toxCSM: comprehensive prediction of small molecule toxicity profiles

Sá, Alex Guimarães Cardoso de; Long, Yangyang; Portelli, Stephanie; Pires, Douglas E V; Ascher, David B.

doi:10.1093/bib/bbac337

Cited by 18 publications

(11 citation statements)

References 49 publications

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“…Users can identify CDK2 inhibitors, predict CDK2 pK i and possible binding modes by providing a single molecule or a list of molecules as SMILES strings (Figure 5 ). Moreover, users can also predict the toxicity profiles via toxCSM, 32 and selectivity profiles via SwissTarget 33 by clicking on the links on the result page to further prioritize safer, less toxic, and more selective CDK2 inhibitors for clinical usage.…”

Section: Resultsmentioning

confidence: 99%

“…Results are presented in a table, including predictions on CDK2 inhibitor (Yes or No), CDK2 pK i , binding modes based on different binary classifiers, and final decisions. Users also have the choice to show molecule depiction and properties via visualization controls, as well as redirecting to toxicity and selectivity predictions by toxCSM 32 and SwissTarget, 33 respectively…”

Section: Resultsmentioning

confidence: 99%

“…To address this Results are presented in a table, including predictions on CDK2 inhibitor (Yes or No), CDK2 pK i , binding modes based on different binary classifiers, and final decisions. Users also have the choice to show molecule depiction and properties via visualization controls, as well as redirecting to toxicity and selectivity predictions by toxCSM 32 and SwissTarget, 33 respectively problem, in our work, the datasets were split into lowredundancy training (70%) and blind test (30%). We ensured the molecules in the training and blind test sets have similar label distribution but are in different similarity clusters.…”

Section: Datasetsmentioning

confidence: 99%

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kinCSM: Using graph‐based signatures to predict small molecule CDK2 inhibitors

et al. 2022

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Protein phosphorylation acts as an essential on/off switch in many cellular signaling pathways. This has led to ongoing interest in targeting kinases for therapeutic intervention. Computer‐aided drug discovery has been proven a useful and cost‐effective approach for facilitating prioritization and enrichment of screening libraries, but limited effort has been devoted providing insights on what makes a potent kinase inhibitor. To fill this gap, here we developed kinCSM, an integrative computational tool capable of accurately identifying potent cyclin‐dependent kinase 2 (CDK2) inhibitors, quantitatively predicting CDK2 ligand–kinase inhibition constants (pKi) and classifying different types of inhibitors based on their favorable binding modes. kinCSM predictive models were built using supervised learning and leveraged the concept of graph‐based signatures to capture both physicochemical properties and geometry properties of small molecules. CDK2 inhibitors were accurately identified with Matthew's Correlation Coefficients (MCC) of up to 0.74, and inhibition constants predicted with Pearson's correlation of up to 0.76, both with consistent performances of 0.66 and 0.68 on a nonredundant blind test, respectively. kinCSM was also able to identify the potential type of inhibition for a given molecule, achieving MCC of up to 0.80 on cross‐validation and 0.73 on the blind test. Analyzing the molecular composition of revealed enriched chemical fragments in CDK2 inhibitors and different types of inhibitors, which provides insights into the molecular mechanisms behind ligand–kinase interactions. kinCSM will be an invaluable tool to guide future kinase drug discovery. To aid the fast and accurate screening of CDK2 inhibitors, kinCSM is freely available at https://biosig.lab.uq.edu.au/kin_csm/.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Datasetsmentioning

confidence: 99%

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kinCSM: Using graph‐based signatures to predict small molecule CDK2 inhibitors

