Prodrugs of Nitroxyl as Potential Aldehyde Dehydrogenase Inhibitors vis-a-vis Vascular Smooth Muscle Relaxants

Nagasawa, Hiromichi; Kawle, Sagar P.; Elberling, James A.; DeMaster, Eugene G.; Fukuto, Jon M.

doi:10.1021/jm00011a005

Cited by 89 publications

(72 citation statements)

References 5 publications

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“…In accordance with the mechanism proposed by Ishii and co-workers [5] the carbon radical chain promoter (NHPI or NHS) is involved in two chain propagation steps (see Scheme 5). Table 7.…”

Section: Mechanistic Considerations: Nhs Vs Nhpisupporting

confidence: 61%

“…[4] We reasoned that the use of Nhydroxysaccharin (NHS; 1b), [5] in which one carbonyl group (CO) is replaced by the more electron-withdrawing sulphonyl (SO 2 ) group, could provide an even more effective carbon radical chain promoter (CRCP). [6] In the course of our study on the oxidation of large ring cycloalkanes with molecular oxygen we found that NHS was an efficient catalyst in combination with cobalt salts.…”

Section: Introductionmentioning

confidence: 99%

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Aerobic Oxidation of Cycloalkanes, Alcohols and Ethylbenzene Catalyzed by the Novel Carbon Radical Chain Promoter NHS (N‐Hydroxysaccharin)

et al. 2004

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Replacement of Ishii×s N-hydroxyphthalimide (NHPI) with the novel carbon radical chain promoter N-hydroxysaccharin (NHS) affords, in combination with metal salts, notably Co, or other additives, selective catalytic autoxidation of hydrocarbons, alcohols and alkylbenzenes under mild conditions (25 ± 100 8C, O 2 1 atm). The effects of solvent, temperature and the nature of the additives were investigated to give an optimised oxidation protocol for the various systems. The NHS/Co combination was more reactive than NHPI/Co in the autoxidation of cycloalkanes. In contrast, the opposite order of reactivity was observed in the autoxidation of ethylbenzene and alcohols. It is suggested, on the basis of bond dissociation energy (BDE) considerations, that this is a result of a change in the rate-limiting step with the more reactive ethylbenzene and alcohol substrates. In the autoxidation of the model cycloalkane, cyclododecane, the best results (90% selectivity to a 4 : 1 mixture of alcohol and ketone at 24% conversion) were obtained with NHS/Co(acac) 3 in PhCF 3 at 80 8C. Competition experiments revealed that, in contrast to what is commonly believed, formation of the dicarboxylic acid by ring opening is not a result of further oxidation of the ketone product. It is suggested that ring opened products are a result of˚-scission of the cycloalkoxy radical formed via (metal-catalysed) decomposition of the hydroperoxide. This is suppressed in the presence of NHS (or NHPI) which efficiently scavenge the alkoxy radicals.

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“…In accordance with the mechanism proposed by Ishii and co-workers [5] the carbon radical chain promoter (NHPI or NHS) is involved in two chain propagation steps (see Scheme 5). Table 7.…”

Section: Mechanistic Considerations: Nhs Vs Nhpisupporting

confidence: 61%

Section: Introductionmentioning

confidence: 99%

Aerobic Oxidation of Cycloalkanes, Alcohols and Ethylbenzene Catalyzed by the Novel Carbon Radical Chain Promoter NHS (N‐Hydroxysaccharin)

et al. 2004

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“…It is tempting to speculate that the cytotoxicity of HNO released from 1b could be amplified by its conversion to ⅐ OH in ischemia-acidified tissue (64). However, further studies are needed to understand the effects of HNO in biological systems, as well as to advance the mechanistic algorithms for interpretation and prediction of the cytotoxicity of HNO-releasing prodrugs such as Na 2 N 2 O 3 , derivatives of nitrosobenzene (10), benzisothiazol (66), chloropropamide (67), and N-hydroxybenzene carboximidate (68). …”

Section: Discussionmentioning

confidence: 99%

Formation of Nitroxyl and Hydroxyl Radical in Solutions of Sodium Trioxodinitrate

