Big Chemical Encyclopedia

Chemical substances, components, reactions, process design ...

Articles Figures Tables About

Synthetase phosphatase

D) inhibition of glycogen synthetase phosphatase activity in liver... [Pg.178]

Several observations regarding this aspect have been published, and are briefly mentioned here. 5,6-Dideoxy-6-C-phosphono-D-arabino-hexofuranose (135), an isosteric phosphonate analog of D-arabinose 5-phosphate, is apparently converted, in the presence of enolpyruvate phosphate, into 3,8,9-trideoxy-9-C-phosphono-D-mcmno-2-nonulosonic acid (136) under catalysis by KDO 8-phosphate synthetase from Escherichia coli K 235. Compound 136, an isosteric phosphonate analog of KDO 8-phosphate, is a product inhibitor of the synthetase, and, by the nature of the phosphonate group, is not subject to dephosphorylation as catalyzed by KDO 8-phosphate phosphatase156 (see Scheme 40). Compound 119 (see Scheme 33) is a weak inhibitor of KDO 8-phosphate synthetase.81 KDO inhibits KDO 8-phosphate phosphatase,139 and D-ribose 5-phosphate has an inhibitory... [Pg.387]

HISTIDINOL-PHOSPHATE PHOSPHATASE HISTIDYL-tRNA SYNTHETASE HISTONE KINASE Hofmann rule,... [Pg.748]

ADENYLATE CYCLASE ALKALINE PHOSPHATASE AMIDOPHOSPHORIBOSYLTRANSFERASE AMINOACYL-tRNA SYNTHETASES... [Pg.775]

Synthases and Synthetases Ligases and Lyases Kinases, Phosphatases, and Phosphorylases Yes, the Names Are Confusing ... [Pg.613]

The reactions, 1-5 respectively, are catalyzed by D-arabinose-5-phosphate isoraerase, KD0-8-phosphate synthase, KD0-8-phosphate phosphatase, CMP-KDO synthetase and KDO transferase (s). Using E. coli B, we have isolated and purified the second, third and fourth enzymes to homogeneity and studied their properties. The fifth enzyme has been partially purified by Osborn s laboratory (15) and we have not improved on its purification or further studied its properties. [Pg.146]

D-Glucose-6-phosphate dehydrogenase, D-gluconate-6-phosphate dehydrogenase, KDO-8-phosphate synthase, KDO-8-phosphate phosphatase and CMP-KDO synthetase have been purified to homogeneity and characterized. Munson, Rasmussen and Osborn (15) have partially purified one KDO transferase. D-Arabinose-5-phosphate isomerase is very unstable and has only been purified about 100 fold. D-Ribose-5-phosphate isomerase activity is approximately 20x that... [Pg.157]

The requirement of the remaining enzymes, KD0-8-phosphate synthase, KD0-8-phosphate phosphatase and CMP-KDO synthetase, for their natural substrates, D-arabinose-5-phosphate + PEP, KD0-8-phosphate and KDO + CTP, respectively, was specific and the inhibition studies with substrate analogues were disappointing. Of the compounds tested as potential substrates of KD0-8-phosphate synthase, only the isosteric phosphonate analogue (Compound 11, Table III) of D-arabinose-5-phosphate was an alternate substrate (see Ref. 28). There were a number of weak competitive inhibitors of the synthase reaction (Compounds 2, 5, 6, 7, 15,and 19,Table III) the best inhibitor of the synthase reaction was 2-deoxy-2-fluoro-D-arabinonate-5-phosphate (compound 14, Table III). [Pg.165]

Animal and bacterial enzymes that utilize or synthesize carbamyl phosphate have activity with acetyl phosphate. Acyl phosphatase hydrolyzes both substrates, and maybe involved in the specific dynamic action of proteins. Ornithine and aspartic transcarbamylases also synthesize acetylornithine and acetyl aspartate. Finally, bacterial carbamate kinase and animal carbamyl phosphate synthetase utilize acetyl phosphate as well as carbamyl phosphate in the synthesis of adenosine triphosphate. The synthesis of acetyl phosphate and of formyl phosphate by carbamyl phosphate synthetases is described. The mechanism of carbon dioxide activation by animal carbamyl phosphate synthetase is reviewed on the basis of the findings concerning acetate and formate activation. [Pg.151]

C. A. Mitchell, S. Brown, J. K. Campbell, A. D. Munday andC.L. Speed (1996). Regulation of second messengers by the inositol polyphosphate 5-phosphatases. Biochem. Soc. Trans., 24, 994-1000. G. J. Mittenhuber (2001). Comparative genomics and evolution of genes encoding bacterial (p)ppGpp synthetases/hydrolases (the Rel, RelA and SpoT proteins). Mol. Microbiol. Biotechnol., 3, 585-600. [Pg.244]

The synthesis of triacylglycerol takes place in the endoplasmic reticulum (ER). In liver and adipose tissue, fatty adds in the cytosol obtained from the diet or from de novo synthesis of palmitic add become inserted into the ER membrane. The reactions are shown in Fig. 13-10. Membrane-bound acyl-CoA synthetase activates two fatty acids, and membrane-bound acyl-CoA transferase esterifies them with glycerol 3-phosphate, to form phosphatidic acid. Phosphatidic acid phosphatase releases phosphate, and in the membrane, 1,2-diacylglycerol is esterified with a third molecule of fatty acid. [Pg.378]

Sucrose phosphate synthetase catalyzes the reaction of UDP-glucose with fructose-6-P to form sucrose-6-P and UDP. This step is the penultimate step in the synthesis of sucrose in leaves. The chromatographic method can be applied to many UDP-glucose-requiring enzymes. The method eliminates the need for treatment of reaction mixtures with alkaline phosphatase. [Pg.300]

See other pages where Synthetase phosphatase is mentioned: [Pg.190]    [Pg.226]    [Pg.579]    [Pg.190]    [Pg.226]    [Pg.579]    [Pg.1295]    [Pg.217]    [Pg.168]    [Pg.704]    [Pg.704]    [Pg.253]    [Pg.191]    [Pg.302]    [Pg.131]    [Pg.98]    [Pg.28]    [Pg.321]    [Pg.584]    [Pg.275]    [Pg.318]    [Pg.389]    [Pg.1201]    [Pg.985]    [Pg.572]    [Pg.597]    [Pg.164]    [Pg.166]    [Pg.167]    [Pg.244]    [Pg.197]    [Pg.331]    [Pg.1295]   
See also in sourсe #XX -- [ Pg.223 , Pg.226 ]



SEARCH



Glycogen synthetase phosphatase

© 2024 chempedia.info