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Evolution of a Signaling Nexus Constrained by Protein Interfaces and Conformational States
by
Temple, Brenda R. S.
, Jones, Corbin D.
, Jones, Alan M.
in
Analysis
/ Biochemistry/Macromolecular Chemistry
/ Biochemistry/Molecular Evolution
/ Biochemistry/Protein Chemistry
/ Computational Biology/Comparative Sequence Analysis
/ Computational Biology/Macromolecular Structure Analysis
/ Cytoplasm
/ Evolution
/ G proteins
/ Genetic aspects
/ Hypotheses
/ Mutation
/ Properties
/ Proteins
2010
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Evolution of a Signaling Nexus Constrained by Protein Interfaces and Conformational States
by
Temple, Brenda R. S.
, Jones, Corbin D.
, Jones, Alan M.
in
Analysis
/ Biochemistry/Macromolecular Chemistry
/ Biochemistry/Molecular Evolution
/ Biochemistry/Protein Chemistry
/ Computational Biology/Comparative Sequence Analysis
/ Computational Biology/Macromolecular Structure Analysis
/ Cytoplasm
/ Evolution
/ G proteins
/ Genetic aspects
/ Hypotheses
/ Mutation
/ Properties
/ Proteins
2010
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Evolution of a Signaling Nexus Constrained by Protein Interfaces and Conformational States
by
Temple, Brenda R. S.
, Jones, Corbin D.
, Jones, Alan M.
in
Analysis
/ Biochemistry/Macromolecular Chemistry
/ Biochemistry/Molecular Evolution
/ Biochemistry/Protein Chemistry
/ Computational Biology/Comparative Sequence Analysis
/ Computational Biology/Macromolecular Structure Analysis
/ Cytoplasm
/ Evolution
/ G proteins
/ Genetic aspects
/ Hypotheses
/ Mutation
/ Properties
/ Proteins
2010
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Evolution of a Signaling Nexus Constrained by Protein Interfaces and Conformational States
Journal Article
Evolution of a Signaling Nexus Constrained by Protein Interfaces and Conformational States
2010
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Overview
Heterotrimeric G proteins act as the physical nexus between numerous receptors that respond to extracellular signals and proteins that drive the cytoplasmic response. The Gα subunit of the G protein, in particular, is highly constrained due to its many interactions with proteins that control or react to its conformational state. Various organisms contain differing sets of Gα-interacting proteins, clearly indicating that shifts in sequence and associated Gα functionality were acquired over time. These numerous interactions constrained much of Gα evolution; yet Gα has diversified, through poorly understood processes, into several functionally specialized classes, each with a unique set of interacting proteins. Applying a synthetic sequence-based approach to mammalian Gα subunits, we established a set of seventy-five evolutionarily important class-distinctive residues, sites where a single Gα class is differentiated from the three other classes. We tested the hypothesis that shifts at these sites are important for class-specific functionality. Importantly, we mapped known and well-studied class-specific functionalities from all four mammalian classes to sixteen of our class-distinctive sites, validating the hypothesis. Our results show how unique functionality can evolve through the recruitment of residues that were ancestrally functional. We also studied acquisition of functionalities by following these evolutionarily important sites in non-mammalian organisms. Our results suggest that many class-distinctive sites were established early on in eukaryotic diversification and were critical for the establishment of new Gα classes, whereas others arose in punctuated bursts throughout metazoan evolution. These Gα class-distinctive residues are rational targets for future structural and functional studies.
Publisher
Public Library of Science,Public Library of Science (PLoS)
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