Intricacies in Iron-Sulfur Cluster Function and Biogenesis: Functional Versatility, Sulfur Sources, and Enzyme Specificity

Abstract

Iron-sulfur (Fe-S) clusters are ancient inorganic cofactors ubiquitous across all domains of life. These cofactors associate with proteins through constitutive or transient coordination, expanding their chemistries and versatility in biological processes. Thus, Fe-S proteins participate in intricate and multifaceted chemistries critical to life on Earth. The biosynthesis of these cofactors has evolved to require complex machinery to catalyze cluster formation and subsequent transfer to target apo-proteins. Five Fe-S cluster biogenesis systems have been identified, with varying degrees of complexity, including: iron-sulfur cluster (ISC), nitrogen fixation (NIF), sulfur mobilization (SUF), minimal iron-sulfur system (MIS), and SUF-like minimal system (SMS). Sulfur mobilization in the biosynthesis of Fe-S clusters is initiated, in most cases, by cysteine sulfurtransferases, also known as cysteine desulfurases. These enzymes use the amino acid cysteine as a sulfur donor and require specific interactions with a sulfur acceptor to promote sulfur transfer. Physical interactions and coordination among biosynthetic components restrict their functions and guarantee the trafficking of reactive intermediates to proper destinations. As recently reported, the occurrence of alternate biosynthetic schemes using sulfide as the sulfur source bypasses the requirement for sulfurtransferases and provides alternate evolutionary strategies to construct Fe-S clusters.