Diethylcarbamoylating/Nitroxylating Agents as Dual Action Inhibitors of Aldehyde Dehydrogenase:  A Disulfiram−Cyanamide Merger

Conway, T. T.; DeMaster, Eugene G.; Goon, David J. W.; Shirota, Frances N.; Nagasawa, Hiromichi

doi:10.1021/jm990235p

Cited by 26 publications

(8 citation statements)

References 22 publications

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“…In a series of studies attempting to elucidate the mechanism of inhibition of AlDH by the hypoglycemic agent chlorpropamide, structure/activity examinations [92][93][94][95] suggested that sulfohydroxamic acids can be derivatized to give esterase-activated (compare DBHC, Scheme 2), as well as cytochrome P-450-acitvated, inhibitors of AlDH. In the case of the N-acylated, O-methylated sulfohydroxamic acids, O-demethylation by cytochrome P-450 gives rise to Nacylated sulfohydroxamic acids (Scheme 6; R groups shown are typical substituents, but not all combinations have been prepared).…”

Section: Scheme (3)mentioning

confidence: 99%

Donors of HNO

Miranda

Nagasawa

Toscano

2005

CTMC

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Recent comparisons of the pharmacological effects of nitric oxide (NO) and nitroxyl (HNO) donors have demonstrated that the responses to these redox-related nitrogen oxides are nearly universally dissimilar. These analyses have suggested the existence of mutually exclusive signaling pathways as a result of discrete chemical interactions of HNO and NO with a variety of critical biomolecules. Although the mechanisms of action are currently unresolved, the pharmacological responses to HNO are promising for clinical treatment of cardiovascular diseases such as heart failure, myocardial infarction and stroke. This review provides a detailed discussion of the most commonly utilized donors of HNO as well as a guideline for the characterization of novel donors.

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Section: Scheme (3)mentioning

confidence: 99%

Donors of HNO

Miranda

Nagasawa

Toscano

2005

CTMC

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“…The choice of O-protecting groups, 14 particularly, acid-labile t-Bu, THP, and 2,4-dimethoxybenzyl 15 makes the subsequent automated high-throughput solid-phase synthesis a more robust process, as the protecting group can also be removed during the final cleavage from the solid support. Some of the known N,O-bisprotected hydroxylamine derivatives used for the synthesis of hydroxamates, including BOC-NH-OTHP, 16 BOC-NH-OTBDMS, 16 BOC-NH-OBn, 3,6 and O- (2,4)-dimethoxybenzyl-N- (2,4,6)-trimethoxybenzylhydroxylamine, 15 and certain previously reported Narylsulfonyl-O-substituted hydroxylamine derivatives, 17,18 suffer mainly from a lack of orthogonality of the N-and O-protecting groups during deprotection.…”

Section: Methodsmentioning

confidence: 99%

O-Protected N-(2-Nitrophenylsulfonyl)hydroxylamines: Novel Reagents for the Synthesis of Hydroxamates

Reddy¹,

Schall²,

Wheatley³

et al. 2004

Synthesis

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“…[5][6][7] In drug development, disulfide agents such as disulfiram exhibit unique pharmacological activities such as antialcoholic, and many other disulfides are used as antipoliovirus and antibacterial effects. [8][9][10] Interestingly, the S-S bond is employed for the delivery of drugs and release systems because of its ability to cleave upon an intracellular thiol-redox process. [11] Additionally, this important bond also substantially exists in natural products and food additives.…”

Section: Introductionmentioning

confidence: 99%

Highly efficient NHC‐iridium(I) catalyzed disulfide bond forming reaction

Iali

Suleiman

Ali

2022

Applied Organom Chemis

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The N‐heterocyclic carbene (NHC) iridium(I) complex [IrCl (COD)(IMes)] [IMes = 1,3‐bis(2,4,6‐trimethylphenyl) imidazole‐2‐ylidene] showed an excellent catalytic activity in the reactions of the aerobic oxidative coupling of thiols into disulfides. The use of oxygen of air as a green oxidant allows the thiols to be quantitatively converted into the corresponding disulfides under mild conditions and in a short reaction time. The replacement of chloride ligand on the iridium by the strong‐donating thiolate ligand yielded an electron‐rich and sensitive‐to‐oxygen active species [Ir(S‐R)(COD)(IMes)] at room light and subsequently promoting the catalytic oxidative coupling reactions. This active species was successfully isolated and characterized by X‐ray diffraction and found also to be essential in revealing a plausible mechanism for this Ir‐catalyzed transformation. The Density Functional Theory (DFT)‐calculated free energy profile of the proposed mechanism of our developed catalyst system can reasonably account for the key role of air in pursuing the catalytic reaction. Overall, the obtained computational and the experimental results of this study are in good agreement.

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Diethylcarbamoylating/Nitroxylating Agents as Dual Action Inhibitors of Aldehyde Dehydrogenase: A Disulfiram−Cyanamide Merger

Cited by 26 publications

References 22 publications

Donors of HNO

Donors of HNO

O-Protected N-(2-Nitrophenylsulfonyl)hydroxylamines: Novel Reagents for the Synthesis of Hydroxamates

Highly efficient NHC‐iridium(I) catalyzed disulfide bond forming reaction

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