AI Article Synopsis

  • The study investigates how protein kinase A (PKA) activity in striatal neurons affects locomotion in mice and finds that this activity is crucial for normal movement.
  • Dopamine is confirmed to activate PKA in direct pathway neurons, but indirect pathway neurons show an even greater PKA increase influenced by adenosine receptors.
  • The research highlights the interaction between dopamine and adenosine in regulating PKA activity, suggesting that both neuromodulators play a key role in coordinating movement in the striatum.

Article Abstract

The canonical model of striatal function predicts that animal locomotion is associated with the opposing regulation of protein kinase A (PKA) in direct and indirect pathway striatal spiny projection neurons (SPNs) by dopamine. However, the precise dynamics of PKA in dorsolateral SPNs during locomotion remain to be determined. It is also unclear whether other neuromodulators are involved. Here we show that PKA activity in both types of SPNs is essential for normal locomotion. Using two-photon fluorescence lifetime imaging of a PKA sensor through gradient index lenses, we measured PKA activity within individual SPNs of the mouse dorsolateral striatum during locomotion. Consistent with the canonical view, dopamine activated PKA activity in direct pathway SPNs during locomotion through the dopamine D receptor. However, indirect pathway SPNs exhibited a greater increase in PKA activity, which was largely abolished through the blockade of adenosine A receptors. In agreement with these results, fibre photometry measurements of an adenosine sensor revealed an acute increase in extracellular adenosine during locomotion. Functionally, antagonism of dopamine or adenosine receptors resulted in distinct changes in SPN PKA activity, neuronal activity and locomotion. Together, our results suggest that acute adenosine accumulation interplays with dopamine release to orchestrate PKA activity in SPNs and proper striatal function during animal locomotion.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10752255PMC
http://dx.doi.org/10.1038/s41586-022-05407-4DOI Listing

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