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      Lack of synergistic interaction between the two mechanisms of action of tapentadol in gastrointestinal transit : Lack of constipation synergy by tapentadol

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          Descending control of pain.

          Upon receipt in the dorsal horn (DH) of the spinal cord, nociceptive (pain-signalling) information from the viscera, skin and other organs is subject to extensive processing by a diversity of mechanisms, certain of which enhance, and certain of which inhibit, its transfer to higher centres. In this regard, a network of descending pathways projecting from cerebral structures to the DH plays a complex and crucial role. Specific centrifugal pathways either suppress (descending inhibition) or potentiate (descending facilitation) passage of nociceptive messages to the brain. Engagement of descending inhibition by the opioid analgesic, morphine, fulfils an important role in its pain-relieving properties, while induction of analgesia by the adrenergic agonist, clonidine, reflects actions at alpha(2)-adrenoceptors (alpha(2)-ARs) in the DH normally recruited by descending pathways. However, opioids and adrenergic agents exploit but a tiny fraction of the vast panoply of mechanisms now known to be involved in the induction and/or expression of descending controls. For example, no drug interfering with descending facilitation is currently available for clinical use. The present review focuses on: (1) the organisation of descending pathways and their pathophysiological significance; (2) the role of individual transmitters and specific receptor types in the modulation and expression of mechanisms of descending inhibition and facilitation and (3) the advantages and limitations of established and innovative analgesic strategies which act by manipulation of descending controls. Knowledge of descending pathways has increased exponentially in recent years, so this is an opportune moment to survey their operation and therapeutic relevance to the improved management of pain.
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            Unmasking the tonic-aversive state in neuropathic pain.

            Tonic pain has been difficult to demonstrate in animals. Because relief of pain is rewarding, analgesic agents that are not rewarding in the absence of pain should become rewarding only when there is ongoing pain. We used conditioned place preference to concomitantly determine the presence of tonic pain in rats and the efficacy of agents that relieve it. This provides a new approach for investigating tonic pain in animals and for evaluating the analgesic effects of drugs.
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              An overview of drug combination analysis with isobolograms.

              Drugs given in combination may produce effects that are greater than or less than the effect predicted from their individual potencies. The historical basis for predicting the effect of a combination is based on the concept of dose equivalence; i.e., an equally effective dose (a) of one will add to the dose (b) of the other in the combination situation. For drugs with a constant relative potency, this leads to linear additive isoboles (a-b curves of constant effect), whereas a varying potency ratio produces nonlinear additive isoboles. Determination of the additive isobole is a necessary procedure for assessing both synergistic and antagonistic interactions of the combination. This review discusses both variable and constant relative potency situations and provides the mathematical formulas needed to distinguish these cases.
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                Author and article information

                Journal
                European Journal of Pain
                EJP
                Wiley
                10903801
                September 2014
                September 2014
                February 26 2014
                : 18
                : 8
                : 1148-1156
                Affiliations
                [1 ]Department of Pharmacology; Temple University School of Medicine and Center for Substance Abuse Research; Philadelphia USA
                [2 ]Department of Pharmaceutical Sciences; Temple University School of Pharmacy; Philadelphia USA
                [3 ]Pain Pharmacology; Grünenthal GmbH; Aachen Germany
                [4 ]Translational Sciences; Grünenthal GmbH; Aachen Germany
                Article
                10.1002/j.1532-2149.2014.00461.x
                c05204ee-17d7-484a-97f5-ffa32f3fcdd3
                © 2014

                http://doi.wiley.com/10.1002/tdm_license_1.1

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