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Conserved allosteric pathways for activation of TRPV3 revealed through engineering vanilloid-sensitivity

机译:工程类香草素敏感性揭示了保守的变构途径激活TRPV3

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摘要

The Transient Receptor Potential Vanilloid 1 (TRPV) channel is activated by an array of stimuli, including heat and vanilloid compounds. The TRPV1 homologues TRPV2 and TRPV3 are also activated by heat, but sensitivity to vanilloids and many other agonists is not conserved among TRPV subfamily members. It was recently discovered that four mutations in TRPV2 are sufficient to render the channel sensitive to the TRPV1-specific vanilloid agonist resiniferatoxin (RTx). Here, we show that mutation of six residues in TRPV3 corresponding to the vanilloid site in TRPV1 is sufficient to engineer RTx binding. However, robust activation of TRPV3 by RTx requires facilitation of channel opening by introducing mutations in the pore, temperatures > 30°C, or sensitization with another agonist. Our results demonstrate that the energetics of channel activation can determine the apparent sensitivity to a stimulus and suggest that allosteric pathways for activation are conserved in the TRPV family.
机译:瞬态受体潜在香草酸1(TRPV)通道被一系列刺激激活,包括热和香草素化合物。 TRPV1的同系物TRPV2和TRPV3也可以通过加热激活,但在TRPV的亚家族成员中,对类香草素和许多其他激动剂的敏感性却未得到保留。最近发现,TRPV2中的四个突变足以使通道对TRPV1特异性类香草酸激动剂resiniferatoxin(RTx)敏感。在这里,我们显示TRPV3中六个残基的突变对应于TRPV1中的类香草醇位点足以工程化RTx结合。然而,RTx对TRPV3的强力激活需要通过在孔中引入突变,温度> 30°C或用另一种激动剂敏化来促进通道开放。我们的结果表明,通道激活的能量学可以确定对刺激的表观敏感性,并表明在TRPV家族中,变构激活途径是保守的。

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