The agonist activities of the putative antipsychotic agents, L‐745,870 and U‐101958 in HEK293 cells expressing the human dopamine D<sub>4.4</sub> receptor

Gazi, Lucien; Bobirnac, Ionel; Danzeisen, M; Schüpbach, E.; Bruinvels, Anne T.; Geisse, Sabine; Sommer, Bernd; Hoyer, Daniel; Tricklebank, Mark D.; Schoeffter, Philippe

doi:10.1038/sj.bjp.0701921

Cited by 44 publications

(35 citation statements)

References 30 publications

(29 reference statements)

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“…For example, FAUC213, CP293,019, and Ro61-6270 are antagonists (Hartmann et al, 1996;Sanner et al, 1998;Lober et al, 2001); FAUC113, NGD 94-1, L750,667, and RBI257 are weak partial agonists (Gazi et al, 1998(Gazi et al, , 1999Lober et al, 2001); and PD168,077 and CP226,269 are agonists (Glase et al, 1997;Zorn et al, 1997), yet each of these ligands display mode-1 binding. Likewise, within mode-3 binding compounds there is no apparent correlation with their functional properties, because whereas PNU101,387G is an antagonist (Merchant et al, 1996), Ro10-4548 is an agonist (C. Riemer, personal communication).…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, the clozapine-like structural analogs olanzapine and quetiapine both display a clozapine-like atypical antipsychotic clinical profile and have higher affinity for the D2 than the D4 subtype (ϳ3-4-and 14-fold, respectively; PDSP database, 2004). Although these later findings seemed to exclude D4 as a viable antipsychotic drug target, subsequent in vitro studies with L745,870 and other compounds considered initially to be highly D4-selective antagonists provided evidence for their weak partial agonist activity (Gazi et al, 1998(Gazi et al, , 1999.…”

Section: Abbreviationsmentioning

confidence: 99%

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Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

et al. 2004

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We previously demonstrated that, in the D4 dopamine receptor, the aromatic microdomain that spans the interface of the second and third transmembrane segments influences the high-affinity interactions with the D4-selective ligand L750,667 [3-{[4-(4-iodophenyl) piperazin-1-yl]methyl}-1H-pyrrolo [2,3-b]pyridine] and the D2-selective ligands methylspiperone, aripiprazole, and its congener OPC4392 [7-[3-(4-(2,3-dimethylphenyl) et al., 2000). Here we tested a variety of 1,4-disubstituted aromatic piperidines/piperazines (1,4-DAPs) with different subtype selectivities and functional properties against a panel of D4 receptor mutations in the aromatic microdomain to ascertain whether these ligands recognize this common site. Mutant D4 receptors were constructed by substituting the nonconserved amino acid(s) from the corresponding locations in the D2 receptor. The D4-L2.60W, D4-F2.61V, and D4-LM3.28-3.29FV substitutions result in alterations of the relative position of members of the aromatic microdomain. From these results and molecular models of the ligand-receptor complexes, we conclude that 9 of the 11 D4-selective 1,4-DAPs, including L750,667, have a common pattern of ligand-receptor recognition that depends upon favorable interactions with the phenylalanine at position 2.61 (D4-F2.61V, 20 -96-fold decrease). Like methylspiperone, aripiprazole, and OPC4392, the two D4-selective 1,4-DAPs that are insensitive to the D4-F2.61V mutation are sensitive to aromatics at position 2.60 (D4-L2.60W, 7-20-fold increase), and they all have longer spacer arms that permit their tethered aromatics to adopt alternative orientations in the binding-site crevice. All 11 of the D4-selective 1,4-DAPs were sensitive to the D4-LM3.28-3.29FV mutation (13-494-fold decrease) but not the moderately D2-selective methylspiperone. The inferences suggest that subtype selectivity involves two different modes of interaction with the microdomain for the D4-selective 1,4-DAPs and a third mode for D2-selective 1,4-DAPs.Dopamine receptors belong to the class A family of G protein-coupled receptors (GPCRs) that share a rhodopsin-like structure. In humans and mammals, the dopamine receptor family is comprised of five genotypically distinct members, which are subclassified as D1-like (D1 and D5) and D2-like (D2, D3, and D4) receptors on the basis of their similarities in structure, G protein-coupling preferences, and pharmacology. After the discovery that antipsychotic efficacy strongly correlates with the strength of D2 receptor antagonism (Creese et al., 1976), it was realized that not one, but three subtypes of D2-like receptors existed and that many antipsy-

