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  A biosynthetic pathway to isovaleryl-CoA in myxobacteria: the involvement of the mevalonate pathway

Mahmud, T., Wenzel, S. C., Wan, E., Wen, K. W., Bode, H. B., Gaitatzis, N., et al. (2004). A biosynthetic pathway to isovaleryl-CoA in myxobacteria: the involvement of the mevalonate pathway. Chembiochem, 6(2), 322-30. doi:10.1002/cbic.200400261.

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Mahmud, T., Author
Wenzel, S. C., Author
Wan, E., Author
Wen, K. W., Author
Bode, H. B.1, Author           
Gaitatzis, N., Author
Muller, R., Author
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1Universität des Saarlandes, External Organization, ou_persistent22              

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Free keywords: Acyl Coenzyme A/*biosynthesis/chemistry/metabolism Animals Glutarates/chemistry/metabolism Leucine/metabolism Methacrylates Mevalonic Acid/chemistry/*metabolism Molecular Structure Myxococcales/chemistry/*metabolism Quinolines/chemistry/metabolism Stigmatella aurantiaca/chemistry/genetics/metabolism Thiazoles/chemistry/metabolism
 Abstract: A biosynthetic shunt pathway branching from the mevalonate pathway and providing starter units for branched-chain fatty acid and secondary metabolite biosynthesis has been identified in strains of the myxobacterium Stigmatella aurantiaca. This pathway is upregulated when the branched-chain alpha-keto acid dehydrogenase gene (bkd) is inactivated, thus impairing the normal branched-chain amino acid degradation process. We previously proposed that, in this pathway, isovaleryl-CoA is derived from 3,3-dimethylacrylyl-CoA (DMA-CoA). Here we show that DMA-CoA is an isomerization product of 3-methylbut-3-enoyl-CoA (3MB-CoA). This compound is directly derived from 3-hydroxy-3-methylglutaryl-CoA (HMG-CoA) by a decarboxylation/ dehydration reaction resembling the conversion of mevalonate 5-diphosphate to isopentenyl diphosphate. Incubation of cell-free extracts of a bkd mutant with HMG-CoA gave product(s) with the molecular mass of 3MB-CoA or DMA-CoA. The shunt pathway most likely also operates reversibly and provides an alternative source for the monomers of isoprenoid biosynthesis in myxobacteria that utilize L-leucine as precursor.

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 Dates: 2004-12-28
 Publication Status: Issued
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 Identifiers: Other: 15619721
DOI: 10.1002/cbic.200400261
ISSN: 1439-4227 (Print)1439-4227 (Linking)
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Title: Chembiochem
Source Genre: Journal
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Pages: - Volume / Issue: 6 (2) Sequence Number: - Start / End Page: 322 - 30 Identifier: -