Intracallosal Neuronal Nitric Oxide Synthase Neurons Colocalize With Neurokinin 1 Substance P Receptor in the Rat

The corpus callosum (cc) contains nitric oxide (NO)-producing neurons. Because NO is a potent vasodilator, these neurons could translate neuronal signals into vascular responses that can be detected by functional brain imaging. Substance P (SP), one of the most widely expressed peptides in the CNS, also produces vasomotor responses by inducing calcium release from intracellular stores through its preferred neurokinin 1 (NK1) receptor, thus inducing NO production via activation of neuronal NO synthase (nNOS). Single- and double-labeling experiments were performed to establish whether NK1-immunopositive neurons (NK1(IP)-n) are found in the rat cc and the extent of NK1 colocalization with nNOS. NK1(IP)-n were seen to constitute a large neuronal population in the cc and had a distribution similar to that of nNOS(IP) neurons (nNOS(IP)-n). NK1(IP)-n were numerous in the lateral cc and gradually decreased in the more medial portions, where they were few or absent. Intracallosal NK1(IP)-n and their dendritic trees were intensely labeled, allowing classification into four morphological types: bipolar, round, polygonal, and pyramidal. Confocal microscopic examination demonstrated that nearly all NK1(IP)-n contained nNOS (96.43%) and that 84.59% of nNOS(IP)-n co-expressed NK1. These data suggest that the majority of intracallosal neurons can release NO as a result of the action of SP. A small proportion of nNOS(IP)-n does not contain NK1 and is not activated by SP; these neurons may release NO via alternative mechanisms. The possible mechanisms by which intracallosal neurons release NO are also reviewed. J. Comp. Neurol. 523:589-607, 2015. (c) 2014 Wiley Periodicals, Inc.