4.5 Article

Neuronal localization of m1 muscarinic receptor immunoreactivity in the monkey basolateral amygdala

Journal

JOURNAL OF COMPARATIVE NEUROLOGY
Volume 529, Issue 10, Pages 2450-2463

Publisher

WILEY
DOI: 10.1002/cne.25104

Keywords

acetylcholine; immunohistochemistry; interneurons; muscarinic receptors; primate; pyramidal cells

Funding

  1. National Institute of Mental Health [R01MH104638]
  2. Yerkes Regional Primate Research Center [P51OD011132]

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The study revealed that both pyramidal projection neurons (PNs) and inhibitory interneurons (INs) in the primate BNC express M1Rs, with a particularly high expression in PNs. The findings also showed that a significant portion of GAD-expressing INs in the BNC are also M1R positive, indicating the potential impact of M1R positive allosteric modulators in targeting both PNs and INs in the BNC.
The basolateral nuclear complex (BNC) of the amygdala plays an important role in the generation of emotional/motivational behavior and the consolidation of emotional memories. Activation of M1 cholinergic receptors (M1Rs) in the BNC is critical for memory consolidation. Previous receptor binding studies in the monkey amygdala demonstrated that the BNC has a high density of M1Rs, but did not have sufficient resolution to identify which neurons in the BNC expressed them. This was accomplished in the present immunohistochemical investigation using an antibody for the m1 receptor (m1R). Analysis of m1Rs in the monkey BNC using immunoperoxidase techniques revealed that their expression was very dense in the BNC, and suggested that virtually all of the pyramidal projection neurons (PNs) in all of the BNC nuclei were m1R-immunoreactive (m1R+). This was confirmed with dual-labeling immunofluorescence using staining for calcium/calmodulin-dependent protein kinase II (CaMK) as a marker for BNC PNs. However, additional dual-labeling studies indicated that one-third of inhibitory interneurons (INs) expressing glutamic acid decarboxylase (GAD) were also m1R+. Moreover, the finding that 60% of parvalbumin (PV) immunoreactive neurons were m1R+ indicated that this IN subpopulation was the main GAD+ subpopulation exhibiting m1R expression. The cholinergic innervation of the amygdala is greatly reduced in Alzheimer's disease and there is currently considerable interest in developing selective M1R positive allosteric modulators (PAMs) to treat the symptoms. The results of the present study indicate that M1Rs in both PNs and INs in the primate BNC would be targeted by M1R PAMs.

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