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Mutation K448E in the external loop 5 of rat GABA transporter rGAT1 induces pH sensitivity and alters substrate interactions

机译:大鼠GABA转运蛋白rGAT1外环5中的突变K448E诱导pH敏感性并改变底物相互作用

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摘要

class="enumerated" style="list-style-type:decimal">The effect of the mutation K448E in the rat GABA transporter rGAT1 was studied using heterologous expression in Xenopus oocytes and voltage clamp.At neutral pH, the transport-associated current vs. voltage (I–V) relationship of the mutated transporter was different from wild-type, and the pre-steady-state currents were shifted towards more positive potentials. The mutated transporter showed an increased apparent affinity for Na+ (e.g. 62 vs. 152 mm at −60 mV), while the opposite was true for GABA (e.g. 20 vs. 13 μm at −60 mV).In both isoforms changes in [Na+]o shifted the voltage dependence of the pre-steady-state and of the transport-associated currents by similar amounts.In the K448E form, the moved charge and the relaxation time constant were shifted by increasing pH towards positive potentials. The transport-associated current of the mutated transporter was strongly reduced by alkalinization, while acidification slightly decreased and distorted the shape of the I–V curve. Accordingly, uptake of [3H]GABA was strongly reduced in K448E at pH 9.0. The GABA apparent affinity of the mutated transporter was reduced by alkalinization, while acidification had the opposite result.These observations suggest that protonation of negatively charged residues may regulate the Na+ concentration in the proximity of the transporter. Calculation of the unidirectional rate constants for charge movement shows that, in the K448E form, the inward rate constant is increased at alkaline pH, while the outward rate constant does not change, in agreement with an effect due to mass action law.A possible explanation for the complex effect of pH on the transport-associated current may be found by combining changes in local [Na+]o with a direct action of pH on GABA concentration or affinity. Our results support the idea that the extracellular loop 5 may participate to form a vestibule to which sodium ions must have access before proceeding to the steps involving charge movement.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 利用异源表达在爪蟾卵母细胞和电压钳中研究了突变K448E在大鼠GABA转运蛋白rGAT1中的作用。 在中性pH值下,转运相关电流与电压(I–V)的关系突变的转运蛋白不同于野生型,稳态前的电流转向更正的电位。突变的转运蛋白对Na + 的表观亲和力增加(例如,在-60 mV时为62 vs. 152 mm),而对于GABA则相反(例如在60 mV时为20 vs. 13μm)。 。[Na + ] o的两种同工型中的变化都使稳态前电压和与运输相关的电流的电压依赖性相近。在K448E形式中,通过增加pH向正电势移动电荷和驰豫时间常数。碱化作用大大降低了突变型转运蛋白的与转运相关的电流,而酸化作用则略有下降,使IV曲线的形状失真。因此,在pH 9.0下,在K448E中[ 3 H] GABA的吸收大大降低。碱化降低了突变体转运蛋白的GABA表观亲和力,而酸化却产生了相反的结果。 这些观察结果表明带负电荷的残基的质子化可能调节Na + 的浓度。运输车附近。电荷运动的单向速率常数的计算表明,在K448E形式下,向内速率常数在碱性pH值下增加,而向外速率常数不变,这与质量作用定律引起的效果一致。 通过将局部[Na + ] o的变化与pH对GABA浓度或亲和力的直接作用相结合,可以找到pH对运输相关电流的复杂影响的可能解释。 。我们的结果支持以下想法:细胞外环5可能参与形成前庭,钠离子必须进入前庭才能进行涉及电荷移动的步骤。

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