Gerhard Satzinger scite author profile

Ralitoline, a thiazolidinone derivative chemically distinct from known antiepileptic drugs, possesses remarkable anticonvulsant properties as demonstrated in various animal models of epilepsy. The efficacy of this compound seems to be comparable or even better than that of conventional antiepileptics. In the present study, the activity of ralitoline was investigated in four seizure models in rodents in order to characterize the anticonvulsant profile of action further. In the maximal electroshock seizure test (mice), this compound showed marked anticonvulsant effects (ED50 2.8 mg/kg i.p.). The efficacy of clinically established anti-epileptics was significantly increased when ralitoline was given as co-medication. In the strychnine seizure test (mice), ralitoline (5 and 10 mg/kg) prolonged the latency of tonic seizures as well as the survival time. On the other hand, in the subcutaneous pentylenetetrazol seizure threshold test (mice), this drug revealed limited protective actions at higher doses and increased the effectiveness of ethosuximide. In unrestrained rats with chronically implanted electrodes, ralitoline (5 mg/kg) significantly reduced the duration of electrically-evoked hippocampal discharges and raised the focal stimulation threshold (10 mg/kg). In the rotorod ataxia test (mice), a TD50 value of 14.5 mg/kg i.p. was determined for ralitoline (protective index TD50/MES-ED50 5.2). With regard to the possible mode of action, whole-cell voltage-clamp experiments on cultured neonatal rat cardiomyocytes showed that ralitoline may act specifically on voltage-sensitive sodium channels. The compound inhibited the fast sodium inward current in a frequency- and voltage-dependent manner. In conclusion, the findings confirm the potent anticonvulsant effects of ralitoline, especially against generalized tonic-clonic and complex partial seizures. Moreover, in combination with antiepileptics, an additive synergism can be found at lower concentrations. Regarding the mode of action, this drug was capable of depressing the fast sodium inward current in cultured heart ventricular cells, suggesting that the local anesthetic properties may be important for the anticonvulsant activity of ralitoline.

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Heterocyclen durch Reaktion von Mercapto‐ und Hydroxycarbonsäureestern mit aktivierten Nitrilen

Satzinger¹

1978

Justus Liebigs Ann. Chem.

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Heterocycles by Reaction of Mercapto-and Hydroxycarboxylic Esters with Activated NitrilesActivated nitriles Y -CHR-CN undergo base-catalyzed reaction with a-and P-mercapto-or a-hydroxycarboxylic esters 2a-k to give the cyclic N-acylketene-S,N-and N-acylketene-0,Nacetals 3 [2-methylenethiazolidin-4-ones 3a-w, -4H-1,3-benzothiazin-4-ones 3gg-ii, -0xazo1idin-4-ones 3x-dd and -tetrahydrothiazin-4-one (3ff)l. With the exception of ethyl glycinate 21 (which yields the imidazolin-4-one 3ee), cc-and P-aminocarboxylic esters do not undergo an analogous reaction. However among the nitriles of the general structure Y-CN, only ethyl cyanoformate reacts (with 2b) in a similar way to furnish the 4-hydroxy-

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Heterocyclen durch Reaktion von Mercapto‐ und Hydroxycarbonsäureestern mit aktivierten Nitrilen

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