Natural-like function in artificial WW domains

William P. Russ; Drew M. Lowery; Prashant Mishra; Michael B. Yaffe; Rama Ranganathan

doi:10.1038/nature03990

Natural-like function in artificial WW domains

William P. Russ, Drew M. Lowery, Prashant Mishra, Michael B. Yaffe, Rama Ranganathan

Research output: Contribution to journal › Article › peer-review

207 Scopus citations

Abstract

Protein sequences evolve through random mutagenesis with selection for optimal fitness. Cooperative folding into a stable tertiary structure is one aspect of fitness, but evolutionary selection ultimately operates on function, not on structure. In the accompanying paper, we proposed a model for the evolutionary constraint on a small protein interaction module (the WW domain) through application of the SCA, a statistical analysis of multiple sequence alignments. Construction of artificial protein sequences directed only by the SCA showed that the information extracted by this analysis is sufficient to engineer the WW fold at atomic resolution. Here, we demonstrate that these artificial WW sequences function like their natural counterparts, showing class-specific recognition of proline-containing target peptides. Consistent with SCA predictions, a distributed network of residues mediates functional specificity in WW domains. The ability to recapitulate natural-like function in designed sequences shows that a relatively small quantity of sequence information is sufficient to specify the global energetics of amino acid interactions.

Original language	English (US)
Pages (from-to)	579-583
Number of pages	5
Journal	Nature
Volume	437
Issue number	7058
DOIs	https://doi.org/10.1038/nature03990
State	Published - Sep 22 2005

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@article{b7798328fcd047ea8e674b2040457ca2,

title = "Natural-like function in artificial WW domains",

abstract = "Protein sequences evolve through random mutagenesis with selection for optimal fitness. Cooperative folding into a stable tertiary structure is one aspect of fitness, but evolutionary selection ultimately operates on function, not on structure. In the accompanying paper, we proposed a model for the evolutionary constraint on a small protein interaction module (the WW domain) through application of the SCA, a statistical analysis of multiple sequence alignments. Construction of artificial protein sequences directed only by the SCA showed that the information extracted by this analysis is sufficient to engineer the WW fold at atomic resolution. Here, we demonstrate that these artificial WW sequences function like their natural counterparts, showing class-specific recognition of proline-containing target peptides. Consistent with SCA predictions, a distributed network of residues mediates functional specificity in WW domains. The ability to recapitulate natural-like function in designed sequences shows that a relatively small quantity of sequence information is sufficient to specify the global energetics of amino acid interactions.",

author = "Russ, {William P.} and Lowery, {Drew M.} and Prashant Mishra and Yaffe, {Michael B.} and Rama Ranganathan",

note = "Funding Information: Acknowledgements We thank members of the Ranganathan laboratory for advice and critical review of the manuscript, J. P. Noel for providing the pHIS8 expression vector, and K. Voegler for contributing to this project. This study was supported by the Robert A. Welch foundation (R.R.), the Mallinckrodt Foundation Scholar Award (R.R.), NIH grants (M.B.Y.), and a Burroughs-Wellcome Career Development Award (M.B.Y.). D.M.L. was supported by a Howard Hughes Medical Institute pre-doctoral award. W.P.R. is an associate and R.R. is an investigator of the Howard Hughes Medical Institute.",

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AU - Ranganathan, Rama

N1 - Funding Information: Acknowledgements We thank members of the Ranganathan laboratory for advice and critical review of the manuscript, J. P. Noel for providing the pHIS8 expression vector, and K. Voegler for contributing to this project. This study was supported by the Robert A. Welch foundation (R.R.), the Mallinckrodt Foundation Scholar Award (R.R.), NIH grants (M.B.Y.), and a Burroughs-Wellcome Career Development Award (M.B.Y.). D.M.L. was supported by a Howard Hughes Medical Institute pre-doctoral award. W.P.R. is an associate and R.R. is an investigator of the Howard Hughes Medical Institute.

PY - 2005/9/22

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N2 - Protein sequences evolve through random mutagenesis with selection for optimal fitness. Cooperative folding into a stable tertiary structure is one aspect of fitness, but evolutionary selection ultimately operates on function, not on structure. In the accompanying paper, we proposed a model for the evolutionary constraint on a small protein interaction module (the WW domain) through application of the SCA, a statistical analysis of multiple sequence alignments. Construction of artificial protein sequences directed only by the SCA showed that the information extracted by this analysis is sufficient to engineer the WW fold at atomic resolution. Here, we demonstrate that these artificial WW sequences function like their natural counterparts, showing class-specific recognition of proline-containing target peptides. Consistent with SCA predictions, a distributed network of residues mediates functional specificity in WW domains. The ability to recapitulate natural-like function in designed sequences shows that a relatively small quantity of sequence information is sufficient to specify the global energetics of amino acid interactions.

AB - Protein sequences evolve through random mutagenesis with selection for optimal fitness. Cooperative folding into a stable tertiary structure is one aspect of fitness, but evolutionary selection ultimately operates on function, not on structure. In the accompanying paper, we proposed a model for the evolutionary constraint on a small protein interaction module (the WW domain) through application of the SCA, a statistical analysis of multiple sequence alignments. Construction of artificial protein sequences directed only by the SCA showed that the information extracted by this analysis is sufficient to engineer the WW fold at atomic resolution. Here, we demonstrate that these artificial WW sequences function like their natural counterparts, showing class-specific recognition of proline-containing target peptides. Consistent with SCA predictions, a distributed network of residues mediates functional specificity in WW domains. The ability to recapitulate natural-like function in designed sequences shows that a relatively small quantity of sequence information is sufficient to specify the global energetics of amino acid interactions.

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Natural-like function in artificial WW domains

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