Peroxynitrite free radical

Nitric oxide, which is produced from arginine in the reaction catalysed by nitric oxide synthase, reacts with O2 to produce the very toxic peroxynitrite free radical (Figure 17.27). 

W. H. Koppenol, The Basic Chemistry of Nitrogen Monoxide and Peroxynitrite. Free Radic Biol. 3/et/2S (1998) 385-91. 

W.H. Koppenol, The basic chemistry of nitrogen monoxide and peroxynitrite. Free Radical Biol. Med., 25 (1998) 385. 

Not all oxidants formed biolc cally have the potential to promote lipid peroxidation. The free radicals superoxide and nitric oxide [or endothelium-derived relaxing aor (EDRF)] are known to be formed in ww but are not able to initiate the peroxidation of lipids (Moncada et tU., 1991). The protonated form of the superoxide radical, the hydroperoxy radical, is capable of initiating lipid peroxidation but its low pili of 4.5 effectively precludes a major contribution under most physiological conditions, although this has been suggested (Aikens and Dix, 1991). Interestingly, the reaction product between nitric oxide and superoxide forms the powerful oxidant peroxynitrite (Equation 2.6) at a rate that is essentially difiiision controlled (Beckman eta/., 1990 Huie and Padmaja, 1993). 

Protein tyrosine residues constitute key targets for peroxynitrite-mediated nitrations. Attack of various free radicals (ONOO-, N02 ) upon tyrosine generates 3-nitrotyrosine, which can be measured immunologically or by GC/MS or HPLC techniques. The detection of 3-nitrotyrosine was considered a biomarker of peroxynitrite action in vivo. Similarly, attack of HOC1 and HOBr on tyrosine generates chlorotyro-sine and bromotyrosine, respectively, both of which are measured most accurately by GC-MS. 

Kooy NW, Royall JA, Ischiropoulos H and Beckma JS. 1994. Peroxynitrite-mediated oxidation of dihy-drorhodamine 123. Free Radic Biol Med 16(2) 149-156. 

Pannala A, Razaq R, Halliwell B, Singh S and Rice-Evans CA. 1998. Inhibition of peroxynitrite dependent tyrosine nitration by hydroxycinnamates nitration or electron donation Free Radic Biol Med 24(4) 594-606. 

Santos MR and Mira L. 2004. Protection by flavonoids against the peroxynitrite-mediated oxidation of dihydrorhodamine. Free Radic Res 38(9) 1011-1018. 

This mode of superoxide-dependent free radical-mediated damaging activity remains an important one although the nature of the generated reactive species (free hydroxyl radicals or perferryl, or ferryl ions) is still obscure. However, after the discovery of the fact that many cells produce nitric oxide in relatively large amounts (see below), it became clear that there is another and possibly a more portent mechanism of superoxide-induced free radical damage, namely, the formation of highly reactive peroxynitrite. 

Reaction of nitric oxide with superoxide is undoubtedly the most important reaction of nitric oxide, resulting in the formation of peroxynitrite, one of the main reactive species in free radical-mediated damaging processes. This reaction is a diffusion-controlled one, with the rate constant (which has been measured by many workers, see, for example, Ref. [41]), of about 2 x 109 1 mol-1 s-1. Goldstein and Czapski [41] also measured the rate constant for Reaction (11) ... 

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. 

On the other hand, in accord with the free radical mechanism peroxynitrite is dissociated into free radicals, which are supposed to be genuine reactive species. Although free radical mechanism was proposed as early as in 1970 [111], for some time it was not considered to be a reliable one because a great confusion ensued during the next two decades because of misinterpretations of inconclusive experiments, sometimes stimulated by improper thermodynamic estimations [85]. The latest experimental data supported its reliability [107-109]. Among them, the formation of dityrosine in the reaction with tyrosine and 15N chemically induced dynamic nuclear polarization (CIDNP) in the NMR spectra of the products of peroxynitrite reactions are probably the most convincing evidences (see below). 

Probably, the most convincing proof of free radical mechanism of peroxynitrite reactions is the formation of dityrosine [117,118]. It has been suggested [118] that the nitric dioxide radical is responsible for the formation of both 3-nitrotyrosine and dityrosine (Figure 21.1), however, hydroxyl radicals (which were identified in this system by ESR spectroscopy [119]) may also participate in this process. Pfeiffer et al. [118] proposed that dityrosine is predominantly formed at low fluxes of superoxide and nitric oxide, which corresponds to in vivo conditions, however, this observation was not confirmed by Sawa et al. [117],... 

