New pyridobenzodiazepine derivatives as potential antipsychotics: synthesis and neurochemical study

Liégeois, Jean François; Bruhwyler, Jacques; Damas, Jacques; Nguyen, Thuy Phuong; Chleide, E.; Mercier, Michel; Rogister, F.; Delarge, J.

doi:10.1021/jm00067a009

Cited by 62 publications

(64 citation statements)

References 12 publications

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“…The titled compound, a fumarate salt of 8-chloro-5-(4-methylpiperazin-1 -yl)pyrido [2,3-i>] [ 1,5]benzoxazepine [2,3] also called JL13 was prepared as part of our study of dopamine receptors and related binding sites implicated in schizophrenia [1,4]. Extensive investigations have revealed a very promising antipsychotic profile in several preclinical models [5], The oxazepine ring has a boat conformation where the four C atoms of the outer ring junction are almost coplanar: the maximum deviation from their mean plane is 0.022(1) A (cf.…”

Section: Discussionmentioning

confidence: 99%

Crystal structure of bis(8-chloro-5-(4-methylpiperazinium-1-yl)pyrido- [2,3-b][1,5]benzoxazepine) fumarate - fumaric acid solvate (1:1), (C17H18ClN4O)2(C4H2O4) · C4H4O4

Dupont¹,

Liégeois²

2004

Zeitschrift Für Kristallographie - New Crystal Structures

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C42H42CI2N8O10, triclinic, PI (no. 2), a = 9.625(1) A, b = 9.929(3) A, c = 11.860(2) A, a = 108.12(2)°, fi = 73.24(1)°, y = 87.38(1)°, V= 1019.9 A 3 , Z = 1, Rgi(F) = 0.043, wR^F 2 ) = 0.131, 7=293 K. Source of materialThe compound was synthesized according to methods previously described [1], Crystals were obtained by slow evaporation of a methanol solution. Experimental detailsThe fumaric acid molecule is disordered, mainly the C2A atom. and their Uij equated. H19, H02A and H2B were located by Fourier difference synthesis. Only H02A was included in the refinement. All other H atoms were restrained (included as riding atoms), with isotropic temperature parameters fixed at 1.2 U e q of the parent atom (1.5 U eq for methyl). In the final cycles of refinement, the position of atom C2A of the fumaric acid molecule (A) was split into two sites, C2A1 and C2A2, with occupation factors of 0.56 and 0.44, respectively (figure, bottom). The introduction of this disordered distribution improved the residual densities in the final difference map and also the conventional R and wRfF 2 ) values. No significant electron density peak was found near 02B. ). The tetrahedral conformation of N19 is similar in both structures: in the fumarate salt, the sum of the three C-N19-C angles is equal to 331.5(1)°, in comparison with 332.05(7)° for JL13. The conformation around N16 is more tetrahedral in the salt than in JL13, with the sums of the three external angles around N16 equal to 346.6(1)° and 352.91(6)°, respectively. Hie centres of symmetry of the fumaric acid molecules coincide respectively with the 1/2,1/2,0 and the 1/2,1/2,1/2 sites. So the asymmetric part of the unit cell contains three residues: the 8-chloro-5-(4-methylpiperazinium-1 -yl)pyrido[2,3-f>] [1,5]benzoxazepine molecular ion with a protonated N19 + amine, half a fumaric acid molecule (A) and half a fumarate moiety (B) with a COO" group. Discussion

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Section: Discussionmentioning

confidence: 99%

Crystal structure of bis(8-chloro-5-(4-methylpiperazinium-1-yl)pyrido- [2,3-b][1,5]benzoxazepine) fumarate - fumaric acid solvate (1:1), (C17H18ClN4O)2(C4H2O4) · C4H4O4

Dupont¹,

Liégeois²

2004

Zeitschrift Für Kristallographie - New Crystal Structures

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“…The compound was synthesized according to Li6geois et al (1993) at the laboratory of Medicinal Chemistry of Liege. Crystals were obtained by slow evaporation of a methanol solution at room temperature.…”

