Biosynthesis of iron-sulphur clusters is a complex and highly conserved process

Author:

Frazzon J.1,Fick J. R.2,Dean D. R.2

Affiliation:

1. Department of Food Sciences, ICTA, Federal University of Rio Grande do Sul, Porto Allegre, RS, 91051-970, Brazil

2. Department of Biochemistry, Virginia Tech, Blacksburg, VA 24061-0346, U.S.A.

Abstract

Iron-sulphur ([Fe-S]) clusters are simple inorganic prosthetic groups that are contained in a variety of proteins having functions related to electron transfer, gene regulation, environmental sensing and substrate activation. In spite of their simple structures, biological [Fe-S] clusters are not formed spontaneously. Rather, a consortium of highly conserved proteins is required for both the formation of [Fe-S] clusters and their insertion into various protein partners. Among the [Fe-S] cluster biosynthetic proteins are included a pyridoxal phosphate-dependent enzyme (NifS) that is involved in the activation of sulphur from L-cysteine, and a molecular scaffold protein (NifU) upon which [Fe-S] cluster precursors are formed. The formation or transfer of [Fe-S] clusters appears to require an electron-transfer step. Another complexity is that molecular chaperones homologous to DnaJ and DnaK are involved in some aspect of the maturation of [Fe-S]-cluster-containing proteins. It appears that the basic biochemical features of [Fe-S] cluster formation are strongly conserved in Nature, since organisms from all three life Kingdoms contain the same consortium of homologous proteins required for [Fe-S] cluster formation that were discovered in the eubacteria.

Publisher

Portland Press Ltd.

Subject

Biochemistry

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