Understanding the role of protein arginylation in health and disease through analytical and biological approaches

Abstract

Post-translational modifications (PTMs) alter the physicochemical and biological properties of a protein, influencing its function in health and disease state. Indeed, PTMs regulate stability, degradation, enzymatic function, protein interaction, and subcellular localization. Protein arginylation is a PTM little-explored described for the first time in 1963. Only in 2002, a study showed that the knockout of the ATE1 gene resulted in abnormalities in important processes such as cardiac development, angiogenesis, and tissue morphogenesis in mammals. Recently, our group identified arginylated proteins in Trypanosoma cruzi, however, the function of these PTMs in the pathogenesis is understood. In order to better understand this PTM, it is imperative to develop a method capable of analyzing and quantifying arginylated proteins, since at the moment there is no methodology in the literature for this purpose. Thus, the objective of this project is to develop and validate a robust, efficient, accurate, and reproducible enrichment method for the identification and quantification of arginylated peptides in complex biological matrices. For this, we will test different liquid chromatography formats from HPLC to microscale in-tip chromatographic columns. The enriched fractions will be analyzed by mass spectrometry. This method will be initially tested on synthetic arginylated peptides spiked in complex biological matrices. Once optimized, the method will be applied to T. cruzi epimastigote and trypomastigote life stages. Moreover, we will apply this method to LLCM-K2 rhesus monkey kidney cells infected and uninfected with T. cruzi. It should be noted that the method developed in this project will have a broad utility in the scientific community and will open the possibility to study this PTM in several biological mechanisms. Shedding lights on the identity of arginylated proteins is the most important step to understand the function and modulation of this PTM in pathophysiological conditions. Moreover, the levels and role of arginylation in biofluids is presently unknown and could introduce a new layer of protein regulation for biomarker discovery. (AU)