Superoxide, reactions, with radicals

In connection with the antioxidant properties of L-ascorbic acid and its stability, many kinetic and mechanistic studies have been performed. For instance, it has been shown a role as a radical scavenger in the autooxidation of methyl linoleate, and its synergistic effect when used with vitamin E.362 The photooxidation,363 superoxide-mediated oxidations,364 reactions with radicals,365 and the influence of other agents, including ultrasound and y-rays,366 have been reported. 

In a study directed to the analysis of the role of Fe and the generation of H2O2 in Escherichia coli (McCormick et al. 1998), hydroxyl radicals were specihcally trapped by reaction with ethanol to give the a-hydroxyethyl radical. This formed a stable adduct with a-(4-pyridyl-l-oxide)-iV-t-butyl nitroxide that was not formed either by superoxide or hydroxyl radicals. The role of redox-reactive iron is to use EPR to analyze the EPR-detectable ascorbyl radicals. 

Fig. 1 Schematic mechanism for the long-distance oxidation of DNA. Irradiation of the anthraquinone (AQ) and intersystem crossing (ISC) forms the triplet excited state (AQ 3), which is the species that accepts an electron from a DNA base (B) and leads to products. Electron transfer to the singlet excited state of the anthraquinone (AQ 1) leads only to back electron transfer. The anthraquinone radical anion (AQ ) formed in the electron transfer reaction is consumed by reaction with oxygen, which is reduced to superoxide. This process leaves a base radical cation (B+-, a hole ) in the DNA with no partner for annihilation, which provides time for it to hop through the DNA until it is trapped by water (usually at a GG step) to form a product, 7,8-dihydro-8-oxoguanine (8-OxoG)...

Other cationic surfactants such as TTAB, DTAB, DODAB, STAC, CEDAB, and DDDAB have been used in CL reactions with less frequency. Thus, tetradecyltrimethylammonium bromide [TTAB] has been used to increase the sensitivity of the method to determine Fe(II) and total Fe based on the catalytic action of Fe(II) in the oxidation of luminol with hydrogen peroxide in an alkaline medium [47], While other surfactants such as HTAB, hexadecylpiridinium bromide (HPB), Brij-35, and SDS do not enhance the CL intensity, TTAB shows a maximum enhancement at a concentration of 2.7 X 10 2 M (Fig. 11). At the same time it was found that the catalytic effect of Fe(II) is extremely efficient in the presence of citric acid. With regard to the mechanism of the reaction, it is thought that Fe(II) forms an anionic complex with citric acid, being later concentrated on the surface of the TTAB cationic micelle. The complex reacts with the hydrogen peroxide to form hydroxy radical or superoxide ion on the... 

The reaction partners for antiradical substances are products of the first reaction. The SOD reacts selectively with 02" the nonenzymic antioxidants can react with both superoxide and luminol radicals. Theoretically, the carbonate radicals can also be involved in the PCL [25, 26],... 

Mechanism of the Interaction of Peroxidases with Hydroperoxides Role of Superoxide and Hydroxyl Radicals in Reactions Catalyzed by Peroxidases... 

In the last 10 to 15 years, many experimental and theoretical studies have been dedicated to the study of peroxynitrite reactions. Free radical and non-free radical mechanisms of peroxynitrite action have been proposed, which were discussed in numerous studies (see for example, Refs. [103-110]). In accord with non-radical mechanism an activated form of peroxynitrous acid is formed in the reaction of superoxide with nitric oxide, which is able to react with biomolecules without the decomposition to HO and N02 radicals. 

Thus the competition between stimulatory and inhibitory effects of NO depends on the competition between two mechanisms the direct interaction of NO with free radicals formed in lipid peroxidation and the conversion of NO into peroxynitrite or other reactive NO metabolites. Based on this suggestion, Freeman and his coworkers [42-44] concluded that the prooxidant and antioxidant properties of nitric oxide depend on the relative concentrations of NO and oxygen. It was supposed that the prooxidant effect of nitric oxide originated from its reaction with dioxygen and superoxide ... 

