PARP1pred: a web server for screening the bioactivity of inhibitors against DNA repair enzyme PARP-1

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DOI:

https://doi.org/10.17179/excli2022-5602

Keywords:

PARP-1, DNA repair, machine learning, QSAR, webserver, cheminformatics

Abstract

Cancer is the leading cause of death worldwide, resulting in the mortality of more than 10 million people in 2020, according to Global Cancer Statistics 2020. A potential cancer therapy involves targeting the DNA repair process by inhibiting PARP-1. In this study, classification models were constructed using a non-redundant set of 2018 PARP-1 inhibitors. Briefly, compounds were described by 12 fingerprint types and built using the random forest algorithm concomitant with various sampling approaches. Results indicated that PubChem with an oversampling approach yielded the best performance, with a Matthews correlation coefficient > 0.7 while also affording interpretable molecular features. Moreover, feature importance, as determined from the Gini index, revealed that the aromatic/cyclic/heterocyclic moiety, nitrogen-containing fingerprints, and the ether/aldehyde/alcohol moiety were important for PARP-1 inhibition. Finally, our predictive model was deployed as a web application called PARP1pred and is publicly available at https://parp1pred.streamlitapp.com, allowing users to predict the biological activity of query compounds using their SMILES notation as the input. It is anticipated that the model described herein will aid in the discovery of effective PARP-1 inhibitors.

Published

2023-01-05

How to Cite

Lerksuthirat, T., Chitphuk, S., Stitchantrakul, W., Dejsuphong, D., Malik, A. A., & Nantasenamat, C. (2023). PARP1pred: a web server for screening the bioactivity of inhibitors against DNA repair enzyme PARP-1. EXCLI Journal, 22, 84–107. https://doi.org/10.17179/excli2022-5602

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Original articles

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