Publication:
Targeting immune-driven opioid analgesia by sigma-1 receptors: Opening the door to novel perspectives for the analgesic use of sigma-1 antagonists.

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Date

2018-02-15

Authors

Tejada, Miguel A
Montilla-Garcia, Angeles
Gonzalez-Cano, Rafael
Bravo-Caparros, Inmaculada
Ruiz-Cantero, M Carmen
Nieto, Francisco R
Cobos, Enrique J

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Elsevier Ltd
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Abstract

Immune cells have a known role in pronociception, since they release a myriad of inflammatory algogens which interact with neurons to facilitate pain signaling. However, these cells also produce endogenous opioid peptides with analgesic potential. The sigma-1 receptor is a ligand-operated chaperone that modulates neurotransmission by interacting with multiple protein partners, including the μ-opioid receptor. We recently found that sigma-1 antagonists are able to induce opioid analgesia by enhancing the action of endogenous opioid peptides of immune origin during inflammation. This opioid analgesia is seen only at the inflamed site, where immune cells naturally accumulate. In this article we review the difficulties of targeting the opioid system for selective pain relief, and discuss the dual role of immune cells in pain and analgesia. Our discussion creates perspectives for possible novel therapeutic uses of sigma-1 antagonists as agents able to maximize the analgesic potential of the immune system.

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MeSH Terms

Analgesia
Analgesics, Opioid
Animals
Humans
Inflammation
Molecular Targeted Therapy
Pain
Receptors, sigma

DeCS Terms

Analgesia
Analgésicos opioides
Animales
Humanos
Inflamación
Pan
Receptores sigma
Terapia molecular dirigida

CIE Terms

Keywords

Analgesia, Endogenous opioid peptides, Immune cells, Neuro-immune interactions, Sigma-1 receptors

Citation

Tejada MÁ, Montilla-García Á, González-Cano R, Bravo-Caparrós I, Ruiz-Cantero MC, Nieto FR, et al. argeting immune-driven opioid analgesia by sigma-1 receptors: Opening the door to novel perspectives for the analgesic use of sigma-1 antagonists. Pharmacol Res. 2018 May;131:224-230.