2013
DOI: 10.3389/fphar.2013.00132
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Targeting peripheral opioid receptors to promote analgesic and anti-inflammatory actions

Abstract: Mechanisms of endogenous pain control are significant. Increasing studies have clearly produced evidence for the clinical usefulness of opioids in peripheral analgesia. The immune system uses mechanisms of cell migration not only to fight pathogens but also to control pain and inflammation within injured tissue. It has been demonstrated that peripheral inflammatory pain can be effectively controlled by an interaction of immune cell-derived opioid peptides with opioid receptors on peripheral sensory nerve termi… Show more

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Cited by 85 publications
(85 citation statements)
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“…Nociceptive stimuli are conducted by different sensitive fibers to the dorsal horn of the spinal medulla and opioids modulate the nociceptive response and cause antinociceptive effect (TRUONG et al, 2003). As observed, crotalphine promoted more analgesia on inflamed tissue and this findingis supported by previous studies which revealed that expression and distribution of receptors in damaged tissue change the potency of opioids ( VAN LOON et al, 2013); there is also activation of peripheral opioid receptors depending on the stage of the inflammatory reaction and opioids do not always act the same way on intact tissue because they induce release of IL-10, which has anti-inflammatory effect (JOHNSTON et al, 2004;IWASZKIEWICZ, 2013) and increase plasmatic level of glucocorticoids by stimulation of the hypothalamicpituitary-adrenal axis (CHISARI et al, 1998). Besides, crotalphine was more efficient in the ischial region because mu receptors are distributed along the spinal medulla in horses, while kappa and delta receptors are restricted to the lumbosacral and cervical segments, respectively (VALADÃO et al, 2002).…”
Section: -----------------------Gc-----------------------------------supporting
confidence: 70%
“…Nociceptive stimuli are conducted by different sensitive fibers to the dorsal horn of the spinal medulla and opioids modulate the nociceptive response and cause antinociceptive effect (TRUONG et al, 2003). As observed, crotalphine promoted more analgesia on inflamed tissue and this findingis supported by previous studies which revealed that expression and distribution of receptors in damaged tissue change the potency of opioids ( VAN LOON et al, 2013); there is also activation of peripheral opioid receptors depending on the stage of the inflammatory reaction and opioids do not always act the same way on intact tissue because they induce release of IL-10, which has anti-inflammatory effect (JOHNSTON et al, 2004;IWASZKIEWICZ, 2013) and increase plasmatic level of glucocorticoids by stimulation of the hypothalamicpituitary-adrenal axis (CHISARI et al, 1998). Besides, crotalphine was more efficient in the ischial region because mu receptors are distributed along the spinal medulla in horses, while kappa and delta receptors are restricted to the lumbosacral and cervical segments, respectively (VALADÃO et al, 2002).…”
Section: -----------------------Gc-----------------------------------supporting
confidence: 70%
“…Peripheral tissue injury causes the migration of immune cells to the injured site (27). These cells express opioid peptides, such as b-endorphin, Met-Enk, and dynorphin A, together with corticotropin-releasing factor (CRF) receptor.…”
Section: Comparison Of Nic Effects Associated With or Without Endogenmentioning
confidence: 99%
“…The opioid receptors are also expressed on immune cells, suggesting that opioids have a direct effect on immune function in host defence and immunity (211). A substantial body of literature evidence over the past decades has shown that the immune-derived opioid peptides produce significant inhibition of inflammatory pain upon their interaction with opioid receptors expressed on the terminals of peripheral sensory neurons in inflamed tissue (10,11,78,142).…”
Section: Discussionmentioning
confidence: 99%
“…Several underlying mechanisms of opioidmediated peripheral analgesia have been shown including alteration in calcium influx, inhibition of calcitonin gene related peptide (CGRP) and cyclic adenosine monophosphate (cAMP) as well as activation of transient receptor potential vanilloid 1 (TRPV1) (13). Likewise, modification of inflammatory cascades has also been observed, thereby expanding the perspective that peripherally active endogenous opioids are not only restricted to analgesia but also possess on immunomodulatory component which is therapeutically beneficial in inflammation-induced pain (4,11). (34,35).…”
Section: Study Backgroundmentioning
confidence: 99%
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