Oxidative activation reaction scheme

Using 9-fluorenone as the radical initiator for the generation of benzylic radical, monoflnorination was found occur with both electron-rich and electron deficient substrates providing the desired product in good-to-exceUent yield (Scheme 9.28). Sanford also found the 8-methylquinoline will undergo facile quinoline-directed C—H activation at Pd(II) to generate a 5-benzyl Pd species and to serve as an excellent snbstrate for the related Pd-catalyzed C—H activation/oxidative functionalization reactions (Scheme 9.29). ... 

Polymerization Initiator. Some unsaturated monomers can be polymerized through the aid of free radicals generated, as transient intermediates, in the course of a redox reaction. The electron-transfer step during the redox process causes the scission of an intermediate to produce an active free radical. The ceric ion, Ce" ", is a strong one-electron oxidizing agent that can readily initiate the redox polymerization of, for example, vinyl monomers in aqueous media at near ambient temperatures (40). The reaction scheme is... 

In the direct coupling reaction (Scheme 30), it is presumed that a coordinatively unsaturated 14-electron palladium(o) complex such as bis(triphenylphosphine)palladium(o) serves as the catalytically active species. An oxidative addition of the organic electrophile, RX, to the palladium catalyst generates a 16-electron palladium(n) complex A, which then participates in a transmetalation with the organotin reagent (see A—>B). After facile trans- cis isomerization (see B— C), a reductive elimination releases the primary organic product D and regenerates the catalytically active palladium ) complex. 

In contrast, Cozzi and Umani-Ronchi found the (salen)Cr-Cl complex 2 to be very effective for the desymmetrization of meso-slilbene oxide with use of substituted indoles as nucleophiles (Scheme 7.25) [49]. The reaction is high-yielding, highly enantioselective, and takes place exclusively at sp2-hybridized C3, independently of the indole substitution pattern at positions 1 and 2. The successful use of N-alkyl substrates (Scheme 7.25, entries 2 and 4) suggests that nucleophile activation does not occur in this reaction, in stark contrast with the highly enantioselective cooperative bimetallic mechanism of the (salen)Cr-Cl-catalyzed asymmetric azidolysis reaction (Scheme 7.5). However, no kinetic studies on this reaction were reported. 

The reaction scheme is as follows (Fig. 21). It is reasonable to assume that BTMA Br3 can be dissociated by water as shown in Equation 1. The resulting hypobromous acid may act as the major active oxidizing species and may convert alcohols into esters as Equation 2. In the case of ethers, we can show as Equation 4. Generated hydrobromic acid can be removed by Na2HP04 which has been added previously (Eqn. 5). 

Reduced nicotinamide-adenine dinucleotide (NADH) plays a vital role in the reduction of oxygen in the respiratory chain [139]. The biological activity of NADH and oxidized nicotinamideadenine dinucleotide (NAD ) is based on the ability of the nicotinamide group to undergo reversible oxidation-reduction reactions, where a hydride equivalent transfers between a pyridine nucleus in the coenzymes and a substrate (Scheme 29a). The prototype of the reaction is formulated by a simple process where a hydride equivalent transfers from an allylic position to an unsaturated bond (Scheme 29b). No bonds form between the n bonds where electrons delocalize or where the frontier orbitals localize. The simplified formula can be compared with the ene reaction of propene (Scheme 29c), where a bond forms between the n bonds. 

The reactions of TTN with a variety of unsaturated systems have been studied systematically during the last two years, and the results obtained clearly establish the synthetic utility of the reagent as a specific oxidant. Attempts were made in 1966 by Uemura et al. 162) to oxidize a,)8-unsatur-ated carbonyl compounds with thallium(III) acetate, but were unsuccessful. In 1970, however, Ollis and his co-workers 121-123) reported that prolonged treatment of highly activated chalcones (Scheme 20) with thal-... 

In the oxidation of methanol to CO2, six electrons ate involved. This high number of electrons implies that the mechanism is inevitably very complex, with several intermediate species participating in the mechanism. In spite of its complexity, it has been proposed that the oxidation mechanism follows the same general scheme as the oxidation of formic acid, i.e., a dual path mechanism with active and poisoning intermediates (see the reaction Scheme 6.16) [Parsons and VanderNoot, 1988]. For that reason, we will compare the behavior with that of formic acid to highlight the similarities and differences. 

In the original proposal of the dual-pathway mechanism (for formic acid oxidation, see [Capon and Parsons, 1973a, b, c] for methanol oxidation, see [Parsons and VanderNoot, 1988 Jarvi and Stuve, 1998 Leung and Weaver, 1990 Lopes et al., 1991 Herrero et al., 1994, 1995]), both pathways lead to CO2 as the final product, as illustrated in the reaction scheme depicted in Fig. 13.8a [Jarvi and Smve, 1998]. In this mechanism, desorption of incomplete oxidation products was not included. The existence of a direct reaction pathway for methanol oxidation, following the dual-pathway mechanism, was justified by the observation of a methanol oxidation current at potentials where COad oxidation is not yet active [Sriramulu et al., 1998, 1999 Herrero et al., 1994, 1995]. The validity of this interpretation was questioned, however, by Vielstich and Xia (1995), who claimed that CO2 formation is observed only with the onset of COad oxidation and that the faradaic current measured at lower potentials is due to the formation of the incomplete oxidation products formaldehyde and formic acid. The latter findings were later confirmed by Wang et al. [2001], Korzeniewski and Childers [1998], and Jusys et al. [2001, 2003]. In more... 

