Abstract:Tautomeric forms of Thiosemicarbazones have been investigated by spectrometric methods, their chemical reactivity and theoretical calculations of the relative tautomers stabilities. The mass spectral fragmentation of thiosemicarbazones synthesized from acetophenones has been studied by CG/MS. The analysis of the corresponding spectra shows not only the regular fragmentation mechanisms but homolytic ruptures from even-electron species. 1 H NMR spectra exhibit signals for the most intense open thioketo tautomeri… Show more
“…46,47 It is worth mentioning that the chemical shi values observed for all the NH protons in the presence of phenylsulfonylmethylene group showed a down-eld shi of approximately +0.40 to +1.3 ppm compared to the previously reported analog lacking phenylsulfonylmethylene group. 48 Also, the 13 C NMR spectrum of the carbothioamide derivative 3 showed a signal at d ¼ 179 ppm assigned to the C]S group, in addition to another signal at d ¼ 139 ppm corresponding to C]N.…”
Thiazole derivatives 7b and 13a were superior to dabrafenib against B-RAFV600E kinase and potently inhibited the growth of WM266.4 melanoma cells. Compound 7b suppressed the phosphorylation of downstream ERK1/2 from WM266.4 cells.
“…46,47 It is worth mentioning that the chemical shi values observed for all the NH protons in the presence of phenylsulfonylmethylene group showed a down-eld shi of approximately +0.40 to +1.3 ppm compared to the previously reported analog lacking phenylsulfonylmethylene group. 48 Also, the 13 C NMR spectrum of the carbothioamide derivative 3 showed a signal at d ¼ 179 ppm assigned to the C]S group, in addition to another signal at d ¼ 139 ppm corresponding to C]N.…”
Thiazole derivatives 7b and 13a were superior to dabrafenib against B-RAFV600E kinase and potently inhibited the growth of WM266.4 melanoma cells. Compound 7b suppressed the phosphorylation of downstream ERK1/2 from WM266.4 cells.
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