Investigations on the 4-Quinolone-3-carboxylic acid motif. 3. Synthesis, structure-affinity relationships, and pharmacological characterization of 6-substituted 4-quinolone-3-carboxamides as highly selective cannabinoid-2 receptor ligands

Pasquini S.; Ligresti A.; Mugnaini C.; Semeraro T.; Cicione L.; De Rosa M.; Guida F.; Luongo L.; De Chiaro M.; Cascio M.G.; Bolognini D.; Marini P.; Pertwee R.; Maione S.; Di Marzo V.; Corelli F.

首页> 外文期刊>Journal of Medicinal Chemistry >Investigations on the 4-Quinolone-3-carboxylic acid motif. 3. Synthesis, structure-affinity relationships, and pharmacological characterization of 6-substituted 4-quinolone-3-carboxamides as highly selective cannabinoid-2 receptor ligands

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Investigations on the 4-Quinolone-3-carboxylic acid motif. 3. Synthesis, structure-affinity relationships, and pharmacological characterization of 6-substituted 4-quinolone-3-carboxamides as highly selective cannabinoid-2 receptor ligands

机译：关于4-喹诺酮-3-羧酸基序的研究。 3. 6-取代的4-喹诺酮-3-羧酰胺作为高选择性大麻素-2受体配体的合成，结构亲和关系和药理学表征

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A set of quinolone-3-carboxamides 2 bearing diverse substituents at position 1, 3, and 6 of the bicyclic nucleus was prepared. Except for six compounds exhibiting K_i > 100 nM, all the quinolone-3-carboxamides 2 proved to be high affinity CB2 ligands, with K_i values ranging from 73.2 to 0.7 nM and selectivity [SI = K_i(CB1)/K_i(CB2)] varying from >14285 to 1.9, with only 2ah exhibiting a reverse selectivity (SI < 1). In the formalin test of peripheral acute and inflammatory pain in mice, 2ae showed analgesic activity that was antagonized by a selective CB2 antagonist. By contrast, 2e was inactive per se and antagonized the effect of a selective CB2 agonist. Finally, 2g and 2p exhibited CB2 inverse agonist-like behavior in this in vivo test. However, two different functional assays carried out in vitro on 2e and 2g indicated for both compounds an overall inverse agonist activity at CB2 receptors.

机译：制备了一组在双环核的1、3和6位带有不同取代基的喹诺酮-3-羧酰胺2。除六种化合物的K_i> 100 nM外，所有喹诺酮-3-羧酰胺2均被证明是高亲和力的CB2配体，其K_i值为73.2至0.7 nM，选择性为[SI = K_i（CB1）/ K_i（CB2）]。从> 14285到1.9，只有2ah表现出反向选择性（SI <1）。在小鼠外周性急性和炎性疼痛的福尔马林测试中，2ae显示出由选择性CB2拮抗剂拮抗的镇痛活性。相比之下，2e本身是无活性的，并且拮抗了选择性CB2激动剂的作用。最后，在该体内测试中，2g和2p表现出CB2反向激动剂样行为。但是，在2e和2g体外进行的两种不同的功能测定表明，这两种化合物对CB2受体的总体反向激动剂活性。

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《Journal of Medicinal Chemistry 》 |2010年第16期| 共14页
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Pasquini S.; Ligresti A.; Mugnaini C.; Semeraro T.; Cicione L.; De Rosa M.; Guida F.; Luongo L.; De Chiaro M.; Cascio M.G.; Bolognini D.; Marini P.; Pertwee R.; Maione S.; Di Marzo V.; Corelli F.;
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1. Investigations on the 4-Quinolone-3-carboxylic acid motif. 3. Synthesis, structure-affinity relationships, and pharmacological characterization of 6-substituted 4-quinolone-3-carboxamides as highly selective cannabinoid-2 receptor ligands [J] . Pasquini S., Ligresti A., Mugnaini C., Journal of Medicinal Chemistry . 2010 ,第16期

机译：关于4-喹诺酮-3-羧酸基序的研究。 3. 6-取代的4-喹诺酮-3-羧酰胺作为高选择性大麻素-2受体配体的合成，结构亲和关系和药理学表征
2. Investigations on the 4-quinolone-3-carboxylic acid motif. 2. Synthesis and structure-activity relationship of potent and selective cannabinoid-2 receptor agonists endowed with analgesic activity in vivo [J] . Pasquini S, Botta L, Scincraro T, Journal of Medicinal Chemistry . 2008 ,第16期

机译：关于4-喹诺酮-3-羧酸基序的研究。 2.具有体内止痛作用的强效和选择性大麻素2受体激动剂的合成及其构效关系
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6. Investigations on the 4-Quinolone-3-Carboxylic Acid Motif. 5. Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach [O] . Dr. Claudia Mugnaini, Stefania Nocerino, Valentina Pedani, -1

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机译：对4-喹诺酮-3-羧酸基序部分5的研究：通过生物等效方法调节一组有效和选择性大麻素-2受体配体的物理化学特征。

Investigations on the 4-Quinolone-3-carboxylic acid motif. 3. Synthesis, structure-affinity relationships, and pharmacological characterization of 6-substituted 4-quinolone-3-carboxamides as highly selective cannabinoid-2 receptor ligands

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