Comment; So now we’ve found naturally occuring “brakes” to the µ mu receptor which causes analgesia & euphoria and being naturally occuring in our brains. What can we do with this?
- Dandan Wang1,
- Hannah M. Stoveken1,
- Stefano Zucca1,
- Maria Dao1,
- Cesare Orlandi1,
- Chenghui Song1,*,
- Ikuo Masuho1,
- Caitlin Johnston1,
- Karla J. Opperman1,
- Andrew C. Giles1,
- Matthew S. Gill2,
- Erik A. Lundquist3,
- Brock Grill1,†,
- Kirill A. Martemyanov1,†
See all authors and affiliations
Science 15 Aug 2019:
Abstract
Opioids target the μ-opioid receptor (MOR) to produce unrivaled pain management but their addictive properties can lead to severe abuse. We developed a whole animal behavioral platform for unbiased discovery of genes influencing opioid responsiveness. Using forward genetics in C. elegans, we identified a conserved orphan receptor, GPR139, with anti-opioid activity. GPR139 is coexpressed with MOR in opioid-sensitive brain circuits, binds to MOR and inhibits signaling to G proteins. Deletion of GPR139 in mice enhanced opioid-induced inhibition of neuronal firing to modulate morphine-induced analgesia, reward, and withdrawal. Thus, GPR139 could be a useful target for increasing opioid safety. These results also demonstrate the potential of C. elegans as a scalable platform for genetic discovery of GPCR signaling principles.
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