Mechanism quinones

The kinetics of proton-coupled electron transfer is an area that is ready for exploitation using redox couples attached to SAMs. There are sporadic reports of kinetic measurements on attached redox molecules with relatively complex two-electron, two-proton (2e2H) mechanisms quinones [127, 136, 149, 241, 242] and... 

Although the anionic polymerization mechanism is the predominant one for the cyanoacryhc esters, the monomer will polymerize free-radically under prolonged exposure to heat or light. To extend the usable shelf life, free-radical stabilizers such as quinones or hindered phenols are a necessary part of the adhesive formulation. 

Aromatic ethers and furans undergo alkoxylation by addition upon electrolysis in an alcohol containing a suitable electrolyte.Other compounds such as aromatic hydrocarbons, alkenes, A -alkyl amides, and ethers lead to alkoxylated products by substitution. Two mechanisms for these electrochemical alkoxylations are currently discussed. The first one consists of direct oxidation of the substrate to give the radical cation which reacts with the alcohol, followed by reoxidation of the intermediate radical and either alcoholysis or elimination of a proton to the final product. In the second mechanism the primary step is the oxidation of the alcoholate to give an alkoxyl radical which then reacts with the substrate, the consequent steps then being the same as above. The formation of quinone acetals in particular seems to proceed via the second mechanism. ... 

In the case of mechanism (6) there are materials available which completely prevent chain growth by reacting preferentially with free radicals formed to produce a stable product. These materials are known as inhibitors and include quinone, hydroquinone and tertiary butylcatechol. These materials are of particular value in preventing the premature polymerisation of monomer whilst in storage, or even during manufacture. 

In addition to the above possible mechanisms the possibility of reaction at w-positions should not be excluded. For example, it has been shown by Koebner that o- and p-cresols, ostensibly difunctional, can, under certain conditions, react with formaldehyde to give insoluble and infusible resins. Furthermore, Megson has shown that 2,4,6-trimethylphenol, in which the two ortho- and the one para-positions are blocked, can condense with formaldehyde under strongly acidic conditions. It is of interest to note that Redfam produced an infusible resin from 3,4,5,-trimethylphenol under alkaline conditions. Here the two m- and the p-positions were blocked and this experimental observation provides supplementary evidence that additional functionalities are developed during reaction, for example in the formation of quinone methides. 

Some other inhibitors from the patent literature include hydroquinone [129], ionoP [130], and quinone [131]. Other inhibitors used to stabilize MMA include butylated hydroxy toluene (BHT), phenothiazine, methylene blue, hydroxy-diphenylamine and di-/jc/<3-napthol [132]. Several good reviews of inhibition and inhibitors have been written [133-136]. The mechanisms of inhibition are subtle and complicated. For example, it has been reported that highly purified benzo-quinone acts as a retarder rather than an inhibitor [137]. It has been proposed... 

Scheme 10. Mechanislic possibililies for PF condensalion. Mechanism a involves an SN2-like attack of a phenolic ring on a methylol. This attack would be face-on. Such a mechanism is necessarily second-order. Mechanism b involves formation of a quinone methide intermediate and should be Hrst-order. The quinone methide should react with any nucleophile and should show ethers through both the phenolic and hydroxymethyl oxygens. Reaction c would not be likely in an alkaline solution and is probably illustrative of the mechanism for novolac condensation. The slow step should be formation of the benzyl carbocation. Therefore, this should be a first-order reaction also. Though carbocation formation responds to proton concentration, the effects of acidity will not usually be seen in the reaction kinetics in a given experiment because proton concentration will not vary.

The mechanism of this reaction has been studied by several groups [133,174-177]. The consensus is that interaction of ester with the phenolic resole leads to a quinone methide at relatively low temperature. The quinone methide then reacts rapidly leading to cure. Scheme 11 shows the mechanism that we believe is operative. This mechanism is also supported by the work of Lemon, Murray, and Conner. It is challenged by Pizzi et al. Murray has made the most complete study available in the literature [133]. Ester accelerators include cyclic esters (such as y-butyrolactone and propylene carbonate), aliphatic esters (especially methyl formate and triacetin), aromatic esters (phthalates) and phenolic-resin esters [178]. Carbamates give analogous results but may raise toxicity concerns not usually seen with esters. 

