Biosynthesis of the Iron-Molybdenum Cofactor of Nitrogenase

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Biosynthesis of the Iron-Molybdenum Cofactor of Nitrogenase

2008; Annual Reviews; Volume: 62; Issue: 1 Linguagem: Inglês

10.1146/annurev.micro.62.081307.162737

ISSN

1545-3251

Autores

Luis M. Rubio, Paul W. Ludden,

Tópico(s)

Ammonia Synthesis and Nitrogen Reduction

Resumo

The iron-molybdenum cofactor (FeMo-co) of nitrogenase is a Mo-Fe-S cluster that has been proposed as the site of substrate reduction for the nitrogenase enzyme complex. Biosynthesis of FeMo-co in Klebsiella pneumoniae requires at least six nif (nitrogen fixation) gene products. One of the nif genes, nifV, apparently encodes a homocitrate synthase. The synthesis and accumulation of homocitrate [(R)-2-hydroxy-1,2,4-butanetricarboxylic acid] in K.pneumoniae is correlated to the presence of a functional nifV gene. K.pneumoniae strains with mutations in nifV synthesize and accumulate an aberrant form of FeMo-co. Nitrogenase from NifV- mutants is capable of reducing some of the substrates of nitrogenase effectively (e.g. acetylene), but reduces N2 poorly. With the aid of an in vitro FeMo-co synthesis system, it recently has been established that homocitrate is an endogenous component of FeMo-co. Substitution of homocitrate with other carboxylic acids results in the formation of aberrant forms of FeMo-co with altered substrate reduction capability.

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Biosynthesis of the Iron-Molybdenum Cofactor of Nitrogenase