Vitamin cobalt porphyrin

Cobaloxime(I) generated by the electrochemical reductions of cobaloxime(III), the most simple model of vitamin Bi2, has been shown to catalyze radical cyclization of bromoacetals.307 Cobalt(I) species electrogenerated from [ConTPP] also catalyze the reductive cleavage of alkyl halides. This catalyst is much less stable than vitamin Bi2 derivatives.296 It has, however, been applied in the carboxylation of benzyl chloride and butyl halides with C02.308 Heterogeneous catalysis of organohalides reduction has also been studied at cobalt porphyrin-film modified electrodes,275,3 9-311 which have potential application in the electrochemical sensing of pollutants. 

Despite the similarities existing among natural tetrapyrrolic macrocycles, e.g. they are all tetradentate equatorial N4 ligands, structural variations cause a fine modulation of the reactivity of the central metal atom. Thus it is most probably the corrin skeleton that enables the cobalt atom of vitamin B12 to carry out reactions impossible for a similar cobalt porphyrinate. 

The incorporation of vitamin B12 derivatives into plasticized poly(vinyl chloride) membranes has resulted in the development of several ion-selective electrodes (ISEs). The response of the electrodes has been related to principles of molecular recognition chemistry. In addition, ISEs have been prepared by electropolymerization of a cobalt porphyrin. These electrodes have selectivity properties that are controlled by both the intrinsic selectivity of the metalloporphyrin and the characteristics of the polymer film (e.g., pore size). 

In this paper, we report the development of ISEs that have been designed by using molecular recognition principles. Specific examples include the development of polymer membrane anion-selective electrodes based on hydrophobic vitamin B12 derivatives and a cobalt porphyrin. The selectivity patterns observed with these electrodes can be related to differences in the structure of the various ionophores, and to properties of the polymer film. 

In summary, it has been demonstrated that ISEs can be designed by employing molecular recognition principles. In particular, the feasibility of using hydrophobic vitamin B12 derivatives and electropolymerized porphyrin films in the development of polymer membrane anion-selective electrodes has been demonstrated. The studies indicated that the changes in the selectivity of these ISEs can be explained by the difference in structure of the ionophores. In addition, it was shown that by electropolymerization of a cobalt porphyrin, anion-selective electrodes can be prepared that have extended lifetimes compared with PVC-based ISEs, which use a similar compound as the ionophore. 

The cobalt porphyrins deserve special interest because of their biological relevance to vitamin Bi2 chemistry, their capacity to bind oxygen reversibly and their catalytic activities in various redox reactions of the axial ligands. Both the latter aspects will be included in the following descriptions. 

Electrocatalytic reductive coupling of aryl chlorides to afford biphenyls can be accomplished with dichloro(l,2-bis(di-propylphosphino)benzene)nickel(II) in yields as high as 96% with 2 mol % of the catalyst in polar, coordinating solvents (55). Similar couplings can also be achieved with nickel-2,2 -bipyridyl and Pd(PPh3)2Cl2 as catalysts (56, 57). Indirect electrochemical reduction of vicinal dibromides to alkenes occurs efficiently with iron and cobalt porphyrins as mediators (58). Vitamin B12 is a mediator for the indirect electrochemical reduction of a-halo acids (59). 

Cobalt porphyrin complexes are often employed as synthetic models for vitamin Bj2 because of their ease of synthesis and the ability to obtain unambiguous structural and spectroscopic data. Some of the (por)Co complexes themselves are known to play important roles in the activation and reduction of NO. For example, [(2-TMPPyP)Co] (1 9j and (TPP)Co supported on TiO2(190,191) have been used as catalyst for the reduction of NO. 

Bi2 Models. A series of models of vitamin B12 (1) and of its organometallic derivatives 2 and 3 have been developed and used, such as Schrauzer s cobaloximes (such as 14), the Costa complexes (such as 15+) (Fig. 10), and various cobalt-porphyrinates (15,17,46,47). In other studies, the cobinamides 8+ and 9+, the B12 derivatives cobester (13), methyl-cobester (Co -methyl-heptamethylcobyrinate, 16), and other lipophilic analogs were used (45). Such... 

The structure of the diamagnetic, cherry-red vitamin B12 is shown in Fig. 26.6 and it can be seen that the coordination sphere of the cobalt has many similarities with that of iron in haem (see Fig. 25.7). In both cases the metal is coordinated to 4 nitrogen atoms of an unsaturated macrocycle (in this case part of a corrin ring which is less symmetrical and not so unsaturated as the porphyrin in haem) with an imidazole nitrogen in the fifth position. A major... 

In comparison to the porphyrins, the corrin nucleus contains one less atom in its innermost ring (that is, it contains a 15-membered ring) and, on coordination, only one NH proton is lost to give the macrocycle a single negative charge. A cobalt corrin complex occurs as part of the structure of vitamin B12. 

Like many vitamins, cobalamin is functionally active as a derived coenzyme, coenzyme B12. Structurally, this is composed of a corrin ring a haem-like porphyrin ring containing cobalt (Co3+) at the centre held by four coordination bonds. The fifth... 

The structure of cobalamin is more complex than that of folic acid (Figure 15.2 and 15.3). At its heart is a porphyrin ring containing the metal ion cobalt at its centre. In catalytic reactions the cobalt ion forms a bond with the one-carbon group, which is then transferred from one compound to another. Vitamin B12 is the prosthetic group of only two enzymes, methylmalonyl-CoAmutase and methionine synthase. The latter enzyme is particularly important, as it is essential for the synthesis of nucleotides which indicates the importance of vitamin B12 in maintenance of good health. 

