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首页> 外文期刊>Molecular Neurobiology >Protective Actions of the Vesicular Monoamine Transporter 2 (VMAT2) in Monoaminergic Neurons
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Protective Actions of the Vesicular Monoamine Transporter 2 (VMAT2) in Monoaminergic Neurons

机译:水泡单胺转运蛋白2(VMAT2)在单胺能神经元中的保护作用。

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摘要

Vesicular monoamine transporters (VMATs) are responsible for the packaging of neurotransmitters such as dopamine, serotonin, norepinephrine, and epinephrine into synaptic vesicles. These proteins evolved from precursors in the major facilitator superfamily of transporters and are among the members of the toxin extruding antiporter family. While the primary function of VMATs is to sequester neurotransmitters within vesicles, they can also translocate toxicants away from cytosolic sites of action. In the case of dopamine, this dual role of VMAT2 is combined—dopamine is more readily oxidized in the cytosol where it can cause oxidative stress so packaging into vesicles serves two purposes: neurotransmission and neuroprotection. Furthermore, the deleterious effects of exogenous toxicants on dopamine neurons, such as MPTP, can be attenuated by VMAT2 activity. The active metabolite of MPTP can be kept within vesicles and prevented from disrupting mitochondrial function thereby sparing the dopamine neuron. The highly addictive drug methamphetamine is also neurotoxic to dopamine neurons by using dopamine itself to destroy the axon terminals. Methamphetamine interferes with vesicular sequestration and increases the production of dopamine, escalating the amount in the cytosol and leading to oxidative damage of terminal components. Vesicular transport seems to resist this process by sequestering much of the excess dopamine, which is illustrated by the enhanced methamphetamine neurotoxicity in VMAT2-deficient mice. It is increasingly evident that VMAT2 provides neuroprotection from both endogenous and exogenous toxicants and that while VMAT2 has been adapted by eukaryotes for synaptic transmission, it is derived from phylogenetically ancient proteins that originally evolved for the purpose of cellular protection.
机译:囊泡单胺转运蛋白(VMAT)负责将神经递质(如多巴胺,5-羟色胺,去甲肾上腺素和肾上腺素)包装到突触小泡中。这些蛋白质是从转运蛋白主要易化子超家族的前体进化而来的,属于毒素挤出反转运蛋白家族的成员。虽然VMAT的主要功能是将神经递质隔离在囊泡中,但它们也可以使毒物从胞质作用位点转移。在多巴胺的情况下,VMAT2的双重作用被结合在一起-多巴胺在细胞质中更容易被氧化,在氧化酶中会引起氧化应激,因此包装入囊泡有两个目的:神经传递和神经保护。此外,VMAT2活性可以减弱外源性毒物对多巴胺神经元(如MPTP)的有害作用。 MPTP的活性代谢物可保留在囊泡中,并防止破坏线粒体功能,从而节省多巴胺神经元。通过使用多巴胺本身破坏轴突末端,高度上瘾的药物甲基苯丙胺对多巴胺神经元也具有神经毒性。甲基苯丙胺会干扰水泡的螯合并增加多巴胺的产生,从而增加细胞溶质的含量并导致末端成分的氧化损伤。囊泡运输似乎通过隔离大量过量的多巴胺而抵抗了这一过程,这在缺乏VMAT2的小鼠体内甲基苯丙胺神经毒性增强了。越来越明显的是,VMAT2对内源性毒物和外源性毒物均具有神经保护作用,并且虽然真核生物已使VMAT2适应突触传递,但VMAT2源自系统发育的古老蛋白质,最初是出于细胞保护的目的而进化的。

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