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The folding pathway, three-dimensional structure and intrinsic dynamics of proteins are governed by their amino acid sequences. Internal protein surfaces with physicochemical properties appropriate to modulate conformational fluctuations could play important roles in folding and dynamics. We show here that proteins contain buried interfaces of high polarity and low packing density, coined as LIPs: Light Interfaces of high Polarity, whose physicochemical properties make them unstable. The structures of well-characterized equilibrium and kinetic folding intermediates indicate that the LIPs of the corresponding native proteins fold late and are involved in local unfolding events. Importantly, LIPs can be identified using very fast and uncomplicated computational analysis of protein three-dimensional structures, which provides an easy way to delineate the protein segments involved in dynamics. Since LIPs can be retained while the sequences of the interacting segments diverge significantly, proteins could in principle evolve new functional features reusing pre-existing encoded dynamics. Large-scale identification of LIPS may contribute to understanding evolutionary constraints of proteins and the way protein intrinsic dynamics are encoded.
Protein Folding, Science, Q, R, Indole-3-Glycerol-Phosphate Synthase, Cytochromes c, Proteins, Protein Structure, Secondary, Protein Structure, Tertiary, Kinetics, Ribonucleases, Bacterial Proteins, Lactalbumin, Medicine, Research Article
Protein Folding, Science, Q, R, Indole-3-Glycerol-Phosphate Synthase, Cytochromes c, Proteins, Protein Structure, Secondary, Protein Structure, Tertiary, Kinetics, Ribonucleases, Bacterial Proteins, Lactalbumin, Medicine, Research Article
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