As mentioned earlier, when NO concentration exceeds that of superoxide, nitric oxide mostly exhibits an inhibitory effect on lipid peroxidation, reacting with lipid peroxyl radicals. These reactions are now well studied [42-44]. The simplest suggestion could be the participation of NO in termination reaction with peroxyl radicals. However, it was found that NO reacts with at least two radicals during inhibition of lipid peroxidation [50]. On these grounds it was proposed that LOONO, a product of the NO recombination with peroxyl radical LOO is rapidly decomposed to LO and N02 and the second NO reacts with LO to form nitroso ester of fatty acid (Reaction (7), Figure 25.1). Alkoxyl radical LO may be transformed into a nitro epoxy compound after rearrangement (Reaction (8)). In addition, LOONO may be hydrolyzed to form fatty acid hydroperoxide (Reaction (6)). Various nitrated lipids can also be formed in the reactions of peroxynitrite and other NO metabolites. 

Thus, LOX-catalyzed oxidative processes are apparently effective producers of superoxide in cell-free and cellular systems. (It has also been found that the arachidonate oxidation by soybean LOX induced a high level of lucigenin-amplified CL, which was completely inhibited by SOD LG Korkina and TB Suslova, unpublished data.) It is obvious that superoxide formation by LOX systems cannot be described by the traditional mechanism (Reactions (1)-(7)). There are various possibilities of superoxide formation during the oxidation of unsaturated compounds one of them is the decomposition of hydroperoxides to alkoxyl radicals. These radicals are able to rearrange into hydroxylalkyl radicals, which form unstable peroxyl radicals, capable of producing superoxide in the reaction with dioxygen. 

Antioxidant activity of flavonoids has already been shown about 40 years ago [90,91]. (Early data on antioxidant flavonoid activity are cited in Ref. [92].) Flavonoids are polyphenols, and therefore, their antioxidant activity depends on the reactivity of hydroxyl substituents in hydrogen atom abstraction reactions. As in the case of vitamins E and C, the most studied (and most important) reactions are the reactions with peroxyl radicals [14], hydroxyl radicals [15], and superoxide [16]. 

Since glutathione is synthesized in cells in relatively huge amounts, it is seldom applied as pharmacological antioxidant. Furthermore, the mechanism of its antioxidant activity is not so simple as that of vitamins E and C. The major reason is that the GS radical formed during scavenging of free radicals by GSH does not disappear by dimerization but participates in the chain reaction, producing superoxide (Reactions (20)-(23)). Furthermore, it has recently been shown that contrary to previous findings the rate constant for the reaction of GSH with superoxide is relatively small (200-1000 lmol-1 s-1) [211,223],... 

The absence of substituents with free radical scavenging properties in most of the (3-blockers makes doubtful their efficacy as powerful antioxidants. Arouma et al. [293] tested the antioxidative properties of several 3-blockers in reactions with superoxide, hydroxyl radicals, hydrogen peroxide, and hypochlorous acid. It was demonstrated that most of the compounds tested were inactive in these experiments. Nonetheless, propranolol, verapamil, and flunarizine effectively inhibited iron ascorbate-stimulated microsomal lipid peroxidation and all drugs (excluding flunarizine) were effective scavengers of hydroxyl radicals. Contrary to Janero et al. [292], these authors did not find the inhibition of xanthine oxidase by propranolol. It was concluded that 3-blockers are not the effective in vivo antioxidants. 

As hydroxyl or hydroxyl-like radicals are produced by the superoxide-driven Fenton reaction, superoxide overproduction must also occur in thalassemic cells. First, it has been shown by Grinberg et al. [382], who demonstrated that thalassemic erythrocytes produced the enhanced amount of superoxide in comparison with normal cells in the presence of prooxidant antimalarial drug primaquine. Later on, it has been found that the production of superoxide and free radical-mediated damage (measured through the MetHb/Hb ratio) was much higher in thalassemic erythrocytes even in the absence of prooxidants, although quinones (menadione, l,4-naphthoquinone-2-methyl-3-sulfonate) and primaquine further increased oxidative stress [383]. Overproduction of superoxide was also observed in thalassemic leukocytes [384]. 

Unfortunately, due to the above shortcomings of hydroxylamine derivatives as spin traps, the uncertainties of the mechanism of their reactions with superoxide are added. Although it is supposed that nitroxide radicals are formed by oxidation with superoxide (Reaction (6)), this reaction cannot be an elemental stage because superoxide cannot abstract a hydrogen atom. 

In addition to superoxide and hydroxyl radicals, luminol produces CL in the reaction with peroxynitrite [67], To discriminate between superoxide- and peroxynitrite-induced CL, the use of lucigenin-amplified CL has been recommended [68] because peroxynitrite does not interfere in this assay. Another way is to apply the inhibitors of peroxynitrite to distinguish between superoxide- and peroxynitrite-induced luminol CL. 

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