Ivanova

Salama

Clancy

et al. 2003

Journal of Biological Chemistry

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Despite its negative redox potential, nitroxyl (HNO) can trigger reactions of oxidation. Mechanistically, these reactions were suggested to occur with the intermediate formation of either hydroxyl radical ( ⅐ OH) or peroxynitrite (ONOO ؊ ). In this work, we present further experimental evidence that HNO can generate ⅐ OH. Sodium trioxodinitrate (Na 2 N 2 O 3 ), a commonly used donor of HNO, oxidized phenol and Me 2 SO to benzene diols and ⅐ CH 3 , respectively. The oxidation of Me 2 SO was O 2 -independent, suggesting that this process reflected neither the intermediate formation of ONOO ؊ nor a redox cycling of transition metal ions that could initiate Fenton-like reactions. In solutions of phenol, Na 2 N 2 O 3 yielded benzene-1,2-diol and benzene-1,4-diol at a ratio of 2:1, which is consistent with the generation of free ⅐ OH. Ethanol and Me 2 SO, which are efficient scavengers of ⅐ OH, impeded the hydroxylation of phenol. A mechanism for the hydrolysis of Na 2 N 2 O 3 is proposed that includes dimerization of HNO to cis-hyponitrous acid (HO-N‫؍‬N-OH) with a concomitant azo-type homolytic fission of the latter to N 2 and ⅐ OH. The HNO-dependent production of ⅐ OH was with 1 order of magnitude higher at pH 6.0 than at pH 7.4. Hence, we hypothesized that HNO can exert selective toxicity to cells subjected to acidosis. In support of this thesis, Na 2 N 2 O 3 was markedly more toxic to human fibroblasts and SK-N-SH neuroblastoma cells at pH 6.2 than at pH 7.4. Scavengers of ⅐ OH impeded the cytotoxicity of Na 2 N 2 O 3 . These results suggest that the formation of HNO may be viewed as a toxicological event in tissues subjected to acidosis.The biochemistry of nitroxyl (HNO) has attracted considerable interest in recent years. In cells, the biosynthesis of HNO is believed to proceed via reduction of NO ⅐ by superoxide dismutase (1) and cytochrome c (2), and reduction of S-nitrosoglutathione by low molecular weight and protein thiols (3-5). It has been suggested that HNO can affect the etiology of various pathophysiological conditions such as inflammation and neurodegenerative diseases, especially when H 2 O 2 and transition metal ions are present (6, 7). Similar to NO ⅐ and NO ϩ , HNO is a potent inducer of the antioxidant protein heme oxygenase 1 (8), exhibits vasorelaxant properties (9), and modulates the activity of thiol-containing proteins, such as aldehyde dehydrogenase (10, 11) and the N-methyl-D-aspartate receptor (12, 13). In in vivo experiments, Paolocci et al. (14) observed that HNO exerts positive inotropic and lusitropic action, which unlike NO ⅐ and nitrates is independent and additive to ␤-adrenergic stimulation and increases the release of plasma calcitonin gene-related peptide; these results suggest that donors of HNO are potential prodrugs for the treatment of heart failure (14). At high doses, HNO has been shown to induce DNA singlestrand breakage (15, 16) and a concentration-dependent cytotoxicity in murine thymocytes (16). This cytotoxicity was associated with activation of the nuclear nick sen...

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“…However, contrary to expectations, extremely low concentrations of nitroxyl deactivate select thiol proteins, such as glyceraldehyde 3-phosphate dehydrogenase, without altering the cellular GSH/GSSG ratio (DeMaster et al, 1998;Paolocci et al, 2007). Pro-drugs of nitroxyl, such as derivatives of N,O-diacylated N-hydroxyarylsulfonamide (Fukuto et al, 1992) and N-acyloxy-Oarenesulfonylated benzenecarboximidic acid (Lee et al, 2001), are being developed, albeit with more emphasis on their use as vasodilators (Nagasawa et al, 1995) that are bioactivated by the esterase activity of the ALDH enzyme. In the treatment of alcohol addiction, cyanamide is a second-line drug relative to disulfiram owing to its greater capacity to induce liver injury compared with disulfiram (Tamai et al, 2000).…”

Section: G Cyanamidementioning

confidence: 99%

Aldehyde Dehydrogenase Inhibitors: a Comprehensive Review of the Pharmacology, Mechanism of Action, Substrate Specificity, and Clinical Application

et al. 2012

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Prodrugs of Nitroxyl as Potential Aldehyde Dehydrogenase Inhibitors vis-a-vis Vascular Smooth Muscle Relaxants

Cited by 89 publications

References 5 publications

Aerobic Oxidation of Cycloalkanes, Alcohols and Ethylbenzene Catalyzed by the Novel Carbon Radical Chain Promoter NHS (N‐Hydroxysaccharin)

Aerobic Oxidation of Cycloalkanes, Alcohols and Ethylbenzene Catalyzed by the Novel Carbon Radical Chain Promoter NHS (N‐Hydroxysaccharin)

Formation of Nitroxyl and Hydroxyl Radical in Solutions of Sodium Trioxodinitrate

Aldehyde Dehydrogenase Inhibitors: a Comprehensive Review of the Pharmacology, Mechanism of Action, Substrate Specificity, and Clinical Application

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