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Andrew Leaver‐Fay

University of North Carolina at Chapel Hill

ORCID: 0000-0003-4609-4340

Publishes on Protein Structure and Dynamics, Enzyme Structure and Function, RNA and protein synthesis mechanisms. 74 papers and 13.8k citations.

74Publications
13.8kTotal Citations
Protein Structure and DynamicsEnzyme Structure and FunctionRNA and protein synthesis mechanismsMonoclonal and Polyclonal Antibodies ResearchGlycosylation and Glycoproteins Research

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Top publicationsby citations

MolProbity: all-atom contacts and structure validation for proteins and nucleic acids
Ian Davis, Andrew Leaver‐Fay, V. B. Chen et al.|Nucleic Acids Research|2007
Cited by 4kOpen Access

MolProbity is a general-purpose web server offering quality validation for 3D structures of proteins, nucleic acids and complexes. It provides detailed all-atom contact analysis of any steric problems within the molecules as well as updated dihedral-angle diagnostics, and it can calculate and display the H-bond and van der Waals contacts in the interfaces between components. An integral step in the process is the addition and full optimization of all hydrogen atoms, both polar and nonpolar. New analysis functions have been added for RNA, for interfaces, and for NMR ensembles. Additionally, both the web site and major component programs have been rewritten to improve speed, convenience, clarity and integration with other resources. MolProbity results are reported in multiple forms: as overall numeric scores, as lists or charts of local problems, as downloadable PDB and graphics files, and most notably as informative, manipulable 3D kinemage graphics shown online in the KiNG viewer. This service is available free to all users at http://molprobity.biochem.duke.edu.

The Rosetta All-Atom Energy Function for Macromolecular Modeling and Design
Rebecca F. Alford, Andrew Leaver‐Fay, Jeliazko R. Jeliazkov et al.|Journal of Chemical Theory and Computation|2017
Cited by 1.6k

Over the past decade, the Rosetta biomolecular modeling suite has informed diverse biological questions and engineering challenges ranging from interpretation of low-resolution structural data to design of nanomaterials, protein therapeutics, and vaccines. Central to Rosetta's success is the energy function: a model parametrized from small-molecule and X-ray crystal structure data used to approximate the energy associated with each biomolecule conformation. This paper describes the mathematical models and physical concepts that underlie the latest Rosetta energy function, called the Rosetta Energy Function 2015 (REF15). Applying these concepts, we explain how to use Rosetta energies to identify and analyze the features of biomolecular models. Finally, we discuss the latest advances in the energy function that extend its capabilities from soluble proteins to also include membrane proteins, peptides containing noncanonical amino acids, small molecules, carbohydrates, nucleic acids, and other macromolecules.