Cob(I)alamin as Catalyst. 8th Communication. Cob(I)alamin and Heptamethyl Cob(I)yrinate During the Reduction of α,β-Unsaturated Carbonyl Derivatives

Hydrogen bonds as presented in Figure 2 cannot account for the enantioselective attack of cob(I)alamin ( 4 ( I )) or heptamethyl cob(I)yrinate ( 5 ( I )) on one of the two enantiotopic faces of the substrates. The attack of the strongly nucleophilic 3d orbital is preferentially directed to the re-side of the starting materials with (Z)-configuration and leads, after the highly stereoselective reductive cleavage of the Co, C bond, to saturated products with (S)-configuration in varying enantiomeric excesses (see Schemes 1, 3 and Table 1).     

Cob(I)alamin Differentiating Alkenes During Saturation

The olefins 2, 7, 11 , and 19 , have been reduced using catalytic amounts of cob(I)alamin( I(I) ). During a slow saturation, the catalyst is able to differentiate the two diastereotopic faces of the endocyclic double bonds in 11 (t_1/2 4 h,. cf. Scheme 3) are reduced much faster. A rationalization of the data can be obtained formulating tertiary alkylcobalamins as intermediates. Of the oxime 6 (cf. Scheme 2) and the p- bromobenzoate 23 (cf. Scheme 5) the structures have been determined by X-ray analysis.     

Oxidative Cyclopropanol Opening by Cob(III)alamin

Starting from the cyclopropanol 2 , the isomeric cyclopropanol 4 and the β, γ-unsasturated aldehydes 7 and 8 have been produced by a cobalamin-dependant transformation. In traces, the two acetoxycyclopropanes 3 and 6 , the saturated aldehydes 5 and 11 and the β,γ-unsaturated aldehyde 9 could be detected (cf. Structural Formulae and Table). Starting from 4 the same products in a rather similar distribution were obtained. The isomerization 2?4 as well as the transformations leading to 7,8 , and 9 are shown to be mediated by cob(III)alamin (1(III)) . The results are explained on the basis of rearranging Co-complexes. The migrations might be driven by the electrophilic nature of the central Co(d⁶)-atom.     

Electrofugal Fragmentation of Alkylcobalamin Derivatives Using Cob(I)Alamin and Heptamethyl Cob (I)yrinate as Catalysts

The cob (I)alamin- ( 1(I) ) and the heptamethyl cob(I)ynnate- ( 2(I) ) catalyzed transformation of an epoxide to the corresponding saturated hydrocarbon 3→4→5 is examined (see Schemes 1 and 3–5). Under the reaction conditions, the epoxyalkyl acetate 3 is opened by the catalysts with formation of appropriate (b?-hydroxyalkyl)-corrinoid derivatives ( 13 , 14 , 17 , 18 , see Schemes 12 and 14). Triggered by a transfer of electrons to the Co-corrin-π system, the Co, C-bond of the intermediates is broken, generating the alkenyl acetate 4 (cf. Schemes 12 and 14) following an electrofugal fragmentation (cf. Schemes 2 and 12). The double bond of 4 is also attacked by the catalysts, leading to the corresponding alkylcorrinoids ( 15 , 19 , see Schemes 12 and 14) which in turn are reduced by electrons from metallic zinc, the electron source in the system, inducing a reductive cleavage of the Co, C-bond with production of the saturated monoacetate 5 (see Schemes 2, 5 and 12). In the cascade of steps involved, the transfer of electrons to the intermediate alkylcorrinoids ( 13–15 , 17–19 , see Schemes 12 and 14) is shown to be rate-limiting. Comparing the two catalytic species 1(I) and 2(I) , it is shown that the ribonucleotide loop protects intermediate alkylcobalamins to some extent from an attack by electrons. The protective function of the ribonucleotide side-chain is shown to be present in alkylcobalamins existing in the base-on form (cf. Chap. 4 and see Scheme 14).     

Stabilisation of Methylene Radicals by Cob(II)alamin in Coenzyme B12 Dependent Mutases

