Prediction of protein oligomer structures using GALAXY in CASP13

Baek, Minkyung; Park, Tae‐Yong; Woo, Hyeonuk; Seok, Chaok

doi:10.1002/prot.25814

Cited by 6 publications

(4 citation statements)

References 39 publications

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“…Even with reasonable subunit structures and interchain contact predictions to guide overall conformational search, small local inaccuracies at the interface can hinder generating correct oligomer structures with ab initio docking. 31 Moreover, as proteins interact with other proteins, their lowest free-energy backbone conformations can shift in response to their partners, complicating typical docking after folding approaches. A "fold-and-dock" method 32 was developed to overcome this limitation, but it is quite computationally expensive as it employs Monte Carlo fragment assembly trajectories.…”

Section: Step 3-2: Gradient-based Fold-and-dockmentioning

confidence: 99%

Protein oligomer modeling guided by predicted interchain contacts in CASP14

et al. 2021

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For CASP14, we developed deep learning-based methods for predicting homo-oligomeric and hetero-oligomeric contacts and used them for oligomer modeling. To build structure models, we developed an oligomer structure generation method that utilizes predicted interchain contacts to guide iterative restrained minimization from random backbone structures. We supplemented this gradient-based fold-and-dock method with templatebased and ab initio docking approaches using deep learning-based subunit predictions on 29 assembly targets. These methods produced oligomer models with summed Z-scores 5.5 units higher than the next best group, with the fold-and-dock method having the best relative performance. Over the eight targets for which this method was used, the best of the five submitted models had average oligomer TM-score of 0.71 (average oligomer TM-score of the next best group: 0.64), and explicit modeling of inter-subunit interactions improved modeling of six out of 40 individual domains (ΔGDT-TS > 2.0).

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Section: Step 3-2: Gradient-based Fold-and-dockmentioning

confidence: 99%

Protein oligomer modeling guided by predicted interchain contacts in CASP14

et al. 2021

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“…Therefore, it is important to elucidate which residues are essential for such molecular interactions to restrain residue positions during the engineering process. Protein-protein interfaces and multimerization can be predicted by protein-protein docking (Baek et al, 2017(Baek et al, , 2019Vangaveti et al, 2020).…”

Section: Module 1: Structure-function Analysis Of Enzymesmentioning

confidence: 99%

Computational Enzyme Engineering Pipelines for Optimized Production of Renewable Chemicals

Scherer

Fleishman

Jones

et al. 2021

Front. Bioeng. Biotechnol.

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To enable a sustainable supply of chemicals, novel biotechnological solutions are required that replace the reliance on fossil resources. One potential solution is to utilize tailored biosynthetic modules for the metabolic conversion of CO2 or organic waste to chemicals and fuel by microorganisms. Currently, it is challenging to commercialize biotechnological processes for renewable chemical biomanufacturing because of a lack of highly active and specific biocatalysts. As experimental methods to engineer biocatalysts are time- and cost-intensive, it is important to establish efficient and reliable computational tools that can speed up the identification or optimization of selective, highly active, and stable enzyme variants for utilization in the biotechnological industry. Here, we review and suggest combinations of effective state-of-the-art software and online tools available for computational enzyme engineering pipelines to optimize metabolic pathways for the biosynthesis of renewable chemicals. Using examples relevant for biotechnology, we explain the underlying principles of enzyme engineering and design and illuminate future directions for automated optimization of biocatalysts for the assembly of synthetic metabolic pathways.

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“…Reviews of these various allergen databases are available (15)(16)(17), in which the features and specific purposes of each resource are described. SDAP for example, can be used to find sequence and structural neighbors for an allergen, and to search for the presence of an epitope (18)(19)(20). AllerML ( 21) is a markup language designed to facilitate exchange of information between databases.…”

Section: Introductionmentioning

confidence: 99%

The COMPARE Database: A Public Resource for Allergen Identification, Adapted for Continuous Improvement

et al. 2021

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Motivation: The availability of databases identifying allergenic proteins via a transparent and consensus-based scientific approach is of prime importance to support the safety review of genetically-modified foods and feeds, and public safety in general. Over recent years, screening for potential new allergens sequences has become more complex due to the exponential increase of genomic sequence information. To address these challenges, an international collaborative scientific group coordinated by the Health and Environmental Sciences Institute (HESI), was tasked to develop a contemporary, adaptable, high-throughput process to build the COMprehensive Protein Allergen REsource (COMPARE) database, a publicly accessible allergen sequence data resource along with bioinformatics analytical tools following guidelines of FAO/WHO and CODEX Alimentarius Commission.Results: The COMPARE process is novel in that it involves the identification of candidate sequences via automated keyword-based sorting algorithm and manual curation of the annotated sequence entries retrieved from public protein sequence databases on a yearly basis; its process is meant for continuous improvement, with updates being transparently documented with each version; as a complementary approach, a yearly key-word based search of literature databases is added to identify new allergen sequences that were not (yet) submitted to protein databases; in addition, comments from the independent peer-review panel are posted on the website to increase transparency of decision making; finally, sequence comparison capabilities associated with the COMPARE database was developed to evaluate the potential allergenicity of proteins, based on internationally recognized guidelines, FAO/WHO and CODEX Alimentarius Commission

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Prediction of protein oligomer structures using GALAXY in CASP13

Cited by 6 publications

References 39 publications

Protein oligomer modeling guided by predicted interchain contacts in CASP14

Protein oligomer modeling guided by predicted interchain contacts in CASP14

Computational Enzyme Engineering Pipelines for Optimized Production of Renewable Chemicals

The COMPARE Database: A Public Resource for Allergen Identification, Adapted for Continuous Improvement

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