Cobalt complexes with square planar tetradentate ligands, including salen, cor-rin, and porphyrin types, all catalyse the reduction of alkyl bromides and iodides. Most preparative and mechanistic work with these reactions has used cobalamines, including vitamin-B,. A generalised catalytic cycle is depicted in Scheme 4.10 [219]. At potentials around -0.9 V vs. see, the parent ligated Co(lll) compound un-... 

According to [96], electrochemical methods, especially the application of cyclic voltammetry, could be a powerful tool to find suitable catalysts for NO removal from combustion products. Investigation of electrocatalytic properties of vitamin B12 toward oxidation and reduction of nitric oxide was reported in [97]. The catalytic activity of meso-tetraphenyl-porphyrin cobalt for nitric oxide oxidation in methanolic solution and in Nafion film was reported in [98]. 

Vitamin B12 consists of a porphyrin-like ring with a central cobalt atom attached to a nucleotide. Various organic groups may be covalently bound to the cobalt atom, forming different cobalamins. Deoxyadenosylcobalamin and methylcobalamin are the active forms of the vitamin in humans. Cyanocobalamin and hydroxocobalamin (both available for therapeutic use) and other cobalamins found in food sources are converted to the active forms. The ultimate source of vitamin Bi2 is from microbial synthesis the vitamin is not synthesized by animals or plants. The chief dietary source of vitamin Bi2 is microbially derived vitamin B12 in meat (especially liver), eggs, and dairy products. Vitamin Bi2 is sometimes called extrinsic factor to differentiate it from intrinsic factor, a protein normally secreted by the stomach that is required for gastrointestinal uptake of dietary vitamin B12. 

Vitamin B12 consists of a porphyrin-like ring structure, with an atom of Co chelated at its centre, linked to a nucleotide base, ribose and phosphoric acid (6.34). A number of different groups can be attached to the free ligand site on the cobalt. Cyanocobalamin has -CN at this position and is the commercial and therapeutic form of the vitamin, although the principal dietary forms of B12 are 5 -deoxyadenosylcobalamin (with 5 -deoxyadeno-sine at the R position), methylcobalamin (-CH3) and hydroxocobalamin (-OH). Vitamin B12 acts as a co-factor for methionine synthetase and methylmalonyl CoA mutase. The former enzyme catalyses the transfer of the methyl group of 5-methyl-H4 folate to cobalamin and thence to homocysteine, forming methionine. Methylmalonyl CoA mutase catalyses the conversion of methylmalonyl CoA to succinyl CoA in the mitochondrion. 

Coenzyme B12 is the cofactor form of vitamin B 2, which is unique among all the vitamins in that it contains not only a complex organic molecule but an essential trace element, cobalt. The complex corrin ring system of vitamin B12 (colored blue in Fig. 2), to which cobalt (as Co3+) is coordinated, is chemically related to the porphyrin ring system of heme and heme proteins (see Fig. 5-1). A fifth coordination position of cobalt is filled by dimethylbenzimidazole ribonucleotide (shaded yellow), bound covalently by its 3 -phosphate group to a side chain of the corrin ring, through aminoisopropanol. 

Several macrocyclic ligands are shown in Figure 2. The porphyrin and corrin ring systems are well known, the latter for the cobalt-containing vitamin Bi2 coenzymes. Of more recent interest are the hydroporphyrins. Siroheme (an isobacteriochlorin) is the prosthetic group of the sulfite and nitrite reductases which catalyze the six-electron reductions of sulfite and nitrite to H2S and NH3 respectively. The demetallated form of siroheme, sirohydrochlorin, is an intermediate in the biosynthesis of vitamin Bi2, and so links the porphyrin and corrin macrocycles. Factor 430 is a tetrahydroporphyrin, and as its nickel complex is the prosthetic group of methyl coenzyme M reductase. F430 shows structural similarities to both siroheme and corrin. 

The structures of the biologically active forms of B12 were solved relatively recently (1961) (78) and were shown to contain a cobalt atom surrounded by a corrin ring as shown in Fig. 16 (80). The crystal structure also showed a cobalt-carbon a bond which was quite surprising since the few compounds with cobalt-carbon a- bonds known at that time were quite unstable (79). The corrin ring is similar to the porphyrin ring, but its greater saturation imports less rigidity than the porphyrin. Corrinoids with the axial 5,6-dimethylbenzimidazole substituent are called cobalamins. Vitamin B12 with Co(III) and CN in the top axial position is... 

If our postulates are correct the most interesting feature of P-450 is the manner in which the protein has adjusted the coordination geometry of the iron and then provided near-neighbour reactive groups to take advantage of the activation generated by the curious coordination. Vallee and Williams (68) have observed this situation in zinc, copper and iron enzymes and referred to it as an entatic state of the protein. It is also apparent that some such adjustment of the coordination of cobalt occurs in the vitamin B12 dependent enzymes. As a final example we have looked at the absorption spectra of chlorophyll for its spectrum is in many respects very like that of a metal-porphyrin. This last note is intended to stress the features of chlorophyll chemistry which parallel those of P-450. 

With the name corrinoid we will refer to a class of compounds which have a molecular skeleton similar to that of the cobalt complex present in Vitamin B12 of which the main characteristics are the direct link between two pyrroles and the fully saturated p positions. These major features afford a macrocycle which is more contracted than a porphyrin and without an aromatic n system. 

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