Ouimet C C, Miller P E, Hemmings H C, Walaas S I, Greengard P
J Neurosci. 1984 Jan;4(1):111-24. doi: 10.1523/JNEUROSCI.04-01-00111.1984.
Immunocytochemical studies have been carried out to determine the regional and cellular distribution of DARPP-32, a protein the phosphorylation of which can be regulated by dopamine and cAMP in intact cells. These immunocytochemical studies indicate tha DARPP-32 is localized primarily in those brain regions enriched in dopaminergic nerve terminals. Moreover, the staining pattern supports the conclusion that the DARPP-32 is present in dopaminoceptive neurons, i.e., neurons that receive a dopamine input, and that it is absent from the dopaminergic neurons themselves. Within the caudatoputamen, nucleus accumbens, olfactory tubercle, bed nucleus of the stria terminalis, and portions of the amygdaloid complex, all of which receive a strong dopamine input, DARPP-32 immunoreactivity is present in neuronal cell bodies and dendrites. In brain regions that are known to receive projections from these nuclei, puncta (presumed nerve terminals) are strongly immunoreactive for DARPP-32 but indigenous cell bodies and dendrites are not immunoreactive. These target areas include the globus pallidus, ventral pallidum, entopeduncular nucleus, and the pars reticulata of the substantia nigra. No immunoreactivity is detected in neuronal cell bodies or dendrites in any of the dopaminergic nuclei. Furthermore, nerve terminals immunoreactive for DARPP-32 do not resemble dopaminergic varicosities in either their morphology or their pattern of distribution. Many neurons are weakly immunoreactive for DARPP-32 and some of these are found in areas that apparently lack a dopaminergic input: weakly labeled neuronal cell bodies and dendrites were found throughout the neocortex, primarily in layer VI, and in the Purkinje neurons of the cerebellum. DARPP-32 immunoreactivity is also present in certain glial cells, especially in the median eminence, arcuate nucleus, and medial habenula. The present immunocytochemical studies, taken together with biochemical studies (Hemmings, H.C., Jr., A.C. Nairn, D.W. Aswad, and P. Greengard (1984) J. Neurosci. 4: 99-110; Walaas, S.I., and P. Greengard (1984) J. Neurosci. 4: 84-98) on DARPP-32, indicate that DARPP-32, is present in the subclass of dopaminoceptive neurons containing D-1 receptors (dopamine receptors coupled to adenylate cyclase). DARPP-32 may be an effective marker for certain of the actions of dopamine that are mediated through cAMP and its associated protein kinase.
已开展免疫细胞化学研究,以确定DARPP - 32的区域和细胞分布。DARPP - 32是一种蛋白质,其磷酸化可在完整细胞中受多巴胺和环磷酸腺苷调节。这些免疫细胞化学研究表明,DARPP - 32主要定位于富含多巴胺能神经末梢的脑区。此外,染色模式支持以下结论:DARPP - 32存在于多巴胺感受神经元中,即接受多巴胺输入的神经元,而多巴胺能神经元本身不存在该蛋白。在尾状核壳核、伏隔核、嗅结节、终纹床核和杏仁复合体的部分区域,所有这些区域都接受强烈的多巴胺输入,DARPP - 32免疫反应性存在于神经元细胞体和树突中。在已知接受这些核投射的脑区,小点(推测为神经末梢)对DARPP - 32有强烈免疫反应,但原生细胞体和树突没有免疫反应。这些靶区域包括苍白球、腹侧苍白球、内苍白球核和黑质网状部。在任何多巴胺能核的神经元细胞体或树突中均未检测到免疫反应性。此外,对DARPP - 32有免疫反应性的神经末梢在形态或分布模式上均与多巴胺能曲张体不同。许多神经元对DARPP - 32有弱免疫反应性,其中一些位于明显缺乏多巴胺能输入的区域:在整个新皮层,主要是在第VI层,以及小脑的浦肯野神经元中发现了弱标记的神经元细胞体和树突。DARPP - 32免疫反应性也存在于某些神经胶质细胞中,尤其是在正中隆起、弓状核和内侧缰核。目前的免疫细胞化学研究与关于DARPP - 32的生化研究(小亨明斯,H.C.、A.C.奈恩、D.W.阿斯瓦德和P.格林加德(1984年)《神经科学杂志》4:99 - 110;瓦拉斯,S.I.和P.格林加德(1984年)《神经科学杂志》4:84 - 98)一起表明,DARPP - 32存在于含有D - 1受体(与腺苷酸环化酶偶联的多巴胺受体)的多巴胺感受神经元亚类中。DARPP - 32可能是多巴胺某些通过环磷酸腺苷及其相关蛋白激酶介导的作用的有效标志物。
