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首页> 外文期刊>Frontiers in Molecular Biosciences >A Single Mutation in the Outer Lipid-Facing Helix of a Pentameric Ligand-Gated Ion Channel Affects Channel Function Through a Radially-Propagating Mechanism
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A Single Mutation in the Outer Lipid-Facing Helix of a Pentameric Ligand-Gated Ion Channel Affects Channel Function Through a Radially-Propagating Mechanism

机译:面向脂质配体的离子通道的外脂的螺旋中的单一突变通过径向传播机构影响通道功能

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Pentameric ligand-gated ion channels (pLGICs) mediate fast synaptic transmission and are crucial drug targets. Their gating mechanism is triggered by ligand binding in the extracellular domain that culminates in the opening of a hydrophobic gate in the transmembrane domain. This domain is made of four α-helices (M1 to M4). Recently the outer lipid-facing helix (M4) has been shown to be key to receptor function, however its role in channel opening is still poorly understood. It could act through its neighbouring helices (M1/M3), or via the M4 tip interacting with the pivotal Cys-loop in the extracellular domain. Mutation of a single M4 tyrosine (Y441) to alanine renders one pLGIC - the 5-HT3A receptor - unable to function despite robust ligand binding. Using Y441A as a proxy for M4 function, we here predict likely paths of Y441 action using molecular dynamics, and test these predictions with functional assays of mutant receptors in HEK cells and Xenopus oocytes using fluorescent membrane potential sensitive dye and two-electrode voltage clamp respectively. We show that Y441 does not act via the M4 tip or Cys-loop, but instead connects radially through M1 to a residue near the ion channel hydrophobic gate on the pore-lining helix M2. This demonstrates the active role of the M4 helix in channel opening.
机译:五聚体配体门通道(PLGICS)介导快速突触传递,是关键的药物靶标。它们的浇注机构通过在细胞外结构域中的配体结合而触发,其在跨膜结构域中的疏水栅的开口中染色。该域由四个α-螺旋(M1至M4)制成。最近,外部脂质的螺旋(M4)已被证明是受体功能的关键,但其在渠道开口中的作用仍然很清楚。它可以通过其相邻的螺旋(M1 / m3)或通过与细胞外结构域中的枢轴综合循环相互作用的M4尖端作用。单个M4酪氨酸(Y441)的突变呈丙氨酸呈一个PLGIC - 5-HT3A受体 - 尽管坚固的配体结合,但是尽管具有稳健的配体结合。使用Y441A作为M4功能的代理,我们在这里预测了使用分子动力学的Y441动作的可能路径,并使用荧光膜电位敏感染料和双电极电压夹和两电极电压夹具的HEK细胞和外爪卵母细胞中的突变受体功能测定的这些预测。我们表明,Y441不通过M4尖端或电源环作用,而是通过径向通过M1连接到孔隙螺旋M2上的离子通道疏水栅极附近的残留物。这证明了M4螺旋在通道开口中的积极作用。

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