Transition metal centered bond activation reactions for obvious reasons require metal complexes ML, with an electron count below 18 ("electronic unsaturation") and with at least one open coordination site. Reactive 16-electron intermediates are often formed in situ by some form of (thermal, photochemical, electrochemical, etc.) ligand dissociation process, allowing a potential substrate to enter the coordination sphere and to become subject to a metal mediated transformation. The term "bond activation" as often here simply refers to an oxidative addition of a C-X bond to the metal atom as displayed for I and 2 in Scheme 1. 

Allenes add nitrile oxides either to one or two double bonds. For mono- and 1,1-disubstituted allenes, relative activity of the two bonds depends on the nature of substituents. The reaction (Scheme 1.18) of N-propadienylanilines 54 with 3,5-dichloro-2,4,6-trimethylbenzonitrile oxide proceeds site- and regioselectively to give 5-substituted 4-methylene-4,5-dihydroisoxazoles 55, which add a second molecule of nitrile oxide to afford 4,5/-spirobi-(4,5-dihydroisoxazoles) 56. Dihy-droisoxazoles 55 isomerize to 4-(2-aminobenzyl)isoxazoles 57 via a Claisen-type rearrangement (224). 

Indicine IV-oxide (169) (Scheme 36) is a clinically important pyrrolizidine alkaloid being used in the treatment of neoplasms. The compound is an attractive drug candidate because it does not have the acute toxicity observed in other pyrrolizidine alkaloids. Indicine IV-oxide apparently demonstrates increased biological activity and toxicity after reduction to the tertiary amine. Duffel and Gillespie (90) demonstrated that horseradish peroxidase catalyzes the reduction of indicine IV-oxide to indicine in an anaerobic reaction requiring a reduced pyridine nucleotide (either NADH or NADPH) and a flavin coenzyme (FMN or FAD). Rat liver microsomes and the 100,000 x g supernatant fraction also catalyze the reduction of the IV-oxide, and cofactor requirements and inhibition characteristics with these enzyme systems are similar to those exhibited by horseradish peroxidase. Sodium azide inhibited the TV-oxide reduction reaction, while aminotriazole did not. With rat liver microsomes, IV-octylamine decreased... 

Tetrahydropyrrolo[l,4]oxazine 74, obtained by photoinduced electron-transfer (PET) oxidative activation of substituted prolinol, undergoes nucleophilic substitution of the OH at position C-3 with allyltrimethylsilane in the presence of TiCU (Scheme 8). The reaction was highly stereoselective and produced, after hydrolysis of the resultant amide 75, optically active a-hydroxy acid 76 together with the auxiliary (.S )-prolinol that can be effectively recycled <1998TL7153>. 

We were interested in the behaviour of polymeric catalysts in order to confirm that typical polymer effects may occur. Oxidative coupling of 2,6-disubstituted phenols, as developped by Hay (7), was chosen as a model reaction and the catalytic activities of coordination complexes of copper with several polymeric tertiary amines were compared with the activities of their low molecular weight analogs. The overall reaction scheme is presented in scheme 1. 

Diarylamides with arenes activated by electron-donating substituents can be converted to azacycles by anodic oxidation through phenolic oxidative coupling reactions that can be a key step in the synthesis of alkaloids (Schemes 16 and 17). According to the nature of substituents and the experimental conditions, either spiro compounds [22] or non-spiro compounds [23, 24] were obtained. 

In a related set of experiments, Nishiguchi and coworkers studied oxidative cyclization reactions that were initiated by the addition of radicals derived from the oxidation of an activated methylene group to an olefin (Scheme 12) [25]. 

The fact that complex 38 does not react further - that is, it does not oxidatively add the N—H bond - is due to the comparatively low electron density present on the Ir center. However, in the presence of more electron-rich phosphines an adduct similar to 38 may be observed in situ by NMR (see Section 6.5.3 see also below), but then readily activates N—H or C—H bonds. Amine coordination to an electron-rich Ir(I) center further augments its electron density and thus its propensity to oxidative addition reactions. Not only accessible N—H bonds are therefore readily activated but also C—H bonds [32] (cf. cyclo-metallations in Equation 6.14 and Scheme 6.10 below). This latter activation is a possible side reaction and mode of catalyst deactivation in OHA reactions that follow the CMM mechanism. Phosphine-free cationic Ir(I)-amine complexes were also shown to be quite reactive towards C—H bonds [30aj. The stable Ir-ammonia complex 39, which was isolated and structurally characterized by Hartwig and coworkers (Figure 6.7) [33], is accessible either by thermally induced reductive elimination of the corresponding Ir(III)-amido-hydrido precursor or by an acid-base reaction between the 14-electron Ir(I) intermediate 53 and ammonia (see Scheme 6.9). 

Until now, for most of the systems described here it has been accepted that alkane activation occurred through oxidative addition to the 14-electron intermediate complexes. Yet, Belli and Jensen [26] showed, for the first time, evidence for an alternative reaction path for the catalytic dehydrogenation of COA with complex [lrClH2(P Pr3)2] (22) which invoked an Ir(V) species. Catalytic and labeling experiments led these authors to propose an active mechanism (Scheme 13.12), on the basis of which they concluded that the dehydrogenation of COA by compound 22 did not involve an intermediate 14-electron complex [17-21], but rather the association of COA to an intermediate alkyl-hydride complex (Scheme 13.12). 

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