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Section: Discussionmentioning

confidence: 99%

Section: Abbreviationsmentioning

confidence: 99%

Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

et al. 2004

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“…9 While the clinical trial of a highly D4R-selective ligand (L-745870) did not reveal any benefit, 10 recent findings suggest this compound may in fact be an agonist, rather than an antagonist. 11 Structural features of the D4R suggest that it could play a unique role in neuropsychiatric disorders. Thus in humans and primates the D4R has a polymorphic 16 amino acid repeat in its third intracellular loop ( Figure 1) and humans can exhibit anywhere from two to ten repeats, 12,13 making the D4R one of the most hypervariable proteins in man.…”

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confidence: 99%

D4 dopamine receptor-mediated phospholipid methylation and its implications for mental illnesses such as schizophrenia

et al. 1999

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Keywords: receptors; G protein-coupled; phospholipid methylation; methionine; folic acid; membrane fluidity; purines; de novo synthesis Schizophrenia is a complex psychiatric disorder affecting approximately 1% of the population worldwide with a typical onset between the late teens and midthirties, often in the absence of significant prodromal psychiatric symptoms.1 Decades of research have yielded many theories on the origin of schizophrenia, although none provides a satisfying mechanistic explanation. Logically, dysfunctional neurotransmission is the most widely held theory, and specific abnormalities involving dopaminergic, 2 glutamatergic, 3 GABAergic 4 and nicotinic cholinergic 5 signaling have been proposed. Of these, the 'Dopamine Hypothesis' is dominant, based largely on the recognized therapeutic efficacy of drugs which block D2-like dopamine receptors (ie D2, D3 and D4 receptors), although their specific mechanism of benefit and the importance of individual receptor subtypes remains unclear. The D4

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“…These findings should be judged with caution since there is no demonstration that these drugs block D 4 receptors in vivo. Moreover, L745,870 has partial agonist properties with a relatively high intrinsic activity (Gazi et al 1998).…”

Section: Discussionmentioning

confidence: 99%

JL13, a pyridobenzoxazepine compound with potential atypical antipsychotic activity, increases extracellular dopamine in the prefrontal cortex, but not in the striatum and the nucleus accumbens of rats

Invernizzi

Garavaglia

Samanin

2000

Naunyn-Schmiedeberg's Arch Pharmacol

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In behavioral and receptor binding studies, 5-(4-methylpiperazin-1-yl)-8-chloro-pyridol[2,3b] [1,5]benzoxazepine (JL13) shows an atypical antipsychotic profile. We used microdialysis in awake rats to study the effects of various intraperitoneal doses of JL13 on extracellular concentrations of dopamine in the prefrontal cortex, nucleus accumbens and striatum. JL13 at 20 mg/kg and 40 mg/kg dose-dependently raised extracellular dopamine (234% and 434% of basal levels at peak, respectively) in the prefrontal cortex whereas lower doses (5 mg/kg and 10 mg/kg) had no effect. Extracellular concentrations of dihydroxyphenylacetic acid and homovanillic acid were also significantly increased in the prefrontal cortex of rats given 40 mg/kg JL13 (310% and 230% of basal levels, respectively). At 20 mg/kg and 40 mg/kg JL13 did not affect the extracellular concentrations of dopamine and its metabolites in the striatum and nucleus accumbens. The mechanisms by which JL13 increases cortical dopamine release and the significance for potential antipsychotic efficacy are discussed.

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The agonist activities of the putative antipsychotic agents, L‐745,870 and U‐101958 in HEK293 cells expressing the human dopamine D_4.4 receptor

Cited by 44 publications

References 30 publications

Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

D4 dopamine receptor-mediated phospholipid methylation and its implications for mental illnesses such as schizophrenia

JL13, a pyridobenzoxazepine compound with potential atypical antipsychotic activity, increases extracellular dopamine in the prefrontal cortex, but not in the striatum and the nucleus accumbens of rats

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The agonist activities of the putative antipsychotic agents, L‐745,870 and U‐101958 in HEK293 cells expressing the human dopamine D4.4 receptor

Cited by 44 publications

References 30 publications

Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

Certain 1,4-Disubstituted Aromatic Piperidines and Piperazines with Extreme Selectivity for the Dopamine D4 Receptor Interact with a Common Receptor Microdomain

D4 dopamine receptor-mediated phospholipid methylation and its implications for mental illnesses such as schizophrenia

JL13, a pyridobenzoxazepine compound with potential atypical antipsychotic activity, increases extracellular dopamine in the prefrontal cortex, but not in the striatum and the nucleus accumbens of rats

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The agonist activities of the putative antipsychotic agents, L‐745,870 and U‐101958 in HEK293 cells expressing the human dopamine D_4.4 receptor