Allosteric communication occurs via networks of tertiary and quaternary motions in proteins
| Autor: | Jeffrey J. Gray, Michael D. Daily |
|---|---|
| Jazyk: | angličtina |
| Rok vydání: | 2009 |
| Předmět: |
Biophysics/Theory and Simulation
Models Molecular Allosteric regulation Computational Biology/Macromolecular Structure Analysis Computational biology DNA-binding protein Motion Structure-Activity Relationship 03 medical and health sciences Cellular and Molecular Neuroscience Protein structure Biophysics/Macromolecular Assemblies and Machines Allosteric Regulation Protein Interaction Mapping Genetics Biophysics/Biocatalysis Binding site Databases Protein Protein Structure Quaternary Molecular Biology lcsh:QH301-705.5 Ecology Evolution Behavior and Systematics Topology (chemistry) 030304 developmental biology 0303 health sciences Binding Sites Ecology biology Effector 030302 biochemistry & molecular biology Proteins Enzyme structure Protein Structure Tertiary Models Chemical Nonlinear Dynamics Computational Theory and Mathematics Biochemistry Allosteric enzyme lcsh:Biology (General) Modeling and Simulation biology.protein Thermodynamics Biophysics/Biomacromolecule-Ligand Interactions Research Article |
| Zdroj: | PLoS Computational Biology, Vol 5, Iss 2, p e1000293 (2009) PLoS Computational Biology |
| ISSN: | 1553-7358 |
| Popis: | Allosteric proteins bind an effector molecule at one site resulting in a functional change at a second site. We hypothesize that allosteric communication in proteins relies upon networks of quaternary (collective, rigid-body) and tertiary (residue–residue contact) motions. We argue that cyclic topology of these networks is necessary for allosteric communication. An automated algorithm identifies rigid bodies from the displacement between the inactive and the active structures and constructs “quaternary networks” from these rigid bodies and the substrate and effector ligands. We then integrate quaternary networks with a coarse-grained representation of contact rearrangements to form “global communication networks” (GCNs). The GCN reveals allosteric communication among all substrate and effector sites in 15 of 18 multidomain and multimeric proteins, while tertiary and quaternary networks exhibit such communication in only 4 and 3 of these proteins, respectively. Furthermore, in 7 of the 15 proteins connected by the GCN, 50% or more of the substrate-effector paths via the GCN are “interdependent” paths that do not exist via either the tertiary or the quaternary network. Substrate-effector “pathways” typically are not linear but rather consist of polycyclic networks of rigid bodies and clusters of rearranging residue contacts. These results argue for broad applicability of allosteric communication based on structural changes and demonstrate the utility of the GCN. Global communication networks may inform a variety of experiments on allosteric proteins as well as the design of allostery into non-allosteric proteins. Author Summary Allosteric regulation is a major mechanism of control in many biological processes, including cell signaling, gene regulation, and metabolic regulation, and malfunctioning allosteric proteins are often involved in cancer and other diseases. In allostery, an effector-binding signal transmits over a long distance through the protein structure, resulting in a functional change at a second site. While many three-dimensional structures of allosteric proteins have been solved, the allosteric communication mechanism is usually not obvious from the motions between inactive and active state structures. In addition, allosteric structural transitions involve both small-scale motions at the level of amino acid residues and large-scale motions at the level of domains. Here, to address allosteric mechanisms, we transform the aforementioned protein motions into a multi-scale “global communication network” (GCN) representation from which substrate-effector pathways and other important allosteric communication properties can be identified. The GCN accounts for substrate-effector pathways in 15 of 18 proteins surveyed, and the GCN reveals that allostery often depends on linkage between the small- and the large-scale motions. This work will inform a wide variety of experiments investigating allostery, and it proposes concepts for engineering allostery into non-allosteric proteins. |
| Databáze: | OpenAIRE |
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