Spirocyclic Delta Opioid Receptor Agonists for the Treatment of Pain: Discovery of <i>N</i>,<i>N</i>-Diethyl-3-hydroxy-4-(spiro[chromene-2,4′-piperidine]-4-yl) Benzamide (ADL5747)

Bourdonnec, Bertrand Le; Windh, Rolf T.; Leister, Lara K.; Zhou, Qun; Ajello, Christopher W.; Gu, Minghua; Chu, Guowei; Tuthill, Paul A.; Barker, William M.; Koblish, Michael; Wiant, Daniel D.; Graczyk, Thomas M.; Belanger, Serge; Cassel, Joel; Feschenko, Marina S.; Brogdon, Bernice L.; Smith, Steven A.; Derelanko, Michael J.; Kutz, Steve; Little, Patrick; DeHaven, Robert N.; DeHaven‐Hudkins, Diane L.; Dolle, Roland E.

doi:10.1021/jm900773n

Cited by 83 publications

(48 citation statements)

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“…Analgesia produced by ADL5747 and ADL5859 in the mouse differed somehow from analgesia obtained in the rat study (Le Bourdonnec et al, 2009). First, the reduction of inflammatory pain in CFA mice seemed weaker compared with antiallodynia observed in the rat (3-to 10-fold higher doses required for an analgesic effect).…”

Section: Discussionmentioning

confidence: 67%

“…SNC80 is well known to increase locomotor activity in rats and mice (Jutkiewicz et al, 2005;Scherrer et al, 2006;Ito et al, 2008;Pradhan et al, 2010), whereas ADL compounds did not induce hyperlocomotion in rats (Le Bourdonnec et al, 2008Bourdonnec et al, , 2009). Therefore, we investigated the locomotor effects of ADL compounds in naive WT mice.…”

Section: Adl5747 and Adl5859 Produce Dose-dependent Analgesia In Bothmentioning

confidence: 98%

“…The novel nonpeptidic compounds N,N-diethyl-4-(5-hydroxyspiro[chromene-2,4Ј-piperidine]-4-yl)benzamide (ADL5859) (Le Bourdonnec et al, 2008) and N,N-diethyl-3-hydroxy-4-(spiro[chromene-2,4Ј-piperidine]-4-yl)benzamide (ADL5747) (Le Bourdonnec et al, 2009) were developed with structures distinct from other ␦-agonist classes to obtain molecules with higher selectivity for ␦ receptors (Fig. 1).…”

Section: Introductionmentioning

confidence: 99%

“…1). They showed ␦-opioid selectivity based on nanomolar affinities and signaling potencies for the receptor in vitro, with no detectable binding at more than 100 nonopioid receptors, channels, or enzymes (Le Bourdonnec et al, 2008Bourdonnec et al, , 2009. In rats, the two drugs display good oral bioavailability and produce antidepressant (ADL5859) and antihyperalgesic effects in a model of inflammatory pain (Le Bourdonnec et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

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δ-Opioid Mechanisms for ADL5747 and ADL5859 Effects in Mice: Analgesia, Locomotion, and Receptor Internalization

Nozaki

Bourdonnec

Reiss

et al. 2012

J Pharmacol Exp Ther

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N,N-diethyl-4-(5-hydroxyspiro[chromene-2,4Ј-piperidine]-4-yl) benzamide (ADL5859) and N,N-diethyl-3-hydroxy-4-(spiro-[chromene-2,4Ј-piperidine]-4-yl)benzamide (ADL5747) are novel ␦-opioid agonists that show good oral bioavailability and analgesic and antidepressive effects in the rat and represent potential drugs for chronic pain treatment. Here, we used genetic approaches to investigate molecular mechanisms underlying their analgesic effects in the mouse. We tested analgesic effects of ADL5859 and ADL5747 in mice by using mechanical sensitivity measures in both complete Freund's adjuvant and sciatic nerve ligation pain models. We examined their analgesic effects in ␦-opioid receptor constitutive knockout (KO) mice and mice with a conditional deletion of ␦-receptor in peripheral voltage-gated sodium channel (Nav)1.8-expressing neurons (cKO mice). Both ADL5859 and ADL5747, and the prototypical ␦ agonist 4-[(R)-[(2S,5R)-4-allyl-2,5-dimethyl-piperazin-1-yl]-(3-methoxyphenyl)methyl]-N,Ndiethyl-benzamide (SNC80) as a control, significantly reduced inflammatory and neuropathic pain. The antiallodynic effects of all three ␦-opioid agonists were abolished in constitutive ␦-receptor KO mice and strongly diminished in ␦-receptor cKO mice. We also measured two other well described effects of ␦ agonists, increase in locomotor activity and agonist-induced receptor internalization by using knock-in mice expressing enhanced green fluorescence protein-tagged ␦ receptors. In contrast to SNC80, ADL5859 and ADL5747 did not induce either hyperlocomotion or receptor internalization in vivo. In conclusion, both ADL5859 and ADL5747 showed efficient pain-reducing properties in the two models of chronic pain. Their effects were mediated by ␦-opioid receptors, with a main contribution of receptors expressed on peripheral Nav1.8-positive neurons. The lack of in vivo receptor internalization and locomotor activation, typically induced by SNC80, suggests agonist-biased activity at the receptor for the two drugs.

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Section: Discussionmentioning

confidence: 67%

Section: Adl5747 and Adl5859 Produce Dose-dependent Analgesia In Bothmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

δ-Opioid Mechanisms for ADL5747 and ADL5859 Effects in Mice: Analgesia, Locomotion, and Receptor Internalization

Nozaki

Bourdonnec

Reiss

et al. 2012

J Pharmacol Exp Ther

Self Cite

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show abstract

“…At the same time, they may also underlie the proconvulsant effects of exogenous DOPr agonists (Broom et Importantly, the potential to generate seizures is not the same for all DOPr agonists. This potential is associated with SNC80 (Broom et al, 2002;Jutkiewicz et al, 2005Jutkiewicz et al, , 2006, BW373U86 (Jutkiewicz et al, 2006), and deltorphin II (De Sarro et al, 1992;Di Giannuario et al, 2001) but not by KNT-127 (Saitoh et al, 2011), ADL5859 (Le Bourdonnec et al, 2008), or ADL5747 (Le Bourdonnec et al, 2009). ADL compounds that were devoid of proconvulsive actions in preclinical models have also been tested for acute (ClinicalTrials.gov identifier NCT00993863) and chronic (ClinicalTrials.…”

Section: D-opioid Receptors and Activation Of G Protein-coupled Inmentioning

confidence: 99%