Theory for protein mutability and biogenesis

Using an elementary physical model for protein folding, of self-avoiding short copolymer chains on two-dimensional square lattices, we address two questions regarding the evolution and origins of globular proteins. (i) How will protein native structures and stabilities be affected by single- and dou...

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Bibliographic Details
Published in:Proceedings of the National Academy of Sciences - PNAS 1990, Vol.87 (2), p.638-642
Main Authors: Lau, K.F, Dill, K.A
Format: Article
Language:English
Subjects:
Active sites
Amino Acid Sequence
amino acid sequences
Amino acids
Analytical, structural and metabolic biochemistry
Biological and medical sciences
computer simulation
Free energy
Fundamental and applied biological sciences. Psychology
Globulins
Lead
Miscellaneous
Modeling
Models, Biological
Models, Genetic
Models, Structural
molecular conformation
Molecular evolution
Molecular structure
Molecules
Mutation
Protein Conformation
protein folding
Proteins
Proteins - genetics
simulation models
Simulations
Space life sciences
structural genes
theory
Thermodynamics
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Summary:Using an elementary physical model for protein folding, of self-avoiding short copolymer chains on two-dimensional square lattices, we address two questions regarding the evolution and origins of globular proteins. (i) How will protein native structures and stabilities be affected by single- and double-site mutations? (ii) What is the probability that a randomly chosen sequence of amino acids will be compact and globular under folding conditions? For a large number of different sequences, we search the conformational space exhaustively to find unequivocally the "native" conformation(s), of global minimum free energy, for each sequence. We find that replacing nonpolar residues in the core by polar residues is generally destabilizing, that surface sites are less sensitive than core sites, that some mutations increase the degeneracy of native states, and that overall it is most probable that a mutation will be neutral, having no effect on the native structure. These results support a "Continuity Principle," that small changes in sequence seldom have large effects on structure or stability of the native state. The simulations also show that (i) the number of "convergent" sequences (different sequences coding for the same native structure) is extremely large and (ii) most sequences become quite dense under folding conditions. This implies that the probability of formation of a globular protein from a random sequence of amino acids by prebiotic or mutational methods is significantly greater than zero.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.87.2.638