Synthesis and Study of Metabolic Antagonists
The central nature of nicotinamide in metabolic processes as a part of the NAD and NADP coenzyme systems prompted the synthesis of a series of N-nicotinyl- and N-isonicotinyl-N'- (substituted)ureas as potential metabolite antagonists of the vitamin. The compounds which were synthesized may be r...
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North Texas State University
1973
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ndltd-unt.edu-info-ark-67531-metadc5009122020-07-15T07:09:31Z Synthesis and Study of Metabolic Antagonists Masingale, Robert Edesta metabolic processes Antimetabolites antimetabolites The central nature of nicotinamide in metabolic processes as a part of the NAD and NADP coenzyme systems prompted the synthesis of a series of N-nicotinyl- and N-isonicotinyl-N'- (substituted)ureas as potential metabolite antagonists of the vitamin. The compounds which were synthesized may be represented by the following general structure, where R = hydrogen, methyl, ethyl, n-propyl, isopropyl, n-butyl, t-butyl, n-hexyl, cyclohexyl, phenyl and a-naphthyl. The observed toxicity of the N-nicotinyl-N'-(substituted)urea analogs may be attributed to the formation of a non-functional N-nicotinyl-N'-(substituted)urea-NAD analog through an exchange reaction catalyzed by NAD-ases in the cell. Support for this view was obtained by an in vitro enzymic synthesis of Nnicotinyl- N'-ethylurea-NAD analog employing N-nicotinyl-7- 1 4CN'- ethylurea. The labeled derivative was characterized through spectral, chromatographic, and chemical reaction studies. North Texas State University Skinner, Charles Gordon Norton, S. J. Brady, William Thomas Dunham, Darrell R. 1973-08 Thesis or Dissertation xv, 112 leaves: ill. Text call-no: 379 N81d no.746 untcat: b2217229 local-cont-no: 1002777715-Masingale https://digital.library.unt.edu/ark:/67531/metadc500912/ ark: ark:/67531/metadc500912 English Public Masingale, Robert Edesta Copyright Copyright is held by the author, unless otherwise noted. All rights reserved. |
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English |
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Others
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metabolic processes Antimetabolites antimetabolites |
spellingShingle |
metabolic processes Antimetabolites antimetabolites Masingale, Robert Edesta Synthesis and Study of Metabolic Antagonists |
description |
The central nature of nicotinamide in metabolic processes as a part of the NAD and NADP coenzyme systems prompted the synthesis of a series of N-nicotinyl- and N-isonicotinyl-N'- (substituted)ureas as potential metabolite antagonists of the vitamin. The compounds which were synthesized may be represented by the following general structure, where R = hydrogen, methyl, ethyl, n-propyl, isopropyl, n-butyl, t-butyl, n-hexyl, cyclohexyl, phenyl and a-naphthyl. The observed toxicity of the N-nicotinyl-N'-(substituted)urea analogs may be attributed to the formation of a non-functional N-nicotinyl-N'-(substituted)urea-NAD analog through an exchange reaction catalyzed by NAD-ases in the cell. Support for this view was obtained by an in vitro enzymic synthesis of Nnicotinyl- N'-ethylurea-NAD analog employing N-nicotinyl-7- 1 4CN'- ethylurea. The labeled derivative was characterized through spectral, chromatographic, and chemical reaction studies. |
author2 |
Skinner, Charles Gordon |
author_facet |
Skinner, Charles Gordon Masingale, Robert Edesta |
author |
Masingale, Robert Edesta |
author_sort |
Masingale, Robert Edesta |
title |
Synthesis and Study of Metabolic Antagonists |
title_short |
Synthesis and Study of Metabolic Antagonists |
title_full |
Synthesis and Study of Metabolic Antagonists |
title_fullStr |
Synthesis and Study of Metabolic Antagonists |
title_full_unstemmed |
Synthesis and Study of Metabolic Antagonists |
title_sort |
synthesis and study of metabolic antagonists |
publisher |
North Texas State University |
publishDate |
1973 |
url |
https://digital.library.unt.edu/ark:/67531/metadc500912/ |
work_keys_str_mv |
AT masingalerobertedesta synthesisandstudyofmetabolicantagonists |
_version_ |
1719328850272321536 |