[HTML][HTML] A Gαs DREADD mouse for selective modulation of cAMP production in striatopallidal neurons

MS Farrell, Y Pei, Y Wan, PN Yadav… - …, 2013 - nature.com
MS Farrell, Y Pei, Y Wan, PN Yadav, TL Daigle, DJ Urban, HM Lee, N Sciaky, A Simmons…
Neuropsychopharmacology, 2013nature.com
Here, we describe a newly generated transgenic mouse in which the Gs DREADD (rM3Ds),
an engineered G protein-coupled receptor, is selectively expressed in striatopallidal medium
spiny neurons (MSNs). We first show that in vitro, rM3Ds can couple to Gα olf and induce
cAMP accumulation in cultured neurons and HEK-T cells. The rM3Ds was then selectively
and stably expressed in striatopallidal neurons by creating a transgenic mouse in which an
adenosine2A (adora2a) receptor-containing bacterial artificial chromosome was employed …
Abstract
Here, we describe a newly generated transgenic mouse in which the Gs DREADD (rM3Ds), an engineered G protein-coupled receptor, is selectively expressed in striatopallidal medium spiny neurons (MSNs). We first show that in vitro, rM3Ds can couple to Gα olf and induce cAMP accumulation in cultured neurons and HEK-T cells. The rM3Ds was then selectively and stably expressed in striatopallidal neurons by creating a transgenic mouse in which an adenosine2A (adora2a) receptor-containing bacterial artificial chromosome was employed to drive rM3Ds expression. In the adora2A-rM3Ds mouse, activation of rM3Ds by clozapine-N-oxide (CNO) induces DARPP-32 phosphorylation, consistent with the known consequence of activation of endogenous striatal Gα s-coupled GPCRs. We then tested whether CNO administration would produce behavioral responses associated with striatopallidal G s signaling and in this regard CNO dose-dependently decreases spontaneous locomotor activity and inhibits novelty induced locomotor activity. Last, we show that CNO prevented behavioral sensitization to amphetamine and increased AMPAR/NMDAR ratios in transgene-expressing neurons of the nucleus accumbens shell. These studies demonstrate the utility of adora2a-rM3Ds transgenic mice for the selective and noninvasive modulation of Gα s signaling in specific neuronal populations in vivo. This unique tool provides a new resource for elucidating the roles of striatopallidal MSN Gα s signaling in other neurobehavioral contexts.
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