Abstract
AbstractMitochondria are membrane-bound organelle hubs of cellular metabolism and signaling. The dysregulation of mitochondria is related to the genesis of several highly prevalent diseases, including cancer and cardiovascular disorders, urging the development of novel technologies to systematically study this organelle and its dynamics. Thermal proteome profiling (TPP) allows the unbiased study of the interactions of proteins with drugs, metabolites, and other proteins, providing a unique understanding of the state of the proteome. Here, we develop and introduce an optimized TPP workflow, mito-TPP, for the direct and extensive study of this organelle. We demonstrate that our approach detects both direct mitochondrial small molecule-protein and metabolite-protein interactions, as well as indirect downstream effects. We also show that mito-TPP preserves features from whole-cell systems, such as the coaggregation of interacting proteins. Finally, we explore the mitochondrial proteoform map, detecting more than 180 proteins with multiple proteoform groups. Overall, we demonstrate that mito-TPP is a powerful new tool for the functional study of the mitochondrial proteome.
Publisher
Cold Spring Harbor Laboratory