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Coenzyme distribution

Mobile coenzymes Distribution of metabolic fragments H , CH3, -COCH3, etc. [Pg.231]

Pantothenic acid is found in extracts from nearly all plants, bacteria, and animals, and the name derives from the Greek pantos, meaning everywhere. It is required in the diet of all vertebrates, but some microorganisms produce it in the rumens of animals such as cattle and sheep. This vitamin is widely distributed in foods common to the human diet, and deficiencies are only observed in cases of severe malnutrition. The eminent German-born biochemist Fritz Lipmann was the first to show that a coenzyme was required to facilitate biological acetylation reactions. (The A in... [Pg.594]

It is very important to realise that if many processes share a component in reaction pathways or controls then this is readily achieved if the binding of that component is at equilibrium with closely the same binding constant at sites within the different paths and controls. This is often true of components such as metal ions, coenzymes and energy-distributing molecules such as ATP. [Pg.116]

ATP and magnesium were required for the activation of acetate. Acetylations were inhibited by mercuric chloride suggesting an SH group was involved in the reaction either on the enzyme or, like lipoic acid, as a cofactor. Experiments from Lipmann s laboratory then demonstrated that a relatively heat-stable coenzyme was needed—a coenzyme for acetylation—coenzyme A (1945). The thiol-dependence appeared to be associated with the coenzyme. There was also a strong correlation between active coenzyme preparations and the presence in them of pantothenic acid—a widely distributed molecule which was a growth factor for some microorganisms and which, by 1942-1943, had been shown to be required for the oxidation of pyruvate. [Pg.78]

The first of these new, electron transferring components was coenzyme Q (CoQ). Festenstein in R.A. Morton s laboratory in Liverpool had isolated crude preparations from intestinal mucosa in 1955. Purer material was obtained the next year from rat liver by Morton. The material was lipid soluble, widely distributed, and had the properties of a quinone and so was initially called ubiquinone. Its function was unclear. At the same time Crane, Hatefi and Lester in Wisconsin were trying to identify the substances in the electron transport chain acting between NADH and cytochrome b. Using lipid extractants they isolated a new quininoid coenzyme which showed redox changes in respiration. They called it coenzyme Q (CoQ). CoQ was later shown to be identical to ubiquinone. [Pg.89]

The best-known aldopentose (1), D-ribose, is a component of RNA and of nucleotide coenzymes and is widely distributed. In these compounds, ribose always exists in the fura-nose form (see p. 34). Like ribose, D-xylose and L-arabinose are rarely found in free form. However, large amounts of both sugars are found as constituents of polysaccharides in the walls of plant cells (see p.42). [Pg.38]

The pyridine nucleotides NAD"" and NADP" (1) are widely distributed as coenzymes of dehydrogenases. They transport hydride ions (2e and 1 see p. 32) and always act in soluble form. NAD" transfers reducing equivalents from catabolic pathways to the respiratory chain and thus contributes to energy... [Pg.104]

It is synthesized within the cholinergic neurons by the transfer of an acetyl group from acetyl coenzyme A to the organic base choline. The specific enzyme choline acetylase is essential for this reaction. Coenzyme A is widely distributed in the body and choline acetylase is synthesized in the cell bodies of the cholinergic neurons. [Pg.156]

Proanthocyanidins and Procyanidins - In a classical study Bate-Smith ( ) used the patterns of distribution of the three principal classes of phenolic metabolites, which are found in the leaves of plants, as a basis for classification. The biosynthesis of these phenols - (i) proanthocyanidins (ii) glycosylated flavonols and (iii) hydroxycinnamoyl esters - is believed to be associated with the development in plants of the capacity to synthesise the structural polymer lignin by the diversion from protein synthesis of the amino-acids L-phenylalanine and L-tyro-sine. Vascular plants thus employ one or more of the p-hydroxy-cinnarayl alcohols (2,3, and 4), which are derived by enzymic reduction (NADH) of the coenzyme A esters of the corresponding hydroxycinnamic acids, as precursors to lignin. The same coenzyme A esters also form the points of biosynthetic departure for the three groups of phenolic metabolites (i, ii, iii), Figure 1. [Pg.124]

FIGURE 19-1 Biochemical anatomy of a mitochondrion. The convolutions (cristae) of the inner membrane provide a very large surface area. The inner membrane of a single liver mitochondrion may have more than 10,000 sets of electron-transfer systems (respiratory chains) and ATP synthase molecules, distributed over the membrane surface. Heart mitochondria, which have more profuse cristae and thus a much larger area of inner membrane, contain more than three times as many sets of electron-transfer systems as liver mitochondria. The mitochondrial pool of coenzymes and intermediates is functionally separate from the cytosolic pool. The mitochondria of invertebrates, plants, and microbial eukaryotes are similar to those shown here, but with much variation in size, shape, and degree of convolution of the inner membrane. [Pg.691]

Pantothenic acid is a component of coenzyme A, which functions in the transfer of acyl groups (Figure 28.17). Coenzyme A contains a thiol group that carries acyl compounds as activated thiol esters. Examples of such structures are succinyl CoA, fatty acyl CoA, and acetyl CoA. Pantothenic acid is also a component of fatty acid synthase (see p. 182). Eggs, liver, and yeast are the most important sources of pan tothenic acid, although the vitamin is widely distributed. Pantothenic acid deficiency is not well characterized in humans, and no RDA has been established. [Pg.379]

Imidazole also acts as a substrate-competitive inhibitor, forming both binary complexes with LADH, and ternary complexes in the presence of coenzyme. X-Ray studies show that imidazole also binds to the. catalytic zinc by displacing the water molecule.1361 The presence of imidazole at the active site also enhances the rate of carboxymethylation14658 of Cys-46 with both iodoacetate and iodoacetamide.1420 This enhancement of alkylation has become known as the promotion effect .1421 Imidazole promotion also improves the specificity of the alkylation.1422 Since Cys-46 is thought to be alkylated as a metal-thiol complex, imidazole, on binding the active site metal, could enhance the reactivity by donating a electrons to the metal atom, which distributes the increased electron density further to the other ligands in the coordination sphere. The increased nucleophilicity of the sulfur results in promoted alkylation.1409... [Pg.1017]

A scries of quinones which are widely distributed in animals, plants, and microorganisms, these quinones have been shown to function in biological electron transport systems which are responsible for energy conversion with living cells. The nature and significance of coenzyme Q was first... [Pg.414]

See other pages where Coenzyme distribution is mentioned: [Pg.482]    [Pg.97]    [Pg.482]    [Pg.97]    [Pg.47]    [Pg.473]    [Pg.289]    [Pg.193]    [Pg.199]    [Pg.202]    [Pg.203]    [Pg.204]    [Pg.233]    [Pg.340]    [Pg.355]    [Pg.827]    [Pg.181]    [Pg.196]    [Pg.252]    [Pg.252]    [Pg.261]    [Pg.274]    [Pg.135]    [Pg.314]    [Pg.131]    [Pg.124]    [Pg.1202]    [Pg.140]    [Pg.877]    [Pg.153]    [Pg.629]    [Pg.687]    [Pg.379]    [Pg.741]    [Pg.1200]    [Pg.751]    [Pg.803]    [Pg.867]    [Pg.1216]    [Pg.281]   
See also in sourсe #XX -- [ Pg.135 ]



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