Comparison of the in vivo pharmacological profiles of sabeluzole and its enantiomers

Werbrouck, Leen; Megens, Anton; Stokbroekx, Raymond A.; Niemegeers, C. J. E.

doi:10.1002/ddr.430240104

Cited by 9 publications

(5 citation statements)

References 9 publications

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“…A 0 1992 WILEY-LISS, INC. similar improvement of memory was obtained in a pilot study with patients suffering from age-associated memory impairment (Clincke et al, 1992;Tritsmans et al, 1990). Apart from cognitive enhancing activity, sabeluzole has also pronounced antihypoxic and anticonvulsant properties (Wauquier et al, 1986;Werbrouck et al, 1991).…”

Section: Introductionsupporting

confidence: 71%

Chronic treatment with sabeluzole protects cultured rat brain neurons from the neurotoxic effects of excitatory amino acids

Pauwels

Assouw

Peeters

et al. 1992

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The neuroprotective properties of the cognitive enhancer sabeluzole were investigated in rat brain neuronal cultures derived from the hippocampal formation of 17-day-old rat embryos. Measurement of the neuronal cytoskeletal microtubule-associated protein, MAP2, was used to assess survival of neurons after exposure of neuronal cultures to glutamate. MAP2 was quantified in neuronal cell homogenates by means of an enzyme-linked immunosorbent assay (ELISA) using a mouse monoclonal MAP2 antibody, peroxidase-labeled goat anti-mouse Ig antiserum, and 2,2'-azido-di-[3-ethylbenz-thiazoline] sulphonate (ABTS) as substrate. Exposure of 7-day-old neuronal cultures to 1 mM glutamate for 16 hours led to a three-fold increase in released lactate dehydrogenase (LDH) and a 40% decrease in cellular MAP2 content. Acute treatment of neuronal cultures with 10 microM sabeluzole yielded a 40% drop in released LDH induced by glutamate. Cultures treated chronically with 0.1 microM sabeluzole on days 1 and 4 in culture showed, after 1 week in culture, a MAP2 content and total LDH activity that was not different from control cultures. A 16-hour exposure to 1 mM glutamate did not induce LDH release or changes in MAP2 levels in sabeluzole-treated cultures. A single treatment with 0.1 microM sabeluzole between day 1 to 5 induced a 70-80% drop in glutamate-induced released LDH in 7-day-old neuronal cultures. Full and partial neuronal protection after chronic sabeluzole treatment at 0.1 microM was also observed for neurotoxicity induced by 5 mM N-methyl-D-aspartate (NMDA) and 1 mM kainic acid or 30 microM veratridine, respectively. Within a series of compounds such as Ca++ and Na+ channel antagonists, glutamate receptor antagonists and various neurotransmitter receptor antagonists, sabeluzole, chronically given, were the most potent for inhibition of released LDH induced by 1 mM glutamate (IC50-value: 34 +/- 13 nM). In conclusion, chronic sabeluzole treatment protects cultured rat brain neurons from excitotoxic aggression.

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Section: Introductionsupporting

confidence: 71%

Chronic treatment with sabeluzole protects cultured rat brain neurons from the neurotoxic effects of excitatory amino acids

Pauwels

Assouw

Peeters

et al. 1992

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“…Non-imidazole structures such as betahistine [17] , phencyclidine [18] , dimaprit [19,20] , clozapine [21] , and sabeluzole [22] which is a benzothiazole derivative, have only weak H 3 antagonist activity. Very recently, Ganellin et al [23] reported a novel series of homologues O and S isosteric tertiary amines of N-ethyl-N-(4-phenylbutyl)amine as potent non-imidazole histamine H 3 receptor antagonists.…”

Section: Introductionmentioning

confidence: 99%

Non-Imidazole Histamine H3 Ligands, Part 2: New 2-Substituted Benzothiazoles as Histamine H3 Antagonists

Walczyński¹,

Guryn²,

Zuiderveld

et al. 1999

Arch. Pharm. Pharm. Med. Chem.

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“…The next step was the conversion of the carbamate 2 into the corresponding 2-benzothiazolyl derivative 3. An earlier two-step procedure 12,21,22 was reported to afford 3 by reaction of 2 with isothiocyanatobenzene to give a thiourea intermediate, which in turn underwent oxidative cyclization affording the desired product (overall yield about 71%). Taking inspiration from a procedure reported in the literature for the preparation of various 2-methylamino-and 2-dimethylamino benzocondensed azoles, 23 we explored the possibility of performing the direct coupling of commercially available 2-chlorobenzothiazole with 2.…”

Section: Resultsmentioning

confidence: 98%

Facile, alternative route to Lubeluzole, its enantiomer, and the racemate

et al. 2006

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Lubeluzole [(S)-9] has been synthesized by a convergent synthesis, alkylation of N-methyl-N-piperidin-4-yl-1,3-benzothiazol-2-amine (4) with (+)-(R)-1-chloro-3-(3,4-difluorophenoxy)propan-2-ol [(+)-(R)-8] being the key step. Alcohol (+)-(R)-8 was obtained from commercially available (R)-epichlorohydrin [(R)-6], while the thiazole derivative 4 was easily obtained starting from N-protected piperidin-4-one (1) in a three-step procedure. The same method was used in order to obtain both the (R)-stereoisomer of lubeluzole [(R)-9] and its racemate [(RS)-9]. Overall yields ranged from 20% to 35%. The enantiomeric excess values for (S)-9 and (R)-9 were 97% and 94% respectively, as analyzed by chiral HPLC.

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Comparison of the in vivo pharmacological profiles of sabeluzole and its enantiomers

Cited by 9 publications

References 9 publications

Chronic treatment with sabeluzole protects cultured rat brain neurons from the neurotoxic effects of excitatory amino acids

Chronic treatment with sabeluzole protects cultured rat brain neurons from the neurotoxic effects of excitatory amino acids

Non-Imidazole Histamine H3 Ligands, Part 2: New 2-Substituted Benzothiazoles as Histamine H3 Antagonists

Facile, alternative route to Lubeluzole, its enantiomer, and the racemate

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