Understanding the physical attributes of protein-ligand interfaces, the source of most biological activity, is a fundamental problem in biophysics. Knowing the characteristic features of interfaces also enables the design of molecules with potent and selective interactions. Prediction of native protein-ligand interactions has traditionally focused on the development of physics-based potential energy functions, empirical scoring functions that are fit to binding data, and knowledge-based potentials that assess the likelihood of pairwise interactions. Here we explore a new approach, testing the hypothesis that protein-ligand binding results in computationally detectable rigidification of the protein-ligand interface. Our SiteInterlock approach uses rigidity theory to efficiently measure the relative interfacial rigidity of a series of small-molecule ligand orientations and conformations for a number of protein complexes. In the majority of cases, SiteInterlock detects a near-native binding mode as being the most rigid, with particularly robust performance relative to other methods when the ligand-free conformation of the protein is provided. The interfacial rigidification of both the protein and ligand prove to be important characteristics of the native binding mode. This measure of rigidity is also sensitive to the spatial coupling of interactions and bond-rotational degrees of freedom in the interface. While the predictive performance of SiteInterlock is competitive with the best of the five other scoring functions tested, its measure of rigidity encompasses cooperative rather than just additive binding interactions, providing novel information for detecting native-like complexes. SiteInterlock shows special strength in enhancing the prediction of native complexes by ruling out inaccurate poses. Proteins 2016; 84:1888-1901. © 2016 Wiley Periodicals, Inc.
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Adv Healthc Mater
December 2024
John A. Paulson School of Engineering and Applied Sciences, Harvard University, Cambridge, MA, 02138, USA.
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December 2024
CAS Key Laboratory of Bio-inspired Materials and Interfacial Science, Technical Institute of Physics and Chemistry, Chinese Academy of Sciences, Beijing 100190, China.
Numerous organisms exploit asymmetrical capillary forces generated by unique fiber or asymmetrical tapered structures to rapidly eliminate undesired liquid for survival in moist or rainy habitats. Human eyelashes, the primary protector of eyes, use a yet-to-be-fully-understood mechanism to efficiently transfer incoming liquid for vision safeguarding. Here, we elucidate that human eyelashes featuring a hydrophobic curved flexible fiber array with surface micro-ratchet and macro-curvature approximating the is adept at directionally and rapidly expelling incoming liquid to maintain clear vision.
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Microcellular Plastics Manufacturing Laboratory, Department of Mechanical and Industrial Engineering, University of Toronto, Toronto, Ontario M5S 3G8, Canada.
In this study, we proposed a novel technique to simultaneously enhance the oxygen barrier properties and stiffness of high-density polyethylene (HDPE) while preserving its ductility. By utilizing in situ nanofibrillation, fiber-in-fiber composites of an HDPE matrix and ethylene-vinyl alcohol (EVOH) nanofibers were fabricated. Due to the high interfacial tension between HDPE and EVOH, stemming from their differences in chemical structure and polarity, styrene/ethylene-butylene/styrene copolymer grafted with maleic anhydride (SEBS--MA) was used as a compatibilizer to improve the affinity between the two polymers.
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December 2024
Department of Physics and Texas Center for Superconductivity at the University of Houston (TcSUH), University of Houston, Houston, TX, 77204, USA.
J Am Chem Soc
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College of Materials Science and Technology, Nanjing University of Aeronautics and Astronautics, Nanjing 210016, China.
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