Sobreviela T, Clary D O, Reichardt L F, Brandabur M M, Kordower J H, Mufson E J
Department of Neurological Sciences, Rush Presbyterian-St. Luke's Medical Center, Chicago, Illinois 60612.
J Comp Neurol. 1994 Dec 22;350(4):587-611. doi: 10.1002/cne.903500407.
The present investigation used an antibody directed against the extracellular domain of the signal transducing nerve growth factor receptor, trkA, to reveal immunoreactive perikarya or fibers within the olfactory bulb and tubercle, cingulate cortex, nucleus accumbens, striatum, endopiriform nucleus, septal/diagonal band complex, nucleus basalis, hippocampal complex, thalamic paraventricular and reuniens nuclei, periventricular hypothalamus, interpeduncular nucleus, mesencephalic nucleus of the fifth nerve, dorsal nucleus of the lateral lemniscus, prepositus hypoglossal nucleus, ventral cochlear nucleus, ventral lateral tegmentum, medial vestibular nucleus, spinal trigeminal nucleus oralis, nucleus of the solitary tract, raphe nuclei, and spinal cord. Colocalization experiments revealed that virtually all striatal trkA-immunoreactive neurons (> 99%) coexpressed choline acetyltransferase (ChAT) but not p75 nerve growth factor receptor (NGFR). Within the septal/diagonal band complex virtually all trkA neurons (> 95%) coexpressed both ChAT and p75 NGFR. More caudally, dual stained sections revealed numerous trkA/ChAT (> 80%) and trkA/p75 NGFR (> 95%) immunoreactive neurons within the nucleus basalis. In the brainstem, raphe serotonergic neurons (45%) coexpressed trkA. Sections stained with a pan-trk antibody that recognizes primarily trkA, as well as trkB and trkC, labeled neurons within all of these regions as well as within the hypothalamic arcuate, supramammilary, and supraoptic nuclei, hippocampus, inferior and superior colliculus, substantia nigra, ventral tegmental area of T'sai, and cerebellular Purkinje cells. Virtually all of these other regions with the exception of the cerebellum also expressed pan-trk immunoreactivity in the monkey. The widespread expression of trkA throughout the central neural axis suggests that this receptor may play a role in signal transduction mechanisms linked to NGF-related substances in cholinergic basal forebrain and noncholinergic systems. These findings suggest that pharmacological use of ligands for trkA could have beneficial effects on the multiple neuronal systems that are affected in such disorders as Alzheimer's disease.
本研究使用一种针对信号转导神经生长因子受体trkA细胞外结构域的抗体,以揭示嗅球和嗅结节、扣带回皮质、伏隔核、纹状体、内梨状核、隔区/斜角带复合体、基底核、海马复合体、丘脑室旁核和连合核、室周下丘脑、脚间核、三叉神经中脑核、外侧丘系背核、舌下前置核、蜗腹侧核、腹侧被盖区、内侧前庭核、三叉神经脊束核吻侧亚核、孤束核、中缝核以及脊髓内的免疫反应性胞体或纤维。共定位实验显示,几乎所有纹状体trkA免疫反应性神经元(>99%)共表达胆碱乙酰转移酶(ChAT),但不表达p75神经生长因子受体(NGFR)。在隔区/斜角带复合体内,几乎所有trkA神经元(>95%)共表达ChAT和p75 NGFR。在更靠尾侧的区域,双重染色切片显示基底核内有大量trkA/ChAT(>80%)和trkA/p75 NGFR(>95%)免疫反应性神经元。在脑干中,中缝5-羟色胺能神经元(45%)共表达trkA。用一种主要识别trkA以及trkB和trkC的泛trk抗体染色的切片,标记了所有这些区域以及下丘脑弓状核、乳头体上核和视上核、海马、上下丘、黑质、蔡氏腹侧被盖区和小脑浦肯野细胞内的神经元。除小脑外,几乎所有这些其他区域在猴中也表达泛trk免疫反应性。trkA在整个中枢神经轴的广泛表达表明,该受体可能在与胆碱能基底前脑和非胆碱能系统中NGF相关物质相关的信号转导机制中发挥作用。这些发现表明,trkA配体的药理学应用可能对受阿尔茨海默病等疾病影响的多个神经元系统产生有益影响。