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Cell biology of molybdenum in plants and humans.

Biochimica et biophysica acta (2012-03-01)
Ralf R Mendel, Tobias Kruse
ABSTRACT

The transition element molybdenum (Mo) needs to be complexed by a special cofactor in order to gain catalytic activity. With the exception of bacterial Mo-nitrogenase, where Mo is a constituent of the FeMo-cofactor, Mo is bound to a pterin, thus forming the molybdenum cofactor Moco, which in different variants is the active compound at the catalytic site of all other Mo-containing enzymes. In eukaryotes, the most prominent Mo-enzymes are nitrate reductase, sulfite oxidase, xanthine dehydrogenase, aldehyde oxidase, and the mitochondrial amidoxime reductase. The biosynthesis of Moco involves the complex interaction of six proteins and is a process of four steps, which also requires iron, ATP and copper. After its synthesis, Moco is distributed to the apoproteins of Mo-enzymes by Moco-carrier/binding proteins. A deficiency in the biosynthesis of Moco has lethal consequences for the respective organisms. In humans, Moco deficiency is a severe inherited inborn error in metabolism resulting in severe neurodegeneration in newborns and causing early childhood death. This article is part of a Special Issue entitled: Cell Biology of Metals.

MATERIALS
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Molybdenum, insulated wire, 10m, conductor diameter 0.125mm, insulation thickness 0.012mm, polyimide insulation, 99.95%
Molybdenum, insulated wire, 20m, conductor diameter 0.125mm, insulation thickness 0.012mm, polyimide insulation, 99.95%
Molybdenum, insulated wire, 5m, conductor diameter 0.125mm, insulation thickness 0.012mm, polyimide insulation, 99.95%
Molybdenum, insulated wire, 50m, conductor diameter 0.125mm, insulation thickness 0.012mm, polyimide insulation, 99.95%