Model, enzyme complexes

Guanidine coordination to Zn -enzyme-model complex in aqueous solution at neutral pH... 

The study of biomimetics can be of great benefit for the understanding of enzymatic reactions. The term biomimetic refers, in the context of this work, to a compound that mimics structural, functional and spectroscopic properties of an enzyme [67]. Often only one or two of these aspects are achieved for a model system and they usually display substantially lower activity. There are, however, advantages over the enzyme model complexes are generally more stable and robust than their enzymatic counterpart, they can be readily crystalUzed and provide easy accessible structural information on metal ion coordination. Also as these model systems are considerably less complex, kinetic and spectroscopic data interpretation is simplified and— by comparison to data derived for the enzyme— the mechanism of action and structural features can be elucidated and thus related back to the parent metalloenzyme. Also models can be obtained on a larger scale and are often less costly to synthesize, a distinct benefit for potential applications. A few structures of model complexes for dinuclear hydrolytic enzymes are shown in Fig. 1.4. The approaches for ligand and complex design are diverse. 

Enzyme-substrate complex, 1041 Ephedrine, structure of, 65 Epibatidine, molecular model of. 332 Epichlorohydrin, epoxy resins from, 673-674 Epimer, 303... 

Substrate and product inhibitions analyses involved considerations of competitive, uncompetitive, non-competitive and mixed inhibition models. The kinetic studies of the enantiomeric hydrolysis reaction in the membrane reactor included inhibition effects by substrate (ibuprofen ester) and product (2-ethoxyethanol) while varying substrate concentration (5-50 mmol-I ). The initial reaction rate obtained from experimental data was used in the primary (Hanes-Woolf plot) and secondary plots (1/Vmax versus inhibitor concentration), which gave estimates of substrate inhibition (K[s) and product inhibition constants (A jp). The inhibitor constant (K[s or K[v) is a measure of enzyme-inhibitor affinity. It is the dissociation constant of the enzyme-inhibitor complex. 

Kimura E, Koike T, Shionoya M (1997) Advances in Zinc Enzyme Models by Small, Mononuclear Zinc(ll) Complexes. 89 1-28... 

It is probable that the negative charge induced by these three electrons on FeMoco is compensated by protonation to form metal hydrides. In model hydride complexes two hydride ions can readily form an 17-bonded H2 molecule that becomes labilized on addition of the third proton and can then dissociate, leaving a site at which N2 can bind (104). This biomimetic chemistry satisfyingly rationalizes the observed obligatory evolution of one H2 molecule for every N2 molecule reduced by the enzyme, and also the observation that H2 is a competitive inhibitor of N2 reduction by the enzyme. The bound N2 molecule could then be further reduced by a further series of electron and proton additions as shown in Fig. 9. The chemistry of such transformations has been extensively studied with model complexes (15, 105). 

The mechanistic and structural chemistry of B12 may be separated into (i) investigations of cobalamin cofactors both apart from and in complex with their enzymes, and (ii) biomimetic model complexes, both structural and functional. 

Zinc alkoxide and aryloxide complexes have been of particular interest as enzyme models and catalysts. Tetrameric alkyl zinc alkoxides are a common structurally characterized motif.81... 

As we saw in the previous sections, inclusion compounds have many structural properties which relate them to other systems based on the hierarchy of non-bound interactions, like enzymes or enzyme-substrate complexes. As a matter of fact, most of the so-called artificial enzymes are based on well-known host molecules (e.g. P-cyclodextrin) and are designed to act partly on such bases 108>109). Most of these models, however, take advantage of the inclusion (intra-host encapsulation) phenomena. Construction of proper covalently bound model molecules is a formidable task for the synthetic chemistuo>. Therefore, any kind of advance towards such a goal is welcomed. 

Finally, we come to enzyme models. D. W. Griffiths and M. L. Bender describe the remarkable catalytic property of certain cycloamyloses which act through formation of inclusion complexes, and in this respect recall the clefts containing the active sites in enzymes such as lysozyme and papain. 

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