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Literature DB >> 33871877

Involvement of TRPC5 channels, inwardly rectifying K⁺ channels, PLCβ and PIP₂ in vasopressin-mediated excitation of medial central amygdala neurons.

Cody A Boyle¹, Binqi Hu¹, Kati L Quaintance¹, Saobo Lei¹.

Abstract

KEY POINTS: Activation of V1a vasopressin receptors facilitates neuronal excitability in the medial nucleus of central amygdala (CeM) V1a receptor activation excites about 80% CeM neurons by opening a cationic conductance and about 20% CeM neurons by suppressing an inwardly rectifying K+ (Kir) channel The cationic conductance activated by V1a receptors is identified as TRPC5 channels PLCβ-mediated depletion of PIP2 is involved in V1a receptor-elicited excitation of CeM neurons Intracellular Ca2+ release and PKC are unnecessary for V1a receptor-mediated excitation of CeM neurons ABSTRACT: Arginine vasopressin (AVP) serves as a hormone in the periphery to modulate water homeostasis and a neuromodulator in the brain to regulate a diverse range of functions including anxiety, social behaviour, cognitive activities and nociception. The amygdala is an essential brain region involved in modulating defensive and appetitive behaviours, pain and alcohol use disorders. Whereas activation of V1a receptors in the medial nucleus of the central amygdala (CeM) increases neuronal excitability, the involved ionic and signalling mechanisms have not been determined. We found that activation of V1a receptors in the CeM facilitated neuronal excitability predominantly by opening TRPC5 channels, although AVP excited about one fifth of the CeM neurons via suppressing an inwardly rectifying K+ (Kir) channel. G proteins and phospholipase Cβ (PLCβ) were required for AVP-elicited excitation of CeM neurons, whereas intracellular Ca2+ release and the activity of protein kinase C were unnecessary. Prevention of the depletion of phosphatidylinositol 4,5-bisphosphate (PIP2 ) blocked AVP-induced excitation of CeM neurons, suggesting that PLCβ-mediated depletion of PIP2 is involved in AVP-mediated excitation of CeM neurons. Our results may provide a cellular and molecular mechanism to explain the anxiogenic effects of AVP in the amygdala.

Entities: Chemical

Keywords: K+ channels; action potential; cation channels; depolarization; excitability; peptide; synapse

Mesh：

Substances：

Year: 2021 PMID： 33871877 PMCID： PMC8207704 DOI： 10.1113/JP281260

Source DB: PubMed Journal: J Physiol ISSN： 0022-3751 Impact factor: 6.228

104 in total

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Involvement of TRPC5 channels, inwardly rectifying K⁺ channels, PLCβ and PIP₂ in vasopressin-mediated excitation of medial central amygdala neurons.

1. Long-term depression in identified stellate neurons of juvenile rat entorhinal cortex.

2. Distinct mechanisms of ethanol potentiation of local and paracapsular GABAergic synapses in the rat basolateral amygdala.

3. Differential activation of arginine-vasopressin receptor subtypes in the amygdaloid modulation of anxiety in the rat by arginine-vasopressin.

4. Molecular cloning and functional characterization of a novel receptor-activated TRP Ca2+ channel from mouse brain.

5. TRPC1 and TRPC5 form a novel cation channel in mammalian brain.

6. Fear conditioning potentiates synaptic transmission onto long-range projection neurons in the lateral subdivision of central amygdala.

7. Depletion of phosphatidylinositol 4,5-bisphosphate by activation of phospholipase C-coupled receptors causes slow inhibition but not desensitization of G protein-gated inward rectifier K+ current in atrial myocytes.

8. On the mechanism of GIRK2 channel gating by phosphatidylinositol bisphosphate, sodium, and the Gβγ dimer.

9. Vasopressin and oxytocin excite distinct neuronal populations in the central amygdala.

10. Acute Treatment with a Novel TRPC4/C5 Channel Inhibitor Produces Antidepressant and Anxiolytic-Like Effects in Mice.

Review 1. Calcium signaling in neurodevelopment and pathophysiology of autism spectrum disorders.

Review 2. Potentials of Neuropeptides as Therapeutic Agents for Neurological Diseases.

3. Ionic and signaling mechanisms involved in neurotensin-mediated excitation of central amygdala neurons.