Coenzyme B₁₂ initiates radical chemistry in two types of enzymatic reactions, the irreversible eliminases (e.g., diol dehydratases) and the reversible mutases (e.g., methylmalonyl‐CoA mutase). Whereas eliminases that use radical generators other than coenzyme B₁₂ are known, no alternative coenzyme B₁₂ independent mutases have been detected for substrates in which a methyl group is reversibly converted to a methylene radical. We predict that such mutases do not exist. However, coenzyme B₁₂ independent pathways have been detected that circumvent the need for glutamate, β‐lysine or methylmalonyl‐CoA mutases by proceeding via different intermediates. In humans the methylcitrate cycle, which is ostensibly an alternative to the coenzyme B₁₂ dependent methylmalonyl‐CoA pathway for propionate oxidation, is not used because it would interfere with the Krebs cycle and thereby compromise the high‐energy requirement of the nervous system. In the diol dehydratases the 5′‐deoxyadenosyl radical generated by homolysis of the carbon–cobalt bond of coenzyme B₁₂ moves about 10 Å away from the cobalt atom in cob(II )alamin. The substrate and product radicals are generated at a similar distance from cob(II )alamin, which acts solely as spectator of the catalysis. In glutamate and methylmalonyl‐CoA mutases the 5′‐deoxyadenosyl radical remains within 3–4 Å of the cobalt atom, with the substrate and product radicals approximately 3 Å further away. It is suggested that cob(II )alamin acts as a conductor by stabilising both the 5′‐deoxyadenosyl radical and the product‐related methylene radicals.     

Kinetics and mechanism of the reversible binding of nitric oxide to reduced cobalamin B(12r) (Cob(II)alamin)

The reduced form of aquacobalamin binds nitric oxide very effectively to yield a nitrosyl adduct, Cbl(II)-NO. UV-vis, (1)H-, (31)P-, and (15)N NMR data suggest that the reaction product under physiological conditions is a six-coordinate, "base-on" form of the vitamin with a weakly bound alpha-dimethylbenzimidazole base and a bent nitrosyl coordinated to cobalt at the beta-site of the corrin ring. The nitrosyl adduct can formally be described as Cbl(III)-NO-. The kinetics of the binding and dissociation reactions was investigated by laser flash photolysis and stopped-flow techniques, respectively. The activation parameters, DeltaH, DeltaS, and DeltaV, for the forward and reverse reactions were estimated from the effect of temperature and pressure on the kinetics of these reactions. For the "on" reaction of Cbl(II) with NO, the small positive DeltaS and DeltaV values suggest the operation of a dissociative interchange (I(d)) substitution mechanism at the Co(II) center. Detailed laser flash photolysis and (17)O NMR studies provide evidence for the formation of water-bound intermediates in the laser flash experiments and strongly support the proposed I(d) mechanism. The kinetics of the "off" reaction was studied using an NO-trapping technique. The respective activation parameters are also consistent with a dissociative interchange mechanism.     

the Mechanism of the Oxidation of Cob(I)alamins

Abstract

Spectroelectrochemical investigations of the reoxidation sequence of the reduced cob(I)alamin to the oxidized cob(III)alamin show that two different cob(II)alamin intermediates are formed during the processes which appear to correlate to base-on and base-off cob(II)-alamin species.     

Cob(I)alamin als Katalysator 2. Mitteilung [1]. Reduktion von gesättigten Nitrilen in wasserfreier Lösung

Cob (I)alamin as Catalyst 2. Communication [1]. Reduction of Saturated Nitriles in Anhydrous Solution Using cob (I)alamin as homogenous catalyst in glacial acetic acid saturated nitriles are reduced following the path of a reductive amination. The results prove the presence of an intermediate imine during the reduction of saturated nitriles with cob (I)alamine.     

Reduction‐Labile Organo‐cob(III)alamins via Cob(II)alamin: Efficient Synthesis and Solution and Crystal Structures of [(Methoxycarbonyl)methyl]cob(III)alamin

An efficient synthesis of Coβ‐[(methoxycarbonyl)methyl]cob(III)alamin ( 6 ) is reported as an example of a new method for the preparation of some easily reducible organo‐cob(III)alamins via the alkylation of cob(II)alamin. The procedure represents a considerable improvement compared to earlier methods that were based on an alkylation of cob(I)alamin. Thus, aquacob(III)alamin chloride ( 5 ⁺?Cl) was reduced to cob(II)alamin ( 4 ), either by controlled potential electrolytic reduction or with an excess of sodium formate as reducing agent. The solution of 4 was then treated with an excess of methyl bromoacetate while being reductively poised potentiostatically or kept reduced by the formate, to give crystalline 6 in a yield of up to 91%. The structure of 6 in aqueous solution was mainly established by the completely assigned ¹H‐ and ¹³CNMR spectra (Table 1). The NOE data (Table 2) were best rationalized by the presence of a single main conformation of the (methoxycarbonyl)methyl ligand. Single crystals of 6 were obtained by crystallization from an aqueous solution, and the crystal structure was determined by X‐ray analysis at cryotemperatures. The NMR and crystallographic data of 6 indicated similar structures in aqueous solution and in the crystal with the (methoxycarbonyl)methyl ligand preferring a ‘southern' orientation in each case.     

