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Effects of Ligand Binding on the Mechanical Properties of Ankyrin Repeat Protein Gankyrin
Authors:Giovanni Settanni  David Serquera  Piotr E Marszalek  Emanuele Paci  Laura S Itzhaki
Institution:1.Physics Department, Johannes Gutenberg University, Mainz, Germany;2.MRC Cancer Cell Unit, Hutchison/MRC Research Centre, Cambridge, United Kingdom;3.Department of Mechanical Engineering and Materials Science, Duke University, Durham, North Carolina, United States of America;4.School of Molecular and Cellular Biology, University of Leeds, Leeds, United Kingdom;5.University of Cambridge Department of Chemistry, Cambridge, United Kingdom;University of Missouri, United States of America
Abstract:Ankyrin repeat proteins are elastic materials that unfold and refold sequentially, repeat by repeat, under force. Herein we use atomistic molecular dynamics to compare the mechanical properties of the 7-ankyrin-repeat oncoprotein Gankyrin in isolation and in complex with its binding partner S6-C. We show that the bound S6-C greatly increases the resistance of Gankyrin to mechanical stress. The effect is specific to those repeats of Gankyrin directly in contact with S6-C, and the mechanical ‘hot spots’ of the interaction map to the same repeats as the thermodynamic hot spots. A consequence of stepwise nature of unfolding and the localized nature of ligand binding is that it impacts on all aspects of the protein''s mechanical behavior, including the order of repeat unfolding, the diversity of unfolding pathways accessed, the nature of partially unfolded intermediates, the forces required and the work transferred to the system to unfold the whole protein and its parts. Stepwise unfolding thus provides the means to buffer repeat proteins and their binding partners from mechanical stress in the cell. Our results illustrate how ligand binding can control the mechanical response of proteins. The data also point to a cellular mechano-switching mechanism whereby binding between two partner macromolecules is regulated by mechanical stress.
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