Serotonin and serotoninergic neurons. A radioautographic and immunocytochemical study of the nucleus raphe dorsalis and nucleus dorsomedialis hypothalami.
F Arezki, I Afailal, O Bosler, H W Steinbusch, A Calas
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引用次数: 0
Abstract
In an attempt to define cytophysiological criteria with which to establish whether or not a given neuron is serotoninergic, radioautography was combined with serotonin (5-HT) immunocytochemistry on the same sections from the nucleus raphe dorsalis (NRD) and/or nucleus dorsomedialis hypothalami (NDM) in rats subjected to intraventricular administrations of (3H)-5-HT or (3H)-dopamine (DA). All the (3H)-5-HT-accumulating neurons (cell bodies, dendrites and terminals) were found to be distinct from the (3H)-DA labeled ones and invariably immunostained for 5-HT in both regions studied. However, some immunoreactive neuronal elements within the area of tracer diffusion did not exhibit significant radioautographic labeling. In the NDM where 5-HT immunoreactive nerve cells could be detected only after intraventricular administration of 5-HT, these were found to be definitely distinct from the tyrosine hydroxylase immunoreactive and (3H)-DA labeled neurons of the dopaminergic periventricular-arcuate complex. After immunostaining for GAD at the electron microscopic level, (3H)-5-HT labeled nerve cells and terminals were not found to exhibit any significant immunoreactivity. Associations between (3H)-DA labeled and GAD immunoreactive processes with 5-HT immunoreactive or (3H)-5-HT-accumulating neurons, respectively, could also be observed in the NDM. When considered as a whole along with previous observations by other authors indicating a probable synthesis of 5-HT within NDM neurons, our data suggest that a given neuron can be classified as serotoninergic on the sole basis of its ability to selectively take up exogenous 5-HT under experimental conditions compatible with non interspecific labeling of catecholaminergic neurons. They also provide valuable information on the neurochemical environment and possible control of central serotoninergic neurons.