Formylation facilitates the reduction of oxidized initiator methionines

Author:

Tan Ruiyue,Hoare Margaret,Bellomio Philip,Broas Sarah,Camacho Konttessa,Swovick Kyle,Welle Kevin A.,Hryhorenko Jennifer R.,Ghaemmaghami Sina

Abstract

AbstractWithin a cell, protein-bound methionines can be oxidized by reactive oxygen species (ROS) or monooxygenases, and subsequently reduced by methionine sulfoxide reductases (Msrs). Methionine oxidation can result in structural damage or be the basis of functional regulation of enzymes. In addition to participating in redox reactions, methionines play an important role as the initiator residue of translated proteins where they are commonly modified at their α-amine group by formylation or acetylation. Here, we investigated how formylation and acetylation of initiator methionines impact their propensity for oxidation and reduction. We show thatin vitro, N-terminal methionine residues are particularly prone to chemical oxidation, and that their modification by formylation or acetylation greatly enhances their subsequent enzymatic reduction by MsrA and MsrB. Concordantly,in vivoablation of methionyl-tRNA formyltransferase (MTF) inE. coliincreases the prevalence of oxidized methionines within synthesized proteins. We show that oxidation of formylated initiator methionines is detrimental in part because it obstructs their ensuing deformylation by peptide deformylase (PDF) and hydrolysis by methionyl aminopeptidase (MAP). Thus, by facilitating their reduction, formylation mitigates the misprocessing of oxidized initiator methionines.Classification: Biological Sciences; Biochemistry

Publisher

Cold Spring Harbor Laboratory

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