Changes of Cell Biochemical States Are Revealed in Protein Homomeric Complex Dynamics

Summary We report here a simple and global strategy to map out gene functions and target pathways of drugs, toxins, or other small molecules based on “homomer dynamics” protein-fragment complementation assays ( hd PCA). hd PCA measures changes in self-association (homomerization) of over 3,500 yeast proteins in yeast grown under different conditions. hd PCA complements genetic interaction measurements while eliminating the confounding effects of gene ablation. We demonstrate that hd PCA accurately predicts the effects of two longevity and health span-affecting drugs, the immunosuppressant rapamycin and the type 2 diabetes drug metformin, on cellular pathways. We also discovered an unsuspected global cellular response to metformin that resembles iron deficiency and includes a change in protein-bound iron levels. This discovery opens a new avenue to investigate molecular mechanisms for the prevention or treatment of diabetes, cancers, and other chronic diseases of aging.