58914-91-3Relevant academic research and scientific papers
Anticonvulsant activity and selective inhibition of nicotinamide adenine dinucleotide dependent oxidations by 10 (2 arylimino 3 acetylamino 4 thiazolidonyl)phenothiazines
Singh,Ali,Auyong,Parmar,De Boer
, p. 391 - 396 (2007/10/04)
Several 10 (1 acetyl 4 arylthiosemicarbazido) phenothiazines and their corresponding cyclized 10 (2 arylimino 3 acetylamino 4 thiazolidonyl) phenothiazines were synthesized and characterized by their sharp melting points and elemental analyses. All compounds inhibited nicotinamide adenine dinucleotide (NAD) dependent oxidation of pyruvate and α ketoglutarate selectively, whereas NAD independent oxidation of succinate remained unaltered. All phenothiazine derivatives exhibited anticonvulsant activity, which was reflected by the 20 to 60% protection observed against pentylenetetrazol induced convulsions in mice. The ability of substituted thiosemicarbazido phenothiazines to inhibit cellular respiratory activity was reduced considerably by cyclization to the corresponding substituted thiazolidino phenothiazines. On the other hand, cyclization generally resulted in increased anticonvulsant activity. Thus, the anticonvulsant activity possessed by these substituted phenothiazines bore no relationship with their ability to inhibit selectively the NAD dependent oxidations. Selective inhibition of NAD dependent oxidation of pyruvate and α ketoglutarate in isolated rat brain mitochondria by some 10 (1 acetyl 4 arylthiosemicarbazido) phenothiazines was concentration dependent and competitive in nature.