Scheme 11. Proposed quinone methide condensation mechanism. Work by Murray (and Lemon unpublished) showed clearly that the quinone methides formed from o-hydroxymethyl and not /7-hydroxymethyl groups in the presenee of ester.

At least two pathways have been proposed for the Nenitzescu reaction. The mechanism outlined below is generally accepted." Illustrated here is the indolization of the 1,4-benzoquinone (4) with ethyl 3-aminocrotonate (5). The mechanism consists of four stages (I) Michael addition of the carbon terminal of the enamine 5 to quinone 4 (II) Oxidation of the resulting hydroquinone 10 to the quinone 11 either by the starting quinone 4 or the quinonimmonium intermediate 13, which is generated at a later stage (HI) Cyclization of the quinone adduct 11, if in the cw-configuration, to the carbinolamine 12 or quinonimmonium intermediate 13 (IV) Reduction of the intermediates 12 or 13 to the 5-hydroxyindole 6 by the initial hydroquinone adduct 7 (or 8, 9,10). 

The requirement for reduction prior to DNA alkylation and crosslinking was first demonstrated by Iyer and Szybalski in 1964 [29], and can be induced both by chemical reducing agents such as sodium dithionite and thiols in vitro and by various reductive enzymes such as DT-diaphorase (NAD(P)H-quinone oxidoreduc-tase) in vitro and in vivo [47]. Much work to characterize the mechanism of reductive activation and alkylation has been carried out, principally by the Tomasz and Kohn groups, and Figure 11.1 illustrates a generally accepted pathway for mitomycin C [16, 48-50] based on these experiments, which is very similar to the mechanism originally proposed by Iyer and Szybalski [29]. 

There is a difference in the behavior of benzenediolatoborate and naphthalenedio-latoborate solutions on the one hand, and lithium bis[2,2 -biphenyldiolato(2-)-0,0 ] borate (point 5 in fig. 8) lithium bis[ sali-cylato (2-) Jborate (point 6) or benzene-diolatoborate/phenolate mixed solutions on the other (Fig.8). This can be tentatively explained by the assumption of different decomposition mechanisms due to different structures, which entail the formation of soluble colored quinones from benzenediolatoborate anions and lithium-ion conducting films from solutions of the latter compounds (points 5 and 6) [80], The assumption of a different mechanism and the formation of a lithium-ion conducting, electronically insulating film is supported by... 

The absolute rate constants for attack of carbon-centered radicals on p-benzoquinone (38) and other quinones have been determined to be in the range I0M08 M 1 s 1.1 -04 This rate shows a strong dependence on the electrophilicity of the attacking radical and there is some correlation between the efficiency of various quinones as inhibitors of polymerization and the redox potential of the quinone. The complexity of the mechanism means that the stoichiometry of inhibition by these compounds is often not straightforward. Measurements of moles of inhibitor consumed for each chain terminated for common inhibitors of this class give values in the range 0.05-2.0.176... 

The photolysis of arenediazonium salts has been widely used for intramolecular cyclizations in the synthesis of 1-phenylethylisoquinoline alkaloids by Kametani and Fukumoto (review 1972). An example is the photolysis of the diazonium ion 10.73, which resulted in the formation of O-benzylandrocymbine (10.74) (Kametani et al., 1971). The mechanism of this cyclization is obviously quite complex, since the carbon (as cation or radical ) to which the diazonio group is attached in 10.73 does not react with the aromatic CH group, but with the tertiary carbon (dot in 10.73), forming a quinone-like ring (10.74). In our opinion the methyl cation released is likely to react with the counter-ion X- or the solvent. 

The photolysis of o-quinone diazides was carefully investigated by Stis in 1944, many years before the development of photoresists. Scheme 10-102 shows the photolysis sequence for the diazoquinone 10.75 formed in the diazotization of 2-amino-1-naphthol. The product of the photolytic step is a ketocarbene (10.76), which undergoes a Wolff rearrangement to a ketene (10.77). In the presence of water in-dene-3-carboxylic acid (10.78) is formed this compound is highly soluble in water and can be removed in the development step. The mechanism given in Scheme 10-102 was not postulated as such by Stis, because in 1944 ketocarbenes were unknown (for a mechanistic discussion of such Wolff rearrangements see review by Zollinger, 1995, Sec. 8.6, and Andraos et al., 1994). 

