Disruption of Cholinergic Circuits as an Area for Targeted Drug Treatment of Alzheimer's Disease: In Vivo Assessment of Short-Term Plasticity in Rat Brain

Vergine Chavushyan; Ani Soghomonyan; Gohar Karapetyan; Karen Simonyan; Konstantin Yenkoyan

doi:10.3390/ph13100297

Disruption of Cholinergic Circuits as an Area for Targeted Drug Treatment of Alzheimer's Disease: In Vivo Assessment of Short-Term Plasticity in Rat Brain

Pharmaceuticals (Basel). 2020 Oct 9;13(10):297. doi: 10.3390/ph13100297.

Authors

Vergine Chavushyan^{1

2}, Ani Soghomonyan^{1

3}, Gohar Karapetyan^{1

3}, Karen Simonyan², Konstantin Yenkoyan^{1

3}

Affiliations

¹ Laboratory of Neuroscience, Yerevan State Medical University after M. Heratsi, Yerevan 0025, Armenia.
² Laboratory of Neuroendocrine Relations, L. Orbeli Institute of Physiology of NAS, Yerevan 0028, Armenia.
³ Department of Biochemistry, Yerevan State Medical University after M. Heratsi, Yerevan 0025, Armenia.

Abstract

The search for new therapeutics for the treatment of Alzheimer's disease (AD) is still in progress. Aberrant pathways of synaptic transmission in basal forebrain cholinergic neural circuits are thought to be associated with the progression of AD. However, the effect of amyloid-beta (Aβ) on short-term plasticity (STP) of cholinergic circuits in the nucleus basalis magnocellularis (NBM) is largely unknown. STP assessment in rat brain cholinergic circuitry may indicate a new target for AD cholinergic therapeutics. Thus, we aimed to study in vivo electrophysiological patterns of synaptic activity in NBM-hippocampus and NBM-basolateral amygdala circuits associated with AD-like neurodegeneration. The extracellular single-unit recordings of responses from the hippocampal and basolateral amygdala neurons to high-frequency stimulation (HFS) of the NBM were performed after intracerebroventricular injection of Aβ 25-35. We found that after Aβ 25-35 exposure the number of hippocampal neurons exhibiting inhibitory responses to HFS of NBM is decreased. The reverse tendency was seen in the basolateral amygdala inhibitory neural populations, whereas the number of amygdala neurons with excitatory responses decreased. The low intensity of inhibitory and excitatory responses during HFS and post-stimulus period is probably due to the anomalous basal synaptic transmission and excitability of hippocampal and amygdala neurons. These functional changes were accompanied by structural alteration of hippocampal, amygdala, and NBM neurons. We have thus demonstrated that Aβ 25-35 induces STP disruption in NBM-hippocampus and NBM-basolateral amygdala circuits as manifested by unbalanced excitatory/inhibitory responses and their frequency. The results of this study may contribute to a better understanding of synaptic integrity. We believe that advancing our understanding of in vivo mechanisms of synaptic plasticity disruption in specific neural circuits could lead to effective drug searches for AD treatment.

Keywords: amyloid-beta 25–35; basolateral amygdala; cholinergic circuit; hippocampus; nucleus basalis magnocellularis; short-term plasticity.

Abstract

Grants and funding