et al. 2022

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“…The atom pharmacophores are characteristics belonging to eight possible classes: hydrophobic, positive, negative, hydrogen acceptor, hydrogen donor, aromatic, sulfur, and neutral. These signatures have shown to be an effective and efficient method to model protein residue environment, its geometry and physicochemical properties, information that has been used to predict the effects of mutations on protein stability and affinity to its partners (Myung, Pires, & Ascher, 2020 ; Myung, Rodrigues, et al, 2020 ; Nguyen et al, 2021 ; Pires et al, 2014 , 2016 ; Pires & Ascher, 2016 , 2017 ; Rodrigues et al, 2019 , 2021a ; 2021b , 2024 ; Rodrigues & Ascher, 2022 , 2023 ; Ryu et al, 2023 ), pharmacodynamic and pharmacokinetics (Al‐Jarf et al, 2021 ; de Sa et al, 2022 ; Iftkhar et al, 2022 ; Morozov et al, 2023 ; Pires et al, 2015 , 2022 ; Pires & Ascher, 2020 ; Rodrigues et al, 2021c , 2022 ; Velloso et al, 2021 ), and identify drug resistance (Hawkey et al, 2018 ; Karmakar et al, 2018 , 2019 , 2020 ; Portelli et al, 2020 ; Portelli, Heaton, & Ascher, 2023 ; Zhan et al, 2021 ; Zhou et al, 2021 ) and disease mutations (Jessen‐Howard et al, 2023 ; Karmakar et al, 2022 ; Lai et al, 2021 ; Portelli et al, 2021 ; Portelli, Albanaz, et al, 2023 ).…”

Section: Methodsmentioning

confidence: 99%

Engineering G protein‐coupled receptors for stabilization

Velloso,

de Sá,

Pires

et al. 2024

Protein Science

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G protein‐coupled receptors (GPCRs) are one of the most important families of targets for drug discovery. One of the limiting steps in the study of GPCRs has been their stability, with significant and time‐consuming protein engineering often used to stabilize GPCRs for structural characterization and drug screening. Unfortunately, computational methods developed using globular soluble proteins have translated poorly to the rational engineering of GPCRs. To fill this gap, we propose GPCR‐tm, a novel and personalized structurally driven web‐based machine learning tool to study the impacts of mutations on GPCR stability. We show that GPCR‐tm performs as well as or better than alternative methods, and that it can accurately rank the stability changes of a wide range of mutations occurring in various types of class A GPCRs. GPCR‐tm achieved Pearson's correlation coefficients of 0.74 and 0.46 on 10‐fold cross‐validation and blind test sets, respectively. We observed that the (structural) graph‐based signatures were the most important set of features for predicting destabilizing mutations, which points out that these signatures properly describe the changes in the environment where the mutations occur. More specifically, GPCR‐tm was able to accurately rank mutations based on their effect on protein stability, guiding their rational stabilization. GPCR‐tm is available through a user‐friendly web server at https://biosig.lab.uq.edu.au/gpcr_tm/.

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“…While significant effort has been invested into the prediction and optimisation of peptides and proteins, the assessment of toxicity typically relies on expensive and time-consuming in-vivo assays late in the development process. Comparatively, we have seen that the introduction of rules and predictive algorithms to assess small molecule toxicities has helped to significantly reduce clinical trial failures [ 2 , 3 , 4 , 5 ].…”

Section: Introductionmentioning

confidence: 99%

CSM-Toxin: A Web-Server for Predicting Protein Toxicity

2023

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Biologics are one of the most rapidly expanding classes of therapeutics, but can be associated with a range of toxic properties. In small-molecule drug development, early identification of potential toxicity led to a significant reduction in clinical trial failures, however we currently lack robust qualitative rules or predictive tools for peptide- and protein-based biologics. To address this, we have manually curated the largest set of high-quality experimental data on peptide and protein toxicities, and developed CSM-Toxin, a novel in-silico protein toxicity classifier, which relies solely on the protein primary sequence. Our approach encodes the protein sequence information using a deep learning natural languages model to understand “biological” language, where residues are treated as words and protein sequences as sentences. The CSM-Toxin was able to accurately identify peptides and proteins with potential toxicity, achieving an MCC of up to 0.66 across both cross-validation and multiple non-redundant blind tests, outperforming other methods and highlighting the robust and generalisable performance of our model. We strongly believe the CSM-Toxin will serve as a valuable platform to minimise potential toxicity in the biologic development pipeline. Our method is freely available as an easy-to-use webserver.

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toxCSM: comprehensive prediction of small molecule toxicity profiles

Cited by 18 publications

References 49 publications

kinCSM: Using graph‐based signatures to predict small molecule CDK2 inhibitors

kinCSM: Using graph‐based signatures to predict small molecule CDK2 inhibitors

Engineering G protein‐coupled receptors for stabilization

CSM-Toxin: A Web-Server for Predicting Protein Toxicity

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