In hydroxylation, quinones are usually obtained since the initial hydroxyl product is further oxidised. Kinetic studies on the hydroxylation of 1,3,5-tri-methoxybenzene with perbenzoic acid gave second-order rate coefficients (Table 29) which remained fairly constant for a wide variation in concentration of aromatic and acid thus indicating that the rate-determining step is bimolecular133. The variation was considered to be within the rather large experimental error for the reaction which was very fast and, therefore, studied at low temperature (—12.4 °C). Since more than one mole of acid per mole of aromatic was eventually consumed, the mechanism was formulated as... 

Many anodic oxidations involve an ECE pathway. For example, the neurotransmitter epinephrine can be oxidized to its quinone, which proceeds via cyclization to leukoadrenochrome. The latter can rapidly undergo electron transfer to form adrenochrome (5). The electrochemical oxidation of aniline is another classical example of an ECE pathway (6). The cation radical thus formed rapidly undergoes a dimerization reaction to yield an easily oxidized p-aminodiphenylamine product. Another example (of industrial relevance) is the reductive coupling of activated olefins to yield a radical anion, which reacts with the parent olefin to give a reducible dimer (7). If the chemical step is very fast (in comparison to the electron-transfer process), the system will behave as an EE mechanism (of two successive charge-transfer steps). Table 2-1 summarizes common electrochemical mechanisms involving coupled chemical reactions. Powerful cyclic voltammetric computational simulators, exploring the behavior of virtually any user-specific mechanism, have... 

The mechanisms for model condensation reactions of para-hydroxymethyl-substituted phenol (and therefore para-quinone methide) with reactive ortho positions are described in Fig. 7.29. The phenolate derivatives react with para-quinone... 

Resole resins are generally crosslinked under neutral conditions between 130 and 200° C or in the presence of an acid catalyst such as hydrochloric acid, phosphoric acid, p-toluenesulfonic acid, and phenolsulfonic acid under ambient conditions.3 The mechanisms for crosslinking under acidic conditions are similar to acid-catalyzed novolac formation. Quinone methides are the key reaction intermediates. Further condensation reactions in resole resin syntheses under basic conditions at elevated temperatures also lead to crosslinking. 

An important problem encountered with polymer electrodes is that of overoxidation. It occurs after reversible charging of the electrode at high oxidation potentials and leads to polymer degeneration. The results of thorough studies show that such degenerative mechanisms are promoted by the nucleophilicity of the solvent. Especially the activity of water leads to the formation of quinone-type compounds, to the cleavage of C—C bonds, the liberation of CO2, and the formation of carboxylic acids Hence, there is a clear tendency to avoid both nucleophile solvents... 

Aldehydes and ketones can also be converted to epoxides by treatment with a diazoalkane,most commonly diazomethane, but an important side reaction is the formation of an aldehyde or ketone with one more carbon than the starting compound (Reaction 18-9). The reaction can be carried out with many aldehydes, ketones, and quinones. A mechanism that accounts for both products is... 

Ordinary aldehydes and ketones can add to alkenes, under the influence of UV light, to give oxetanes. Quinones also react to give spirocyclic oxetanes. This reaction, called the Patemo-BUchi reaction,is similar to the photochemical dimerization of alkenes discussed at 15-61.In general, the mechanism consists of the addition of an excited state of the carbonyl compound to the ground state of the alkene. Both singlet (5i) and n,n triplet states have been shown to add to... 

Quinones, which become reduced to the corresponding hydroquinones. Two important quinones often used for aromatizations are chloranil (2,3,5,6-tetrachloro-1,4-benzoquinone) and DDQ (2,3-dichloro-5,6-dicyano-l,4-ben-zoquinone). The latter is more reactive and can be used in cases where the substrate is difficult to dehydrogenate. It is likely that the mechanism involves a transfer of hydride to the quinone oxygen, followed by the transfer of a proton to the phenolate ion °... 

Less is known about the mechanism than is the case for 19-3, but, as in that it seems to vary with the oxidizing agent. For oxidation of catechol with NaI04, it was found that the reaction conducted in H2 0 gave unlabeled quinone, " so the following mechanismwas proposed ... 

The reaction mechanism has not been elucidated the ammonium monovanadate presumably oxidizes the phenols to quinones, that then react with />-anisidine to form quinonimines. 

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