| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2042312 | Cell Reports | 2012 | 8 Pages |
SummaryThe consistent observation across all kingdoms of life that highly abundant proteins evolve slowly demonstrates that cellular abundance is a key determinant of protein evolutionary rate. However, other empirical findings, such as the broad distribution of evolutionary rates, suggest that additional variables determine the rate of protein evolution. Here, we report that under the global selection against the cytotoxic effects of misfolded proteins, folding stability (ΔG), simultaneous with abundance, is a causal variable of evolutionary rate. Using both theoretical analysis and multiscale simulations, we demonstrate that the anticorrelation between the premutation ΔG and the arising mutational effect (ΔΔG), purely biophysical in origin, is a necessary requirement for abundance–evolutionary rate covariation. Additionally, we predict and demonstrate in bacteria that the strength of abundance–evolutionary rate correlation depends on the divergence time separating reference genomes. Altogether, these results highlight the intrinsic role of protein biophysics in the emerging universal patterns of molecular evolution.
Graphical AbstractFigure optionsDownload full-size imageDownload as PowerPoint slideHighlights► Protein stability and abundance mutually determine its evolutionary rate ► Coupling of stability changes with wild-type stability affects rate of evolution ► Abundance–evolutionary rate covariation depends on divergence time
