Cytosolic iron-sulfur protein assembly system identifies clients by a C-terminal tripeptide.
Melissa D MarquezCarina GrethAnastasiya BuzukYaxi LiuCatharina M BlinnSimone BellerLaura LeiskauAnthony HushkaKassandra WuKübra NurDaili J A NetzDeborah L PerlsteinAntonio J PierikPublished in: Proceedings of the National Academy of Sciences of the United States of America (2023)
The eukaryotic cytosolic Fe-S protein assembly (CIA) machinery inserts iron-sulfur (Fe-S) clusters into cytosolic and nuclear proteins. In the final maturation step, the Fe-S cluster is transferred to the apo-proteins by the CIA-targeting complex (CTC). However, the molecular recognition determinants of client proteins are unknown. We show that a conserved [LIM]-[DES]-[WF]-COO - tripeptide is present at the C-terminus of more than a quarter of clients or their adaptors. When present, this targeting complex recognition (TCR) motif is necessary and sufficient for binding to the CTC in vitro and for directing Fe-S cluster delivery in vivo. Remarkably, fusion of this TCR signal enables engineering of cluster maturation on a nonnative protein via recruitment of the CIA machinery. Our study advances our understanding of Fe-S protein maturation and paves the way for bioengineering novel pathways containing Fe-S enzymes.