acid-insensitive TASK-2 was. Using confocal imaging with pH-, Ca(2+)-, and voltage-sensitive dyes, we tested pharmacological agents that are diagnostic for these channels. Riluzole (500 microM), selective for TREK-1 and -2 channels, enhanced acid taste responses. In contrast, halothane (< or = approximately 17 mM), which acts on TREK-1 and TASK-1 channels, blocked acid taste responses. Agents diagnostic for other 2-pore domain and voltage-gated potassium channels (anandamide, 10 microM; Gd(3+), 1 mM; arachidonic acid, 100 microM; quinidine, 200 microM; quinine, 100 mM; 4-AP, 10 mM; and TEA, 1 mM) did not affect acid responses. The expression of 2-pore domain channels and our pharmacological characterization suggest that a matrix of ion channels, including one or more acid-sensitive 2-pore domain K channels, could play a role in sour taste transduction. However, our results do not unambiguously identify any one channel as the acid taste transducer.
机译:酸(酸)味被认为是由细胞内酸化引起的,酸化作用调节味觉受体细胞中的一个或多个酸敏感离子通道。这样的信道的身份仍然不确定。通过调节味觉细胞的兴奋性,钾通道是酸转化子的候选者。几个2孔域钾泄漏电导通道(K(2)P家族)对细胞内酸化敏感。我们使用RT-PCR检查了它们在小鼠vallate和叶酸味蕾中的表达,并检测到TWIK-1和-2,TREK-1和-2和TASK-1。其中,相对于周围的非感觉上皮细胞,TWIK-1和TASK-1在味觉细胞中优先表达。未检测到相关的TRESK通道,而检测到了酸不敏感的TASK-2。使用共聚焦成像与pH-,Ca(2 +)-和电压敏感的染料,我们测试了诊断这些通道的药理剂。 Riluzole(500 microM)对TREK-1和-2通道具有选择性,增强了酸味反应。相反,作用于TREK-1和TASK-1通道的氟烷(<或=约17 mM)阻止了酸味反应。诊断其他2孔结构域和电压门控钾通道的试剂(阿糖酰胺10 microM; Gd(3+)1 mM;花生四烯酸100 microM;奎尼丁200 microM;奎宁100 mM; 4-AP 10 mM; TEA为1 mM)不影响酸反应。 2孔结构域通道的表达和我们的药理特性表明,包括一个或多个酸敏感的2孔结构域K通道的离子通道基质可能在酸味传递中起作用。但是,我们的结果并未明确地将任何一个通道识别为酸味传感器。

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