Inhibiting the Breakdown of Endogenous Opioids and Cannabinoids to Alleviate Pain

Inhibiting the Breakdown of Endogenous Opioids and Cannabinoids to Alleviate Pain

REVIEWS Inhibiting the breakdown of endogenous opioids and cannabinoids to alleviate pain Bernard P. Roques1,2, Marie-Claude Fournié-Zaluski1 and Michel Wurm1 Abstract | Chronic pain remains unsatisfactorily treated, and few novel painkillers have reached the market in the past century. Increasing the levels of the main endogenous opioid peptides — enkephalins — by inhibiting their two inactivating ectopeptidases, neprilysin and aminopeptidase N, has analgesic effects in various models of inflammatory and neuropathic pain. Stemming from the same pharmacological concept, fatty acid amide hydrolase (FAAH) inhibitors have also been found to have analgesic effects in pain models by preventing the breakdown of endogenous cannabinoids. Dual enkephalinase inhibitors and FAAH inhibitors are now in early-stage clinical trials. In this Review, we compare the effects of these two potential classes of novel analgesics and describe the progress in their rational design. We also consider the challenges in their clinical development and opportunities for combination therapies. Pain is a unique, conscious experience with sensory- to the market. There is an urgent need for novel treat- Fibromyalgia A disorder of unknown discriminative, cognitive-evaluative and affective- ments for all types of pain, particularly neuropathic pain, 1 aetiology that is characterized emotional components . Transient and acute pain can be that show greater efficacy, better tolerability and wider by widespread pain, abnormal effectively alleviated by activating the endogenous safety margins11. pain processing, sleep opioid system, which has a key role in discriminating One innovative approach12 for the development disturbance, fatigue and between innocuous and noxious sensations2,3. However, of analgesics is based on the fact that the painkillers often psychological distress. chronic pain can occur after several pathophysiological found in Papaver somniferum (morphine) or Cannabis Neuropathic pain processes, as well as without any identifiable cause (such sativa (Δ9‑tetrahydrocannabinol; Δ9‑THC) mimic Pain caused by a lesion as in fibromyalgia)4. One example is neuropathic pain — a endogenous opioids and endogenous cannabinoids, or a disease of the frequent complication of shingles, diabetes, antiviral or respectively. Indeed, exogenous agonists of opioid and somatosensory nervous system. antitumour chemotherapy, as well as surgery or lower- cannabinoid receptors elicit marked analgesic effects back disorders — which is unsatisfactorily treated with but they may excessively stimulate these ubiquitously morphine5,6. distributed receptors, thereby inducing serious side At present, tricyclic antidepressants, the anticonvul- effects such as respiratory depression, sedation, consti- sants gabapentin and pregabalin, and the antidepressant pation, nausea, tolerance and dependence in the case of duloxetine are the only available treatments for neuro- opiates13, or dysphoria, changes in motor coordination pathic pain. However, their efficacy and tolerability are and memory disorders in the case of cannabinoids14. So, often mediocre and it is therefore not surprising that alternative strategies to harness the endogenous opioid more than 100 new chemical entities have been under and cannabinoid systems are desirable. 1Pharmaleads SAS, 11 Rue investigation for the treatment of neuropathic pain in Watt, 75013 Paris, France. recent years. Among these, neurokinin 1 receptor (also Pain reduction by endogenous enkephalins. The main 2Université Paris-Descartes, known as TACR1) antagonists7, sodium channel blockers endogenous opioids endowed with antinociceptive 4 Avenue de l’Observatoire, and NMDA (N-methyl-d-aspartate) receptor antago- properties are Met-enkephalin and Leu-enkephalin. 75006 Paris, France. nists8,9 have failed in clinical trials despite showing signs They are expressed as pre-propeptides (preproenkeph­ Correspondence to B.P.R. e-mail: bernard.roques@ of efficacy in preclinical studies. Other compounds tar- alin (PENK)), which are processed within specific neu- 10 2+ 15 pharmaleads.com geting acid-sensitive channels or vanilloid receptors rons and released by a Ca -dependent mechanism doi:10.1038/nrd3673 are being investigated, but none of them has yet made it to interact specifically with two G protein-coupled 292 | APRIL 2012 | VOLUME 11 www.nature.com/reviews/drugdisc © 2012 Macmillan Publishers Limited. All rights reserved REVIEWS receptors (GPCRs): the μ-opioid receptors (MORs) The synaptic concentrations of AEA are crucially and the δ-opioid receptors (DORs)16. The affinity of dependent on a recently characterized reuptake system enkephalins for MORs is similar to that of morphine, known as