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Dopaminergic neurons intrinsic to the striatum.

机译:纹状体固有的多巴胺能神经元。

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The striatum - the largest integrative component of the basal ganglia - harbors a population of neurons that express the enzyme tyrosine hydroxylase (TH), a faithful marker of dopaminergic neurons. The dopaminergic nature of these neurons is further supported by the fact that they express the dopamine (DA) transporter (DAT) and the nuclear orphan receptor Nurr1, a transcription factor essential for the expression of the DA phenotype by midbrain neurons. The vast majority of these neurons are morphologically similar to the medium-sized aspiny striatal interneurons and they all express the enzyme GAD(65). The striatal TH-positive neurons increase markedly in number in animal models of Parkinson's disease (PD), where striatal DA concentrations are low, but this increase is abolished by L-dopa treatment. Hence, local DA concentrations appear to regulate the numerical density of this ectopic neuronal population, a phenomenon that is more likely the result of a shift in the phenotype of preexistent striatal interneurons rather than the recruitment of newborn neurons that will develop a DA phenotype. Altogether, these findings suggest that striatal TH-positive neurons act as a local source of DA and, as such, are part of a compensatory mechanism that could be artificially enhanced to alleviate or delay PD symptoms.
机译:纹状体-基底神经节的最大组成部分-含有大量表达酪氨酸羟化酶(TH)的神经元,酪氨酸羟化酶是多巴胺能神经元的忠实标记。这些神经元表达多巴胺(DA)转运蛋白(DAT)和核孤儿受体Nurr1,这是中脑神经元表达DA表型必不可少的转录因子,这一事实进一步支持了这些神经元的多巴胺能性质。这些神经元的绝大多数在形态上与中等大小的棘状纹状体中间神经元相似,并且都表达GAD(65)酶。在帕金森病(PD)的动物模型中,纹状体TH阳性神经元的数量显着增加,帕金森病(PD)的纹状体DA浓度较低,但是这种增加被左旋多巴治疗所消除。因此,局部DA浓度似乎可以调节该异位神经元种群的数量密度,这种现象很可能是先前存在的纹状体中间神经元表型发生转变的结果,而不是新生的神经元会发展为DA表型。总而言之,这些发现表明纹状体TH阳性神经元是DA的局部来源,因此是补偿机制的一部分,可以人为增强补偿机制以减轻或延迟PD症状。

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