Peroxynitrite reacts with heme proteins such as prostacycline synthase (PGI2), microperoxidase, and the heme thiolate protein P450 to form a ferryl nitrogen dioxide complex as an intermediate [120]. Peroxynitrite also reacts with acetaldehyde with the rate constant of 680 1 mol 1 s" 1 forming a hypothetical adduct, which is decomposed into acetate, formate, and methyl radicals [121]. The oxidation of NADH and NADPH by peroxynitrite most certainly occurs by free radical mechanism [122,123], Kirsch and de Groot [122] concluded that peroxynitrite oxidized NADH by a one-electron transfer mechanism to form NAD and superoxide ... 

The reaction of peroxynitrite with the biologically ubiquitous C02 is of special interest due to the presence of both compounds in living organisms therefore, we may be confident that this process takes place under in vivo conditions. After the discovery of this reaction in 1995 by Lymar [136], the interaction of peroxynitrite with carbon dioxide and the reactions of the formed adduct nitrosoperoxocarboxylate ONOOCOO has been thoroughly studied. In 1996, Lymar et al. [137] have shown that this adduct is more reactive than peroxynitrite in the reaction with tyrosine, forming similar to peroxynitrite dityrosine and 3-nitrotyrosine. Experimental data were in quantitative agreement with free radical-mediated mechanism yielding tyrosyl and nitric dioxide radicals as intermediates and were inconsistent with electrophilic mechanism. The lifetime of ONOOCOO was estimated as <3 ms, and the rate constant of Reaction (42) k42 = 2 x 103 1 mol 1 s 1. 

Other very convincing evidences for free radical-mediated mechanism of decomposition and reactions of peroxynitrite and nitrosoperoxocarboxylate were demonstrated by Lehnig [140] with the use of CIDNP technique. This technique is based on the effects observed exclusively for the products of free radical reactions their NMR spectra exhibit emission characterizing a radical pathway of their formation. Lehnig has found the enhanced emission in the 15N NMR spectra of N03- formed during the decomposition of both peroxynitrite and nitrosoperoxocarboxylate. This fact indicates that N03- was formed from radical pairs [ N02, H0 ] and [ N02, C03 ]. Emission was also observed in the reaction of both nitrogen compounds with tyrosine supposedly due to the formation of radical pair [ N02, tyrosyl ]. 

Simultaneous generation of nitric oxide and superoxide by NO synthases results in the formation of peroxynitrite. As the reaction between these free radicals proceeds with a diffusion-controlled rate (Chapter 21), it is surprising that it is possible to detect experimentally both superoxide and NO during NO synthase catalysis. However, Pou et al. [147] pointed out that the reason is the fact that superoxide and nitric oxide are generated consecutively at the same heme iron site. Therefore, after superoxide production NO synthase must cycle twice before NO production. Correspondingly, there is enough time for superoxide to diffuse from the enzyme and react with other biomolecules. 

In addition to nitric oxide, superoxide, and peroxynitrite, NO synthases are able to generate secondary free radicals because similar to cytochrome P-450 reductase, the reductase domain can transfer an electron from the heme to a xenobiotic. Thus it has been found [158,159] that neuronal NO synthase NOS I catalyzed the formation of CH3CH(OH) radical from ethanol. It was suggested that the perferryl complex of NOS I is responsible for the formation of such secondary radicals. Miller [160] also demonstrated that 1,3-dinitrobenzene mediated the formation of superoxide by nNOS. It was proposed that the enhancement of superoxide production in the presence of 1,3-dinitrobenzene converted nNOS into peroxynitrite-produced synthase and may be a mechanism of neurotoxicity of certain nitro compounds. 

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 ... 

It should be noted that Reaction (4) is not a one-stage process.) Both free radical N02 and highly reactive peroxynitrite are the initiators of lipid peroxidation although the elementary stages of initiation by these compounds are not fully understood. (Crow et al. [45] suggested that trans-ONOO is protonated into trans peroxynitrous acid, which is isomerized into the unstable cis form. The latter is easily decomposed to form hydroxyl radical.) Another possible mechanism of prooxidant activity of nitric oxide is the modification of unsaturated fatty acids and lipids through the formation of active nitrated lipid derivatives. 

Thus, physiological free radicals superoxide and nitric oxide produced by phagocytes and nonphagocytes are responsible for the two major pathways of LDL oxidation transition metal-dependent and peroxynitrite-dependent mechanisms. However, there is another mode... 

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