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DisruPPI: structure-based computational redesign algorithm for protein binding disruption

https://doi.org/10.1093/bioinformatics/bty274

Choi, Yoonjoo ; Furlon, Jacob M. ; Amos, Ryan B. ; Griswold, Karl E. ; Bailey-Kellogg, Chris ( June 2018 , Bioinformatics)

Abstract Motivation
Disruption of protein–protein interactions can mitigate antibody recognition of therapeutic proteins, yield monomeric forms of oligomeric proteins, and elucidate signaling mechanisms, among other applications. While designing affinity-enhancing mutations remains generally quite challenging, both statistically and physically based computational methods can precisely identify affinity-reducing mutations. In order to leverage this ability to design variants of a target protein with disrupted interactions, we developed the DisruPPI protein design method (DISRUpting Protein–Protein Interactions) to optimize combinations of mutations simultaneously for both disruption and stability, so that incorporated disruptive mutations do not inadvertently affect the target protein adversely.
Results
Two existing methods for predicting mutational effects on binding, FoldX and INT5, were demonstrated to be quite precise in selecting disruptive mutations from the SKEMPI and AB-Bind databases of experimentally determined changes in binding free energy. DisruPPI was implemented to use an INT5-based disruption score integrated with an AMBER-based stability assessment and was applied to disrupt protein interactions in a set of different targets representing diverse applications. In retrospective evaluation with three different case studies, comparison of DisruPPI-designed variants to published experimental data showed that DisruPPI was able to identify more diverse interaction-disrupting and stability-preserving variants more efficiently and effectively than previous approaches. In prospective application to an interaction between enhanced green fluorescent protein (EGFP) and a nanobody, DisruPPI was used to design five EGFP variants, all of which were shown to have significantly reduced nanobody binding while maintaining function and thermostability. This demonstrates that DisruPPI may be readily utilized for effective removal of known epitopes of therapeutically relevant proteins.
Availability and implementation
DisruPPI is implemented in the EpiSweep package, freely available under an academic use license.
Supplementary information
Supplementary data are available at Bioinformatics online.

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Ensuring scientific reproducibility in bio-macromolecular modeling via extensive, automated benchmarks

https://doi.org/10.1038/s41467-021-27222-7

Koehler Leman, Julia ; Lyskov, Sergey ; Lewis, Steven M. ; Adolf-Bryfogle, Jared ; Alford, Rebecca F. ; Barlow, Kyle ; Ben-Aharon, Ziv ; Farrell, Daniel ; Fell, Jason ; Hansen, William A. ; et al ( December 2021 , Nature Communications)

Abstract Each year vast international resources are wasted on irreproducible research. The scientific community has been slow to adopt standard software engineering practices, despite the increases in high-dimensional data, complexities of workflows, and computational environments. Here we show how scientific software applications can be created in a reproducible manner when simple design goals for reproducibility are met. We describe the implementation of a test server framework and 40 scientific benchmarks, covering numerous applications in Rosetta bio-macromolecular modeling. High performance computing cluster integration allows these benchmarks to run continuously and automatically. Detailed protocol captures are useful for developers and users of Rosetta and other macromolecular modeling tools. The framework and design concepts presented here are valuable for developers and users of any type of scientific software and for the scientific community to create reproducible methods. Specific examples highlight the utility of this framework, and the comprehensive documentation illustrates the ease of adding new tests in a matter of hours.
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Computationally optimized deimmunization libraries yield highly mutated enzymes with low immunogenicity and enhanced activity

https://doi.org/10.1073/pnas.1621233114

Salvat, Regina S. ; Verma, Deeptak ; Parker, Andrew S. ; Kirsch, Jack R. ; Brooks, Seth A. ; Bailey-Kellogg, Chris ; Griswold, Karl E. ( June 2017 , Proceedings of the National Academy of Sciences)