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Unidirectional cross-activation of GRPR by MOR1D uncouples itch and analgesia induced by opioids.


ABSTRACT: Spinal opioid-induced itch, a prevalent side effect of pain management, has been proposed to result from pain inhibition. We now report that the ?-opioid receptor (MOR) isoform MOR1D is essential for morphine-induced scratching (MIS), whereas the isoform MOR1 is required only for morphine-induced analgesia (MIA). MOR1D heterodimerizes with gastrin-releasing peptide receptor (GRPR) in the spinal cord, relaying itch information. We show that morphine triggers internalization of both GRPR and MOR1D, whereas GRP specifically triggers GRPR internalization and morphine-independent scratching. Providing potential insight into opioid-induced itch prevention, we demonstrate that molecular and pharmacologic inhibition of PLC?3 and IP3R3, downstream effectors of GRPR, specifically block MIS but not MIA. In addition, blocking MOR1D-GRPR association attenuates MIS but not MIA. Together, these data suggest that opioid-induced itch is an active process concomitant with but independent of opioid analgesia, occurring via the unidirectional cross-activation of GRPR signaling by MOR1D heterodimerization.

SUBMITTER: Liu XY 

PROVIDER: S-EPMC3197217 | biostudies-literature | 2011 Oct

REPOSITORIES: biostudies-literature

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Unidirectional cross-activation of GRPR by MOR1D uncouples itch and analgesia induced by opioids.

Liu Xian-Yu XY   Liu Zhong-Chun ZC   Sun Yan-Gang YG   Ross Michael M   Kim Seungil S   Tsai Feng-Fang FF   Li Qi-Fang QF   Jeffry Joseph J   Kim Ji-Young JY   Loh Horace H HH   Chen Zhou-Feng ZF  

Cell 20111001 2


Spinal opioid-induced itch, a prevalent side effect of pain management, has been proposed to result from pain inhibition. We now report that the μ-opioid receptor (MOR) isoform MOR1D is essential for morphine-induced scratching (MIS), whereas the isoform MOR1 is required only for morphine-induced analgesia (MIA). MOR1D heterodimerizes with gastrin-releasing peptide receptor (GRPR) in the spinal cord, relaying itch information. We show that morphine triggers internalization of both GRPR and MOR1D  ...[more]

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