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首页> 外文期刊>Journal of chemical neuroanatomy >Non-dopaminergic neurons partly expressing dopaminergic phenotype: distribution in the brain, development and functional significance.
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Non-dopaminergic neurons partly expressing dopaminergic phenotype: distribution in the brain, development and functional significance.

机译:非多巴胺能神经元部分表达多巴胺能表型:在脑中的分布,发展和功能意义。

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摘要

Besides the dopaminergic (DA-ergic) neurons possessing the whole set of enzymes of DA synthesis from l-tyrosine and the DA membrane transporter (DAT), the neurons partly expressing the DA-ergic phenotype have been first discovered two decades ago. Most of the neurons express individual enzymes of DA synthesis, tyrosine hydroxylase (TH) or aromatic l-amino acid decarboxylase (AADC) and lack the DAT. A list of the neurons partly expressing the DA-ergic phenotype is not restricted to so-called monoenzymatic neurons, e.g. it includes some neurons co-expressing both enzymes of DA synthesis but lacking the DAT. In contrast to true DA-ergic neurons, monoenzymatic neurons and bienzymatic non-dopaminergic neurons lack the vesicular monoamine transporter 2 (VMAT2) that raises a question about the mechanisms of storing and release of their final synthetic products. Monoenzymatic neurons are widely distributed all through the brain in adulthood being in some brain regions even more numerous than DA-ergic neurons. Individual enzymes of DA synthesis are expressed in these neurons continuously or transiently in norm or under certain physiological conditions. Monoenzymatic neurons, particularly those expressing TH, appear to be even more numerous and more widely distributed in the brain during ontogenesis than in adulthood. Most populations of monoenzymatic TH neurons decrease in number or even disappear by puberty. Functional significance of monoenzymatic neurons remained uncertain for a long time after their discovery. Nevertheless, it has been shown that most monoenzymatic TH neurons and AADC neurons are capable to produce l-3,4-dihydroxyphenylalanine (L-DOPA) from l-tyrosine and DA from L-DOPA, respectively. L-DOPA produced in monoenzymatic TH neurons is assumed to play a role of a neurotransmitter or neuromodulator acting on target neurons via catecholamine receptors. Moreover, according to our hypothesis L-DOPA released from monoenzymatic TH neurons is captured by monoenzymatic AADC neurons for DA synthesis. Such cooperative synthesis of DA is considered as a compensatory reaction under a failure of DA-ergic neurons, e.g. in neurodegenerative diseases like hyperprolactinemia and Parkinson's disease.Thus, a substantial number of the brain neurons express partly the DA-ergic phenotype, mostly individual complementary enzymes of DA synthesis, serving to produce DA in cooperation that is supposed to be a compensatory reaction under the failure of DA-ergic neurons.
机译:除了拥有从l-酪氨酸和DA膜转运蛋白(DAT)合成DA的整套酶的多巴胺能(DA-能)神经元外,二十多年前首次发现了部分表达DA-能表型的神经元。大多数神经元表达DA合成的个别酶,酪氨酸羟化酶(TH)或芳香族1-氨基酸脱羧酶(AADC),但缺乏DAT。部分表达DA-能级表型的神经元的列表不限于所谓的单酶神经元,例如。它包括一些共表达DA合成酶但缺乏DAT的神经元。与真正的DA能神经元相反,单酶神经元和双酶非多巴胺能神经元缺乏囊泡单​​胺转运蛋白2(VMAT2),这引发了有关其最终合成产物的存储和释放机制的问题。成年后,单酶神经元在整个大脑中分布广泛,在某些大脑区域甚至比DA能神经元还多。在这些神经元中正常或在某些生理条件下连续或瞬时表达DA合成的各个酶。单酶神经元,特别是那些表达TH的神经元,在成虫过程中比在成年时期似乎在大脑中的分布更为广泛和广泛。大多数单酶TH神经元数量减少,甚至在青春期消失。发现单酶神经元的功能重要性很长一段时间仍不确定。然而,已经显示出大多数单酶TH神经元和AADC神经元能够分别从L-酪氨酸和L-DOPA产生1-3,4-二羟基苯丙氨酸(L-DOPA)。假定在单酶TH神经元中产生的L-DOPA发挥通过儿茶酚胺受体作用于目标神经元的神经递质或神经调节剂的作用。此外,根据我们的假设,从单酶TH神经元释放的L-DOPA被单酶AADC神经元捕获,用于DA合成。这种DA的协同合成被认为是在DA能神经元例如神经元衰竭时的补偿性反应。因此,大量的大脑神经元部分表达DA能量表型,主要是DA合成的各个互补酶,共同产生DA,这被认为是在这种情况下的代偿性反应。 DA能神经元的衰竭。

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