Current Knowledge of Buprenorphine and Its Unique Pharmacological Profile

Pergolizzi, Joseph V.; Aloisi, Anna Maria; Dahan, Albert; Filitz, Joerg; Langford, R. M.; Likar, Rudolf; Mercadante, Sebastiano; Morlion, Bart; Raffa, Robert B.; Sabatowski, Rainer; Sacerdote, Paola; Torres, L.M.; Weinbroum, Avi A.

doi:10.1111/j.1533-2500.2010.00378.x

Cited by 251 publications

(222 citation statements)

References 99 publications

(279 reference statements)

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“…Buprenorphine is well known as a MOP partial agonist that has been used for both pain management and opioid abuse/addiction and it has less rewarding property compared to other MOP agonists in primates. 51,93 When a NOP agonist (either Ro 64-6198 or SCH 221510) is combined with systemic buprenorphine, the NOP agonist dose-dependently potentiated buprenorphine-induced analgesia. 52 It is worth noting that NOP antagonists potentiated the antinociceptive effects of buprenorphine in rodents, indicating that buprenorphine's own NOP agonist activity attenuated its own MOP agonist activity.…”

Section: ■ Effects Of Systemic Nop-related Ligandsmentioning

confidence: 99%

The Therapeutic Potential of Nociceptin/Orphanin FQ Receptor Agonists as Analgesics without Abuse Liability

Lin

2012

ACS Chem. Neurosci.

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Although mu opioid (MOP) receptor agonists are the most commonly used analgesics for the treatment of moderate to severe pain in the clinic, the side effects of MOP agonists such as abuse liability limit their value as a medication. Research to identify novel analgesics without adverse effects is pivotal to advance the health care of humans. The nociceptin/ orphanin FQ peptide (NOP) receptor, the fourth opioid receptor subtype, mediates distinctive actions in nonhuman primates which suggests the possibility that activity at this receptor may result in strong analgesia in the absence of virtually all of the side effects associated with MOP agonists. The present review highlights the recent progress of pharmacological studies of NOP-related ligands in primates. Selective NOP agonists, either peptidic or nonpeptidic, produce full analgesia in various assays in primates, when delivered systemically or intrathecally. Yet small molecule NOP agonists do not serve as reinforcers, indicating a lack of abuse liability. Given that NOP agonists have low abuse liability and that coactivation of NOP and MOP receptors produces synergistic antinociception, it is worth developing bifunctional NOP/MOP ligands. The outcomes of these studies and recent developments provide new perspectives to establish a translational bridge for understanding the biobehavioral functions of NOP receptors in primates and for facilitating the development of NOP-related ligands as a new generation of analgesics without abuse liability in humans.

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Section: ■ Effects Of Systemic Nop-related Ligandsmentioning

confidence: 99%

The Therapeutic Potential of Nociceptin/Orphanin FQ Receptor Agonists as Analgesics without Abuse Liability

Lin

2012

ACS Chem. Neurosci.

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“…The risk of inducing chronic hyperalgesia seems to vary with the opiate used, and is assumed to be highest for remifentanil (van Gulik et al, 2012), while the partial μ receptor agonist and κ receptor antagonist, buprenorphine has even been associated with an antihyperalgesic effect (Pergolizzi et al, 2010). OIH is prevented by the administration of the NMDA receptor antagonist, ketamine (Laulin et al, 2002).…”

Section: Perioperative Opiatesmentioning

confidence: 99%

Epigenetics in the perioperative period

Lirk

Fiegl

Weber

et al. 2015

British J Pharmacology

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The perioperative period is characterized by profound changes in the body's homoeostatic processes. This review seeks to address whether epigenetic mechanisms may influence an individual's reaction to surgery and anaesthesia. Evidence from animal and human studies suggests that epigenetic mechanisms can explain many facets of susceptibility to acute and chronic pain, making them potential therapeutic targets. Modern pain management is still based upon opiates, and both the developmental expression of opioid receptors and opioid-induced hyperalgesia have been linked to epigenetic mechanisms. In general, opiates seem to increase global DNA methylation levels. This is in contrast to local anaesthetics, which have been ascribed a global demethylating effect. Even though no direct investigations have been carried out, the potential influence of epigenetics on the inflammatory response that follows surgery seems a promising area for research. There is a considerable body of evidence that supports the involvement of epigenetics in the complex process of wound healing. Epigenetics is an important emerging research topic in perioperative medicine, with a huge potential to positively influence patient outcome. LINKED ARTICLESThis article is part of a themed section on Epigenetics and Therapy. To view the other articles in this section visit http://dx

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“…Buprenorphine is the most commonly used analgesic in laboratory rodents 33 and the drug of choice for analgesia in this model but the impact on inflammatory response is unknown. Buprenorphine is a semi-synthetic opioid and has been found to function as a full m-agonist for analgesia 34 and its analgesic potency has been found to be 25-40 times that of morphine in mice when administered parenterally. 35 Most research on opioids and their effect on the inflammatory response concern morphine and heroin and describe increased production of pro-inflammatory cytokines.…”

mentioning

confidence: 99%

Buprenorphine does not impact the inflammatory response in haemophilia A mice with experimentally-induced haemarthrosis

et al. 2014

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Haemarthrosis is the most common clinical manifestation of haemophilia and is responsible for significant morbidity in haemophilic patients. The murine experimentally-induced knee bleeding model is an important model in haemophilia research but it is currently unknown if the use of analgesia in this model might impact on the inflammatory response. The aim was to investigate the inflammatory response after a needle induced knee bleed in haemophilia A mice treated with buprenorphine or saline. One hundred and sixty mice were randomized into two groups to blindly receive buprenorphine or saline. All the mice were anaesthetized and knee injury was induced by inserting a 30 G needle into the right knee joint. At t ¼ 6, 24, 48 and 72 h, 20 mice from each group were terminated and the following parameters were assessed: change in body weight and joint diameter, visual bleeding score (VBS), white blood counts, haematocrit, platelet concentrations, haemoglobin, plasma haptoglobin and plasma and synovial fluid levels of 23 cytokines. Twenty mice were terminated at t ¼ 0 receiving no injury or treatment to provide baseline measures. Twenty-one cytokines in plasma and 22 cytokines in synovial fluid, joint diameter change, VBS and blood parameters were not significantly altered by the administration of buprenorphine. Slight alterations of plasma haptoglobin at t ¼ 48 h, body weight, plasma and synovial eotaxin and plasma G-CSF were found in buprenorphine-treated mice. We demonstrated that buprenorphine does not overall impact on the inflammatory response, and the use of buprenorphine in the knee bleeding model in haemophilic mice should be continued.

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Current Knowledge of Buprenorphine and Its Unique Pharmacological Profile

Cited by 251 publications

References 99 publications

The Therapeutic Potential of Nociceptin/Orphanin FQ Receptor Agonists as Analgesics without Abuse Liability

The Therapeutic Potential of Nociceptin/Orphanin FQ Receptor Agonists as Analgesics without Abuse Liability

Epigenetics in the perioperative period

Buprenorphine does not impact the inflammatory response in haemophilia A mice with experimentally-induced haemarthrosis

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