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Dissociation of the Opioid Receptor Mechanisms that Control Mechanical and Heat Pain
Author(s) -
Grégory Scherrer,
Noritaka Imamachi,
Yuqing Cao,
Candice Contet,
Françoise Mennicken,
Dajan O’Donnell,
Brigitte L. Kieffer,
Allan I. Basbaum
Publication year - 2009
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2009.04.019
Subject(s) - receptor , substance p , trpv1 , μ opioid receptor , neuroscience , biology , nociceptor , inhibitory postsynaptic potential , afferent , opioid , opioid receptor , δ opioid receptor , microbiology and biotechnology , nociception , neuropeptide , transient receptor potential channel , biochemistry
Delta and mu opioid receptors (DORs and MORs) are inhibitory G protein-coupled receptors that reportedly cooperatively regulate the transmission of pain messages by substance P and TRPV1-expressing pain fibers. Using a DOReGFP reporter mouse we now show that the DOR and MOR are, in fact, expressed by different subsets of primary afferents. The MOR is expressed in peptidergic pain fibers, the DOR in myelinated and nonpeptidergic afferents. Contrary to the prevailing view, we demonstrate that the DOR is trafficked to the cell surface under resting conditions, independently of substance P, and internalized following activation by DOR agonists. Finally, we show that the segregated DOR and MOR distribution is paralleled by a remarkably selective functional contribution of the two receptors to the control of mechanical and heat pain, respectively. These results demonstrate that behaviorally relevant pain modalities can be selectively regulated through the targeting of distinct subsets of primary afferent pain fibers.

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