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Modulation of mechanosensation by endogenous dopaminergic signaling in the lateral parabrachial nucleus in mice.

Ho KooJigong WangRamesh PariyarRegan M HammondJun-Ho La
Published in: Pain reports (2024)
These results suggest that endogenous dopaminergic signaling occurs in the LPBN upon noxious mechanical stimulation, inhibiting mechanosensitivity through D1-like receptors while enhancing it through D2-like receptors. D2-like receptor signaling in the LPBN may contribute to an injury-induced increase in mechanical nociception, indicating that inhibiting the receptor within the LPBN could offer potential as a novel analgesic strategy.
Keyphrases
  • signaling pathway
  • high glucose
  • neuropathic pain
  • drug induced
  • risk assessment
  • adipose tissue
  • spinal cord injury
  • human health
  • metabolic syndrome
  • endothelial cells