FAUC 213, a highly selective dopamine D4 receptor full antagonist, exhibits atypical antipsychotic properties in behavioural and neurochemical models of schizophrenia

Boeckler, Frank M.; Russig, Holger; Zhang, Weining; Löber, Stefan; Schetz, John A.; Hübner, Harald; Ferger, Boris; Gmeiner, Peter; Feldon, Joram

doi:10.1007/s00213-004-1782-1

Cited by 34 publications

(19 citation statements)

References 36 publications

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“…Visiers et al (2002) and Ebersole et al (2003) have already demonstrated that such differential positioning can lead to different functional phenotypes. Our discriminant findings should have clinical relevance as well, because the D4 dopamine receptor has been implicated in the treatment of a broad range of medical conditions, including attention deficit hyperactivity disorder (Avale et al, 2004), substance abuse (Lusher et al, 2001), neurodegeneration (Ishige et al, 2001), and psychosis (Boeckler et al, 2004).…”

Section: Discussionmentioning

confidence: 98%

“…The assignment of the 2Ј-substituted diazole FAUC213 as a "neutral antagonist" using different measures of functional activity (fluorometric imaging plate reader G␣ qo5 -based versus mitogenesis-based) has been discussed recently (Stewart et al, 2004). It is remarkable that the D4-selective neutral antagonist FAUC213 was recently shown to have atypical antipsychotic potential in animal models predictive of antipsychotic efficacy in humans (Boeckler et al, 2004), in contrast to the structurally distinct D4-selective neutral antagonist PNU101,387G (sonepiprazole), which has no demonstrable antipsychotic activity in humans (Corrigan et al, 2004). It was previously demonstrated that the D4/D2 pharmacological selectivity profile of L745,870 and its differentially halogenated congener L750,667 become more like the substituted receptor when the corresponding amino acids present in the rat D2 subtype are substituted into a rat D4 receptor background (i.e., D4-F2.61V and D4-LM3.28-3.29FV mutants;Schetz et al, 2000) and when some of these and other reciprocal mutations are made in an N-and C-terminally epitope-tagged human D2 receptor background .…”

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: 98%

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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“…Ropinirole is a preferential D 3/2 agonist (Gerlach et al 2003) with a 20-fold selectivity for D 3 over D 2 receptors (Reavill et al 2000), but it also has affinity for the DRD 4 subtype (Newman-Tancredi et al 2002). The DRD 4 subtype may also play a role in PPI modulation, as selective D 4 antagonists restore amphetamine-induced PPI deficits in mice (Mansbach et al 1998;Okuyama et al 1999;Boeckler et al 2004), although negative results have also been reported (Bristow et al 1997). While administration of agents that facilitate DA neurotransmission reliably disrupts PPI in animal studies (Mansbach et al 1988;Swerdlow et al 1998Swerdlow et al , 2001Swerdlow et al , 2002Swerdlow et al , 2003Geyer et al 2001), results in humans seem to depend on study design and baseline PPI at pretest (Bitsios et al 2005).…”

Section: Introductionmentioning

confidence: 94%

Disruption of prepulse inhibition of the startle reflex by the preferential D3 agonist ropinirole in healthy males

Giakoumaki

Roussos

Frangou³

et al. 2007

Psychopharmacology

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“…Today, seven types of dopaminergic receptors are counted. Because of the large structural variety of heteroarenes, specific ligands of the dopaminergic receptor D3 [126,127] and selective modulators of the dopaminergic receptor D4 were developed [128,129]. New ferrocenyl carboxamides have shown a good affinity for these receptors and also, for serotoninergic receptors from the central nervous system.…”

Section: Dopaminergic Receptors Ligandsmentioning

confidence: 99%

Organometallic Complexes: New Tools for Chemotherapy

Chavain¹,

Biot²

2010

CMC

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The importance of organometallics can be noticed by their presence in all life organisms. The most known natural organometallic molecule is vitamin B12, a porphyrin containing a cobalt atom, useful for several enzymatic transformations. Based on the remarkable properties of this class of compounds, a new area of medicinal research was developed. Gérard Jaouen was the first to introduce the term of "bioorganometallic chemistry" in 1985 although the first organometallic therapeutical was Salvarsan®, discovered by Paul Ehrlich (Nobel Prize in Medicine in 1908). Bioorganometallic chemistry consists of the synthesis and the study of organometallic complexes, complexes with at least one metal-carbon bond, in a biological and medicinal interest. This field of research was accentuated by the discovery of the ferrocene in 1951 by Pauson and Kealy, confirmed in 1952 by Wilkinson (Nobel Prize in 1973). Today, bioorganometallic chemistry includes 5 main domains: (1) organometallic therapeuticals, (2) toxicology and environment, (3) molecular recognition in aqueous phases, (4) enzymes, proteins and peptides, (5) bioanalysis and pharmaceutical sensors. In this review, we focused on organometallic therapeuticals. The exceptional properties of organometallics are first described and then, an overview on the main organometallic complexes used for drug design is presented. This review gives an idea how organometallics can be used for the rational design of new drugs.

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FAUC 213, a highly selective dopamine D4 receptor full antagonist, exhibits atypical antipsychotic properties in behavioural and neurochemical models of schizophrenia

Cited by 34 publications

References 36 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

Disruption of prepulse inhibition of the startle reflex by the preferential D3 agonist ropinirole in healthy males

Organometallic Complexes: New Tools for Chemotherapy

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