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Nicotinic Acid is a Common Regulator of Heat-Sensing TRPV1-4 Ion Channels

机译:烟酸是热敏TRPV1-4离子通道的常见调节剂

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Nicotinic acid (NA, a.k.a. vitamin B3 or niacin) can reduce blood cholesterol and low-density lipoproteins whereas increase high-density lipoproteins. However, when NA is used to treat dyslipidemias, it causes a strong side effect of cutaneous vasodilation, commonly called flushing. A recent study showed that NA may cause flushing by lowering activation threshold temperature of the heat-sensitive capsaicin receptor TRPV1 ion channel, leading to its activation at body temperature. The finding calls into question whether NA might also interact with the homologous heat-sensitive TRPV2–4 channels, particularly given that TRPV3 and TRPV4 are abundantly expressed in keratinocytes of the skin where much of the flushing response occurs. We found that NA indeed potentiated TRPV3 while inhibited TRPV2 and TRPV4. Consistent with these gating effects, NA lowered the heat-activation threshold of TRPV3 but elevated that of TRPV4. We further found that activity of TRPV1 was substantially prolonged by extracellular NA, which may further enhance the direct activation effect. Consistent with the broad gating effect on TRPV1–4 channels, evidence from the present study hints that NA may share the same activation pathway as 2-aminoethoxydiphenyl borate (2-APB), a common agonist for these TRPV channels. These findings shed new light on the molecular mechanism underlying NA regulation of TRPV channels.
机译:烟酸(NA,又称维生素B3或烟酸)可以降低血液中的胆固醇和低密度脂蛋白,而增加高密度脂蛋白。然而,当NA被用于治疗血脂异常时,它引起皮肤血管舒张的强烈副作用,通常被称为潮红。最近的研究表明,NA可能会通过降低热敏辣椒素受体TRPV1离子通道的激活阈值温度而引起潮红,从而导致其在体温下被激活。这一发现使人们怀疑NA是否也可能与同源的热敏TRPV2-4通道相互作用,特别是考虑到TRPV3和TRPV4在发生大量潮红反应的皮肤角质形成细胞中大量表达。我们发现,NA确实能增强TRPV3,同时抑制TRPV2和TRPV4。与这些门控效应一致,NA降低了TRPV3的热激活阈值,但提高了TRPV4的热激活阈值。我们进一步发现,胞外NA大大延长了TRPV1的活性,这可能进一步增强了直接激活作用。与对TRPV1-4通道的广泛门控作用一致,本研究的证据表明NA可能与这些TRPV通道的共同激动剂2-氨基乙氧基二苯基硼酸酯(2-APB)共享相同的激活途径。这些发现为TRPV通道NA调控的分子机制提供了新的思路。

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