<p>The anterior cingulate cortex is a key brain region involved in the affective and motivational dimensions of pain, but how opioid analgesics modulate this cortical circuit remains unclear<sup><CitationRef CitationID="CR1">1</CitationRef></sup>. Uncovering how opioids alter nociceptive neural dynamics to produce pain relief is essential for developing safer and more targeted treatments for chronic pain. Here we show that a population of cingulate neurons encodes spontaneous pain-related behaviours and is selectively modulated by morphine. Using deep learning behavioural analyses combined with longitudinal neural recordings in mice, we identified a persistent shift in cortical activity patterns following nerve injury that reflects the emergence of an unpleasant, affective chronic pain state. Morphine reversed these neuropathic neural dynamics and reduced affective–motivational behaviours without altering sensory detection or reflexive responses, mirroring how opioids alleviate pain unpleasantness in humans. Leveraging these findings, we built a biologically inspired chemogenetic gene therapy that targets opioid-sensitive neurons in the cingulate using a synthetic μ-opioid receptor promoter to drive inhibition<sup><CitationRef CitationID="CR2">2</CitationRef></sup>. This opioid-mimetic chemogenetic gene therapy recapitulated the analgesic effects of morphine during chronic neuropathic pain, thereby offering a new strategy for precision pain management that targets a key nociceptive cortical opioid circuit with safe, on-demand analgesia.</p>

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Mimicking opioid analgesia in cortical pain circuits

  • Corinna S. Oswell,
  • Sophie A. Rogers,
  • Justin G. James,
  • Nora M. McCall,
  • Alex I. Hsu,
  • Gregory J. Salimando,
  • Malaika Mahmood,
  • Lisa M. Wooldridge,
  • Meghan Wachira,
  • Adrienne Y. Jo,
  • Raquel Adaia Sandoval Ortega,
  • Jessica A. Wojick,
  • Katherine Beattie,
  • Sofia A. Farinas,
  • Samar N. Chehimi,
  • Amrith Rodrigues,
  • Jacqueline W. K. Wu,
  • Lindsay L. Ejoh,
  • Blake A. Kimmey,
  • Emily Lo,
  • Ghalia Azouz,
  • Jose J. Vasquez,
  • Matthew R. Banghart,
  • Kevin T. Beier,
  • Kate Townsend Creasy,
  • Richard C. Crist,
  • Charu Ramakrishnan,
  • Benjamin C. Reiner,
  • Karl Deisseroth,
  • Eric A. Yttri,
  • Gregory Corder

摘要

The anterior cingulate cortex is a key brain region involved in the affective and motivational dimensions of pain, but how opioid analgesics modulate this cortical circuit remains unclear1. Uncovering how opioids alter nociceptive neural dynamics to produce pain relief is essential for developing safer and more targeted treatments for chronic pain. Here we show that a population of cingulate neurons encodes spontaneous pain-related behaviours and is selectively modulated by morphine. Using deep learning behavioural analyses combined with longitudinal neural recordings in mice, we identified a persistent shift in cortical activity patterns following nerve injury that reflects the emergence of an unpleasant, affective chronic pain state. Morphine reversed these neuropathic neural dynamics and reduced affective–motivational behaviours without altering sensory detection or reflexive responses, mirroring how opioids alleviate pain unpleasantness in humans. Leveraging these findings, we built a biologically inspired chemogenetic gene therapy that targets opioid-sensitive neurons in the cingulate using a synthetic μ-opioid receptor promoter to drive inhibition2. This opioid-mimetic chemogenetic gene therapy recapitulated the analgesic effects of morphine during chronic neuropathic pain, thereby offering a new strategy for precision pain management that targets a key nociceptive cortical opioid circuit with safe, on-demand analgesia.