Spinal Opioid Bioavailability in Postoperative Pain

Bujedo, Borja Mugabure

doi:10.1111/papr.12099

Cited by 54 publications

(49 citation statements)

References 88 publications

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“…Increased water solubility is responsible for slow onset of effect and long duration of action. Potency of spinal opioids increases with increasing hydrophobicity [9].…”

Section: The Pharmacokinetics Of Spinal Opioidsmentioning

confidence: 98%

Which Epidural Opioid is More Suitable for Postoperative Pain Management?

2017

JACCOA

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Opioids have always been considered the best option in clinical practice for the treatment of severe postoperative pain. However, the spinal administration of an opioid drug does not always guarantee selective action and segmental analgesia in the spine. This fact is due to partial reuptake to blood systemic circulation reaching brain receptors. Recent evidence from clinical studies indicates that bioavailability in the spinal cord biophase is negatively correlated with liposolubility, which is higher for hydrophilic opioids, than for lipophilic ones. Actually, clinical guidelines recommend using a mixture of local anesthetic plus a strong opioid to improve the global analgesic effect, minimize adverse effects and improve the overall patient´s satisfaction. Moreover, an opioid alone like morphine can be administered to provide a long period of postoperative analgesia for 24h, or even 48 h when an extended release epidural formulation is used. In this narrative review, practical information for correct spinal opioid selection is provided to help the physicians a better choice for postoperative epidural analgesia.

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“…Increased water solubility is responsible for slow onset of effect and long duration of action. Potency of spinal opioids increases with increasing hydrophobicity [9].…”

Section: The Pharmacokinetics Of Spinal Opioidsmentioning

confidence: 98%

Which Epidural Opioid is More Suitable for Postoperative Pain Management?

2017

JACCOA

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“…Intrathecal Morphine (ITM) is widely used for the treatment of pain after CD [3] [8]. After administration, it has a slow onset of action and long duration of action (12 to 48 h) [9]. In particular, ITM leads to significant cost savings for the first 24 hours when compared with intravenous opioid patient-controlled analgesia [10].…”

Section: Introductionmentioning

confidence: 99%

Three Different Doses of Intrathecal Morphine as Part of a Multimodal Regimen for Post-Cesarean Delivery Analgesia: A Randomized Double-Blinded Trial

Benevides¹,

Nochi²,

Solcia³

et al. 2018

OJOG

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Brazil is one of the countries that carry out cesarean delivery in the world. The pain after cesarean delivery (CD) is one of the main concerns of parturient. Intrathecal Morphine (ITM) is widely used for the treatment of pain after CD; however, the optimal dose with minimal side effects is to be established. Objectives: To compare the analgesia and side effects resulted by three different doses of ITM as part of a multimodal regimen for postcesarean delivery analgesia. Methods: One hundred ninety-four patients were sampled in this randomized, double-blinded, three-arm study (group 0.075: ITM 0.75 mg; group 0.1: ITM 0.1 mg and group 0.15: ITM 0.15 mg). All patients received intravenous dexamethasone, dipyrone and ketoprofen. The primary endpoint was pain intensity measured at rest and on movement, while the secondary endpoint was overall satisfaction with pain relief, the incidence of nausea and vomiting, intensity of pruritus, and the use of additional tramadol, antipruritic and antiemetic use within 24 hours after postoperation. Results: The three groups showed similar pain intensity at rest and on movement. The pain intensity on movement was significantly higher than at rest in the groups (p < 0.001). There were no significant differences among the groups regarding secondary endpoint. Conclusions: Our findings suggest that in cases of an elective CD, 0.075 mg of ITM produces postoperative analgesia of similar quality that provided by 0.1 or 0.15 mg ITM. The patients should have a multimodal analgesia approach that includes: ITM, anti-inflammatory agents and access to additional systemic analgesic if necessary.

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“…In fact, the U.S. Food and Drugs Administration (FDA) has so far only approved hydrophilic opioids (morphine, hydromorphone) as fi rst-line drugs for spinal use. Other opioids are recommended only if these drugs are not well tolerated or effective, though pain physicians used them on an off-label basis for either postoperative or chronic pain, given the multiple studies indicating that these opioids can be useful [28]. * Into brackets opioid liposolubility in relation to morphine, expressed as octanol/ buffer distribution coeffi cient.…”

Section: Spinal Diffusionmentioning

confidence: 99%

Physiology of Spinal Opioids and its relevance for Pain Management Selection

Bujedo¹

2017

Open J Pain Med

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Spinal Opioid Bioavailability in Postoperative Pain

Cited by 54 publications

References 88 publications

Which Epidural Opioid is More Suitable for Postoperative Pain Management?

Which Epidural Opioid is More Suitable for Postoperative Pain Management?

Three Different Doses of Intrathecal Morphine as Part of a Multimodal Regimen for Post-Cesarean Delivery Analgesia: A Randomized Double-Blinded Trial

Physiology of Spinal Opioids and its relevance for Pain Management Selection

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