FAAH-like anandamide transporter (FLAT)38. whereas their affinity for DORs is about tenfold higher16. The basal release of AEA is very low in the brain and The crucial role of enkephalins in physiological requires a stimulus before neuronal secretion39. When it pain control is supported by the increase in sensitivity is delivered into the brain by intravenous (i.v.) injection, to noxious stimuli elicited by PENK gene ablation17,18. AEA alone does not reduce acute pain but it elicits a Furthermore, when Met-enkephalin is injected into significant antinociceptive response when it is co- the rodent brain, it produces a morphine-like transient administered with a compound that inhibits its catabo- antinociceptive effect19. The limited duration of this lism40. Nevertheless, even after stressful stimulation41, effect is due to the rapid interruption of endogenous endogenous cannabinoid‑mediated analgesia19,42 is never opioidergic signalling by the concomitant action of two as efficacious as the morphine‑like analgesia induced zinc metallopeptidases — the neutral endopeptidase by enkephalins or dual enkephalinase (DENK) inhibi- neprilysin (NEP; also known as CD10) and aminopepti- tors21,30 in acute pain models. By contrast, in a chronic dase N (APN; also known as CD13) — which break pain model in which cannabinoid receptors are perma- down enkephalins to produce the inactive metabolites nently stimulated by protected endo­genous cannabi- Tyr-Gly-Gly and Tyr, respectively20,21 (FIG. 1a). noids, significant analgesic effects were observed43–49. Blocking the enzymatic inactivation of enkephalins increases their basal extracellular levels near the release Harnessing the endogenous opioid and cannabinoid site, so the effect of blocking NEP and APN is limited systems. These results have encouraged the development to local opioid receptors21. The intensity of the response of dual NEP–APN inhibitors (now usually described as therefore depends on: first, the levels of enkepha- DENK inhibitors) and reversible or irreversible FAAH lins released by a given stimulus; second, the levels of inhibitors25,27,30,34,37,42,50. To this end, the structure of the opioid receptors; and third, the activity of inactivating metabolizing enzymes in complex with an inhibitor51–54, enzymes. All three of these factors vary according to their central21,55 and peripheral distribution56,57 as well the neuronal pathways involved and the type of stimu- as their molecular mechanisms of hydrolysis21,37,52,58 have lation21–24. When administered systemically, selective been taken into account. NEP inhibitors have no significant analgesic effects in Interestingly, both endogenous opioids and endog- rodents25 or in humans26 because the level of protected enous cannabinoids are present in primary sensory neu- enkephalins is too low23 and the stimulation of opioid rons57,59–65, offering the possibility to relieve, or at least receptors is therefore insufficient. This finding led to the reduce, the noxious inputs at their initial stage34,49,58–61,66–68. proposal that dual inhibitors targeting both NEP and Indeed, more than 50% of the effects of morphine are APN27 might be more effective, and promising results attributable to the stimulation of peripheral neurons32,69,70. were obtained with some of these compounds in vari- Therefore, the development of DENK inhibitors and ous animal models of pain21,25,27–32. Accordingly, in a non- FAAH inhibitors has focused on the treatment of neuro­ controlled open-label study, intrathecal administration pathic pain and inflammatory pain with compounds of the combination of a selective NEP inhibitor12 and a that are unable to enter the brain (and are thus devoid of nonspecific APN inhibitor elicited marked and lasting possible behavioural adverse effects)30,49,58,63,66,67,71. pain relief in terminally ill patients with cancer who were Results with one of the first synthetic orally active unresponsive to morphine33. DENK inhibitors — PL37 (REF. 72) — in various ani- mal models of pain have revealed interesting analgesic Pain reduction by endogenous cannabinoids. The major effects32,73,74; PL37 is the first DENK inhibitor to reach endogenous substances recognizing the same recep- clinical trials. The first orally active FAAH inhibitor, tors as Δ9‑THC are the endogenous cannabinoids URB597, was developed following a structure–activity N‑arachidonoyl ethanolamide (also known as anandamide study42 and remains the most studied FAAH inhibitor (AEA)) and 2‑arachidonoylglycerol. Like Δ9‑THC, AEA for both its antinociceptive and anxiolytic properties. interacts with two GPCRs, namely cannabinoid recep- The orally active FAAH inhibitor PF‑04457845 was in tor 1 (CB1R) and cannabinoid receptor 2 (CB2R)34. In Phase II development for the treatment of osteoarthritic brain homogenates, the affinity

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