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去甲肾上腺素转运体具有通道传导模式。

Norepinephrine transporters have channel modes of conduction.

作者信息

Galli A, Blakely R D, DeFelice L J

机构信息

Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, TN 37232-6600, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Aug 6;93(16):8671-6. doi: 10.1073/pnas.93.16.8671.

Abstract

Neurotransmitter transporters couple to existing ion gradients to achieve reuptake of transmitter into presynaptic terminals. For coupled cotransport, substrates and ions cross the membrane in fixed stoichiometry. This is in contrast to ion channels, which carry an arbitrary number of ions depending on the channel open time. Members of the gamma-aminobutyric acid transporter gene family presumably function with fixed stoichiometry in which a set number of ions cotransport with one transmitter molecule. Here we report channel-like events from a presumably fixed stoichiometry [norepinephrine (NE)+, Na+, and Cl-], human NE (hNET) in the gamma-aminobutyric acid transporter gene family. These events are stimulated by NE and by guanethidine, an hNET substrate, and they are blocked by cocaine and the antidepressant desipramine. Voltage-clamp data combined with NE uptake data from these same cells indicate that hNETs have two functional modes of conduction: a classical transporter mode (T-mode) and a novel channel mode (C-mode). Both T-mode and C-mode are gated by the same substrates and antagonized by the same blockers. T-mode is putatively electrogenic because the transmitter and cotransported ions sum to one net charge. However, C-mode carries virtually all of the transmitter-induced current, even though it occurs with low probability. This is because each C-mode opening transports hundreds of charges per event. The existence of a channel mode of conduction in a previously established fixed-stoichiometry transporter suggests the appearance of an aqueous pore through the transporter protein during the transport cycle and may have significance for transporter regulation.

摘要

神经递质转运体与现有的离子梯度偶联,以实现递质重新摄取到突触前终末。对于偶联共转运,底物和离子以固定的化学计量比穿过膜。这与离子通道不同,离子通道根据通道开放时间携带任意数量的离子。γ-氨基丁酸转运体基因家族的成员可能以固定的化学计量比发挥作用,即一定数量的离子与一个递质分子共转运。在此我们报告了γ-氨基丁酸转运体基因家族中一种可能具有固定化学计量比(去甲肾上腺素(NE)+、Na+和Cl-)的人NE(hNET)的类似通道的事件。这些事件受到NE和hNET底物胍乙啶的刺激,并被可卡因和抗抑郁药地昔帕明阻断。电压钳数据与来自这些相同细胞的NE摄取数据相结合表明,hNETs有两种功能传导模式:经典转运体模式(T模式)和新型通道模式(C模式)。T模式和C模式都由相同的底物门控,并被相同的阻滞剂拮抗。T模式被认为是生电的,因为递质和共转运的离子总和为一个净电荷。然而,C模式几乎承载了所有递质诱导的电流,尽管其发生概率较低。这是因为每个C模式开放事件每次转运数百个电荷。在先前已确定的固定化学计量比转运体中存在通道传导模式,这表明在转运循环过程中通过转运体蛋白出现了一个水相孔,并且可能对转运体调节具有重要意义。

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Norepinephrine transporters have channel modes of conduction.去甲肾上腺素转运体具有通道传导模式。
Proc Natl Acad Sci U S A. 1996 Aug 6;93(16):8671-6. doi: 10.1073/pnas.93.16.8671.

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