Section: Methodsmentioning

confidence: 99%

3-Methyl-6-(4-methylpiperazin-1-yl)-11H-pyrido[2,3-b][1,4]benzodiazepine

Dupont¹,

Liégeois

Rogister³

et al. 1995

Acta Crystallogr C

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The synthesis and crystal structure of C18H21N5 has been undertaken as part of a study of dopamine receptors. The diazepine ring has a boat conformation. The four C atoms of the outer ring junctions are almost coplanar; the maximum deviation from their mean plane CommentThe molecular structure of the title compound, (I), may be compared, for example, with that of IIformyl -5 -(4-methylpiperazin-1 -yl )-1 IH-pyrido [ 2,3-b] Johnson, 1976) of the title compound showing the molecular structure and the atom-labelling scheme. Displacement ellipsoids are shown at 50% probability levels and H atoms are drawn as small circles of arbitrary radii.The diazepine ring has a boat conformation, where N5 is the 'prow' and C12 and C13 constitute the 'stem'. The piperazine ring has the normal chair conformation. The dihedral angle between the benzene and pyridine rings is 119.41 (7) ° [this angle is 115.1 (1)and 115.0(1) ° in compounds (II) and (III), respectively]. The distances between the methylpiperazine N atom and the centres of the two aromatic rings are 7.727 (4) and 6.084 (4)A [7.768 (4) and 6.107 (4) in (II); 7.726 (4) and 5.934 (4)/~ in (IH)]. The cohesion of the crystal is the result of both van der Waals interactions and one hydrogen bond, N5--H5...N7 i [N5...N7 i 3.048 (2), H5...N7 i 2.01/~, N5--H5...N7 i 174°; symmetry code: (i) 1-x, 2-y, -z]. Analogues of the title compound will be the subject of future investigations. ExperimentalThe compound was synthesized according to Li6geois et al. (2) C4---N5---C6114.66 (14) N12--C13--NI6 118.6 (2) C11----C6---N5 120.9 (2) N12---C13---C14 126.3 (2) C6---N7----C8 117.8 (2) N16----C13---C14 114.9 (2) C6--C1 I--N12 123.5 (2) C4---C1~-C13 120.1 (2)H atoms were placed at standard calculated positions, except for atom HN5, which was obtained from a difference map. In the refinement, H atoms were constrained (included as riding atoms), except for HN5, which was kept fixed.Data collection: DIF4 (Stoe & Cie, 1987a). Cell refinement: DIF4. Data reduction: REDU4 (Stoe & Cie, 1987c). Program(s) used to solve structure: SHELXS86 (Sheldrick, 1990). Program(s) used to refine structure: SHELXL93 . Molecular graphics: ORTEPII (Johnson, 1976). Software used to prepare material for publication: SHELXL93.The authors thank M. M. Vermeire for his helpful assistance in the diffractometry measurements and the Belgian FNRS for financial support.Lists of structure factors, anisotropic displacement parameters, Hatom coordinates and complete geometry have been deposited with the IUCr (Reference: BM1002).

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“…7,8 Although the use of atypical antipsychotic drug clozapine in treatment of schizophrenia avoided the main disadvantage of typical ones e.g. extrapyrimidal side effects, still its use is limited due to the ability to induce agranulocytosis sedation, dizziness, headache, nausea, vomiting (neurotoxicity) and other side effects.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and Pharmacological Studies for New Benzotriazole and Dibenzodiazepine Derivatives as Antipsychotic Agents

2009

Bulletin of the Korean Chemical Society

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New benzotriazoles (5-8) or dibenzodiazepine derivatives (11-18) were synthesized starting from 3-[(2-amino-4,5-disubstitutedphenyl)amino]-5,5-disubstitutedcyclohex-2-enones (1-4) through internal coupling of their diazonium salts or internal Mannich reaction in the presence of aromatic aldehydes. Pharmacological evaluation of benzotriazole and dibenzodiazepine derivatives for their clozapine-like properties revealed that dibenzodiazepine 11 bearing 4-bromophenyl group exhibited the same antipsychotic activity as the reference drug clozapine while the activity of benzotriazole 7 was 25% lesser than that of clozapine. Moreover, compounds 7 and 11 did not show significant CNS depressant activity as well as no or slight neurotoxicity on contrast to clozapine when tested in mice using forced swim, rotarod and horizontal screen tests.

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New pyridobenzodiazepine derivatives as potential antipsychotics: synthesis and neurochemical study

Cited by 62 publications

References 12 publications

Crystal structure of bis(8-chloro-5-(4-methylpiperazinium-1-yl)pyrido- [2,3-b][1,5]benzoxazepine) fumarate - fumaric acid solvate (1:1), (C17H18ClN4O)2(C4H2O4) · C4H4O4

Crystal structure of bis(8-chloro-5-(4-methylpiperazinium-1-yl)pyrido- [2,3-b][1,5]benzoxazepine) fumarate - fumaric acid solvate (1:1), (C17H18ClN4O)2(C4H2O4) · C4H4O4

3-Methyl-6-(4-methylpiperazin-1-yl)-11H-pyrido[2,3-b][1,4]benzodiazepine

Synthesis and Pharmacological Studies for New Benzotriazole and Dibenzodiazepine Derivatives as Antipsychotic Agents

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