Autor: |
Stepanyuk AR; Bogomoletz Institute of Physiology, Kiev, Ukraine; State Key Laboratory of Molecular and Cellular Biology, Kiev, Ukraine., Belan PV; Bogomoletz Institute of Physiology, Kiev, Ukraine; State Key Laboratory of Molecular and Cellular Biology, Kiev, Ukraine., Kononenko NI; Bogomoletz Institute of Physiology, Kiev, Ukraine; State Key Laboratory of Molecular and Cellular Biology, Kiev, Ukraine. |
Jazyk: |
angličtina |
Zdroj: |
PloS one [PLoS One] 2014 Sep 05; Vol. 9 (9), pp. e106152. Date of Electronic Publication: 2014 Sep 05 (Print Publication: 2014). |
DOI: |
10.1371/journal.pone.0106152 |
Abstrakt: |
When dispersed and cultured in a multielectrode dish (MED), suprachiasmatic nucleus (SCN) neurons express fast oscillations of firing rate (FOFR; fast relative to the circadian cycle), with burst duration ∼10 min, and interburst interval varying from 20 to 60 min in different cells but remaining nevertheless rather regular in individual cells. In many cases, separate neurons in distant parts of the 1 mm recording area of a MED exhibited correlated FOFR. Neither the mechanism of FOFR nor the mechanism of their synchronization among neurons is known. Based on recent data implicating vasoactive intestinal polypeptide (VIP) as a key intercellular synchronizing agent, we built a model in which VIP acts as both a feedback regulator to generate FOFR in individual neurons, and a diffusible synchronizing agent to produce coherent electrical output of a neuronal network. In our model, VIP binding to its (VPAC2) receptors acts through Gs G-proteins to activate adenylyl cyclase (AC), increase intracellular cAMP, and open cyclic-nucleotide-gated (CNG) cation channels, thus depolarizing the cell and generating neuronal firing to release VIP. In parallel, slowly developing homologous desensitization and internalization of VPAC2 receptors terminates elevation of cAMP and thereby provides an interpulse silent interval. Through mathematical modeling, we show that this VIP/VPAC2/AC/cAMP/CNG-channel mechanism is sufficient for generating reliable FOFR in single neurons. When our model for FOFR is combined with a published model of synchronization of circadian rhythms based on VIP/VPAC2 and Per gene regulation synchronization of circadian rhythms is significantly accelerated. These results suggest that (a) auto/paracrine regulation by VIP/VPAC2 and intracellular AC/cAMP/CNG-channels are sufficient to provide robust FOFR and synchrony among neurons in a heterogeneous network, and (b) this system may also participate in synchronization of circadian rhythms. |
Databáze: |
MEDLINE |
Externí odkaz: |
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