Dechlorination of chloroethylenes by cob(I)alamin and cobalamin model complexes

Cobalt-mediated dehalogenation reactions, specifically those that employ cobalamin, have attracted particular attention because these complexes rapidly degrade tetrachloroethylene (PCE) and trichloroethylene (TCE), which are common groundwater contaminants. Although questions remain about the relative importance of several pathways, both radicals and organometallic intermediates, specifically chlorovinyl complexes, play an important role in these processes. This Perspective highlights recent studies focused on elucidating the mechanism of chloroethylene degradation, including experimental studies on PCE and TCE dechlorination, computational studies, preparation of model complexes, and the study of model catalytic systems.     

Cob (I)alamin als Katalysator 4. Mitteilung. Reduktion von α,β-ungesättigten Nitrilen

Cob(I)alamin as Catalyst. 4. Communication. Reduction of α,β-Unsaturated Nitriles Using catalytic amounts of cob (I)alamin and an excess of metallic zinc as source of electrons 1-naphthonitril ( 5 ) has been reduced to (1-naphthyl)methylamin ( 6 ) and in small amounts to (1-naphthyl)methanol ( 7 ) and (1,2,3,4-tetrahydro-1-naphthyl)methanol ( 8 ) (5 ½ h, CH₃COOH/H₂O; s. Scheme 3). Starting from cyclododecylideneacetonitrile ( 15 ) similar conditions (68 h, CH₃COOH/H₂O) produced the amines 16–19 as well as the nitrogen free saturated aldehyde 20 , the corresponding allylic alcohol 21 and the saturated derivative 22 (s. Scheme 6). It is deduced that the first attack of cob (I)alamin on an α,β-unsaturated nitrile might occur on both the nitrile dipole as well as on the carbon atom in β-position. Cob (I)alamin in aqueous acetic acid saturates the isolated double bonds in allylic alcohols and amines. In a slow reaction the two different aromatic rings of (1-naphthyl)methanol ( 7 ) have been reduced giving the corresponding tetrahydronaphthalene derivatives 8 and 12 , and in one case the production of the octahydroderivative 14 has been observed in a low yield (s. Scheme 5).     

Cob(I)alamin als Katalysator. 1. Mitteilung. Reduktion von gesättigten Nitrilen in wässeriger Lösung

Co(I)alamin as Catalyst. 1. Communication. Reduction of Saturated Nitriles in Aqueous Solution Using cob(I)alamin as homogeneous catalyst in the presence of aqueous acetic acid saturated nitriles 5a – m are reduced to the corresponding aldehydes 6a – m in good yields. A possible reaction mechanism for this reduction is discussed.     

Cob(I)alamin als Katalysator. 6. Mitteilung [1]. Bildung und Fragmentierung von Alkylcobalaminen,ein Gleichgewichtsprozess zwischen nukleophiler Addition und reduktiver Fragmentierung

Cob(I)alamin as Catalyst. 6. Communication [1]. Formation and Fragmentation of Alkylcobalamins: the Nucleophilic Addition – Reductive Fragmentation Equilibrium Isolated olefines can be saturated using catalytic amounts of cob(I)alamin in aqueous acetic acid; as electron source an excess of zinc dust is added to the solution containing the homogeneous catalyst. During this overall hydrogenation of isolated double bonds intermediate alkylcobalamins are formed (compare e.g. Schemes 2, 4, 5, 7 and 12). Clear evidence is presented that the nucleophilic attack on the isolated double bond is carried out by cob(I)alamin and not by cob(II)alamin also present in the system (see Scheme 3b and 3c). As this catalytic saturation of olefins depends on the pH of the solution, characterized by a slow reaction at pH = 7.0 compared to the same reduction in aqueous acetic acid (see Scheme 2, 2 → 4 , and Scheme 3a), it is reasonable to accept the participation of an electrophilic attack by a proton during the generation of alkylcobalamins. – We use the term nucleophilic addition to describe the formation of alkylcobalamins from a proton, an olefin and cob(I)alamin (compare Schemes 4–7 and 12). A special sequence of experiments showed the nucleophilic addition to be regioselective. Preferentially the higher substituted alkylcobalamin revealed to be produced. Therefore, the nucleophilic addition of cob(I)alamin follows the Markownikoff rule (compare chap. 4: formation and fragmentation of β-hydroxyalkylcobalamins). Under the reaction conditions applied the intermediate alkylcobalamins can be present in base-on and base-off forms. They are known to exist as octahedral complexes and might also be stable to some extent as tetragonal-pyramidal species. In addition the base-off forms can partially be protonated at the dimethylbenzimidazole moiety in aqueous acetic acid (compare Scheme 12). From this equilibrium of intermediate alkylcobalamins three modes of decay disclosed to be possible: (i) The reductive fragmentation leading to an olefin, a proton, and cob(I)alamin is the formal retro-reaction of the nucleophilic addition (see Schemes 2, 4 and 6–12). This equilibrium of an associated alkylcobalamin and the corresponding dissociation products revealed to be a fast process compared to the reductive cleavage of the Co, C-bond cited below (s. (iii)). (ii) As the second reaction pattern an oxidative fragmentation producing an olefin, a hydroxy anion (or water, respectively) and cob (III)alamin has been observed (see Schemes 7, 8, 10 and 12). (iii) The slow reductive cleavage of the Co, C-bond, initiated by addition of electrons (see [1a] [24]), was the third reaction path observed (see Schemes 2, 4–8 and 10–12). – The stereochemistry of the three transformations originating from the intermediate alkylcobalamins is unknown up to now. The antiperiplanar pattern of the fragmentation reactions presented in the Schemes has been chosen arbitrarily (see e.g. Scheme 12).     

