Literature DB >> 15327807

The functional expression of mu opioid receptors on sensory neurons is developmentally regulated; morphine analgesia is less selective in the neonate.

Reema Nandi1, Daniel Beacham, Jacqueta Middleton, Martin Koltzenburg, Richard F Howard, Maria Fitzgerald.   

Abstract

Opioid requirements in neonatal patients are reported to be lower than older infants and this may be a reflection of the developmental regulation of opioid receptors. In this study we have investigated the postnatal regulation of Mu opioid receptor (MOR) function in both rat lumbar dorsal root ganglion (DRG) cultures and behavioural mechanical and thermal reflex tests in rat pups. Immunostaining with MOR and selective neurofilament (NF200) antibodies was combined with calcium imaging of MOR function in cultured neonatal and adult rat dorsal root ganglion cells. Calcium imaging showed that a significantly greater number of neonatal DRG neurons expressed functional MOR compared to adult (56.5+/-3.4 versus 39.9+/-1.5%, n=8, mean+/-SEM, P<0.001). This expression is confined to the large, neurofilament positive sensory neurons, while expression in small, nociceptive, neurofilament negative neurons remains unchanged. Sensory threshold testing in rat pups showed that the analgesic potency of systemic morphine to mechanical stimulation is significantly greater in the neonate and declines with postnatal age. Morphine analgesic potency in thermal nociceptive tests did not change with postnatal age. These experiments show that the MOR expressed on large DRG neurons in neonates are functional and are subject to postnatal developmental regulation. This changing functional receptor profile is consistent with greater morphine potency in mechanical, but not thermal, sensory tests in young animals. These results have important clinical implications for the use of morphine in neonates and provide a possible explanation for the differences in morphine requirements observed in the youngest patients.

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Year:  2004        PMID: 15327807     DOI: 10.1016/j.pain.2004.05.025

Source DB:  PubMed          Journal:  Pain        ISSN: 0304-3959            Impact factor:   6.961


  22 in total

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Review 2.  Understanding developmental pharmacodynamics: importance for drug development and clinical practice.

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3.  Tolerance, opioid-induced allodynia and withdrawal associated allodynia in infant and young rats.

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4.  Intrathecal clonidine in the neonatal rat: dose-dependent analgesia and evaluation of spinal apoptosis and toxicity.

Authors:  Suellen M Walker; Marjorie Grafe; Tony L Yaksh
Journal:  Anesth Analg       Date:  2012-03-30       Impact factor: 5.108

5.  Preemptive morphine analgesia attenuates the long-term consequences of neonatal inflammation in male and female rats.

Authors:  Jamie L Laprairie; Malcolm E Johns; Anne Z Murphy
Journal:  Pediatr Res       Date:  2008-12       Impact factor: 3.756

6.  Gi- and Gq-coupled ADP (P2Y) receptors act in opposition to modulate nociceptive signaling and inflammatory pain behavior.

Authors:  Sacha A Malin; Derek C Molliver
Journal:  Mol Pain       Date:  2010-04-15       Impact factor: 3.395

7.  Pharmacologic management of chronic pain.

Authors:  Hue Jung Park; Dong Eon Moon
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8.  Long-term behavioral effects in a rat model of prolonged postnatal morphine exposure.

Authors:  Michael M Craig; Dusica Bajic
Journal:  Behav Neurosci       Date:  2015-07-27       Impact factor: 1.912

Review 9.  Infant pain management: a developmental neurobiological approach.

Authors:  Maria Fitzgerald; Suellen M Walker
Journal:  Nat Clin Pract Neurol       Date:  2009-01

10.  A functional link between T-type calcium channels and mu-opioid receptor expression in adult primary sensory neurons.

Authors:  Zi-Zhen Wu; You-Qing Cai; Hui-Lin Pan
Journal:  J Neurochem       Date:  2009-02-24       Impact factor: 5.372

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