Cob(I)alamin als Katalysator. Retention der Konfiguration bei der reduktiv-protonenübertragenden Spaltung der Co,C-Bindung eines Alkylcobalamins. 7. Mitteilung [1]

Cob(I)alamin as Catalyst. 7. Communication [1]. Retention of Configuration during the Reductive Cleavage of the Co, C-Bond of an Alkylcobalamin Using catalytic amounts of cob(I)alamin (see Scheme 1) in aqueous acetic acid (?)-α-pinen ( 1 ) and (?)-β-pinen ( 2 ; s. Scheme 3) have been reduced. A large excess of metallic zinc served as electron source. The saturated products 5–8 (see Scheme 3) and the mechanistic aspects of their generation are discussed. The relative amounts of cis- ( 5 ) and trans-pinane ( 6 ) lead to the conclusion that the reductive cleavage of the Co, C-bond accompanied by H⁺ transfer in an alkylcobalamin occurs with retention of configuration. This result is in agreement with the corresponding cleavage of the Co,C-bond of an alkyl[hydroxy-diazaoctahydroporphinato]cobalt complex [9].     

Fabrication of Poly(lactic acid) Diacrylate Nanospheres with Double Bonds

Summary: In this paper, unsaturated groups were introduced into poly(lactic acid) (PLA) for fabricating PLA‐based nanospheres with carbon‐carbon double bonds as functional groups. The morphology dependencies on fabrication conditions, including the fabrication time as well as the stirring rate, were also investigated.

SEM‐EDX image of poly(lactic acid) diacrylate nanospheres after exposure to osmium tetroxide vapor for 14 h.     

Dioldehydratase Binds Coenzyme B12 in the “Base-On” Mode: ESR Investigations on Cob(II)alamin

Even in the enzyme-bound state the dimethylbenzimidazole ligand in the dioldehydratase from Salmonella typhimurium remains bound to the cobalt ion in contrast to some coenzyme B₁₂-dependent enzymes. Direct, ESR spectroscopic proof for this “base-on” binding mode was obtained by using a coenzyme in which one of the nitrogen atoms of the dimethylbenzimidazole ligand was ¹⁵N labeled (see schematic representation on the right).     

Cob(I)alamin als Katalysator, 5. Mitteilung [1]. Enantioselektive Reduktion α,β-ungesättigter Carbonylderivate

Cob(I)alamin as Catalyst. 5. Communication [1]. Enantioselective Reduction of α,β-Unsaturated Carbonyl Derivatives The cob(I)alamin-catalyzed reduction of an α,β-unsaturated ethyl ester in aqueous acetic acid produced the (S)-configurated saturated derivative 2 with an enantiomeric excess of 21%. The starting material 1 is not reduced at pH = 7.0 in the presence of catalytic amounts of cob(I)alamin (see Scheme 2). It is shown that the attack of cob(I)alamin and not of cob(II)alamin, also present in Zn/CH₃COOH/H₂O, accounts for the enantioselective reduction observed. All the (Z)-configurated starting materials 1 , 3 , 5 , 7 , 9 and 11 have been transformed to the corresponding (S)-configurated saturated derivatives 2 , 4 , 6 , 8 , 10 and 12 , respectively. The highest enantiomeric excess revealed to be present in the saturated product 12 (32,7%, S) derived from the (Z)-configurated methyl ketone 11 (see Scheme 3 and Table 1). The reduction of the (E)-configurated starting materials led mainly to racemic products. A saturated product having the (R)-configuration with a rather weak enantiomeric excess (5.9%) has been obtained starting from the (E)-configurated methyl ketone 23 (see Scheme 5 and Table 2). The allylic alcohols 16 and 24 have been reduced to the saturated racemic derivative 17 .