1. Academic Validation
  2. Development of Machine Learning Models and the Discovery of a New Antiviral Compound against Yellow Fever Virus

Development of Machine Learning Models and the Discovery of a New Antiviral Compound against Yellow Fever Virus

  • J Chem Inf Model. 2021 Aug 23;61(8):3804-3813. doi: 10.1021/acs.jcim.1c00460.
Victor O Gawriljuk 1 Daniel H Foil 2 Ana C Puhl 2 Kimberley M Zorn 2 Thomas R Lane 2 Olga Riabova 3 Vadim Makarov 3 Andre S Godoy 1 Glaucius Oliva 1 Sean Ekins 2
Affiliations

Affiliations

  • 1 São Carlos Institute of Physics, University of São Paulo, Av. João Dagnone, 1100 - Santa Angelina, São Carlos, São Paulo 13563-120, Brazil.
  • 2 Collaborations Pharmaceuticals, Inc., 840 Main Campus Drive, Lab 3510, Raleigh, North Carolina 27606, United States.
  • 3 Research Center of Biotechnology RAS, Leninsky Prospekt 33-2, 119071 Moscow, Russia.
Abstract

Yellow fever (YF) is an acute viral hemorrhagic disease transmitted by infected mosquitoes. Large epidemics of YF occur when the virus is introduced into heavily populated areas with high mosquito density and low vaccination coverage. The lack of a specific small molecule drug treatment against YF as well as for homologous infections, such as zika and dengue, highlights the importance of these flaviviruses as a public health concern. With the advancement in computer hardware and bioactivity data availability, new tools based on machine learning methods have been introduced into drug discovery, as a means to utilize the growing high throughput screening (HTS) data generated to reduce costs and increase the speed of drug development. The use of predictive machine learning models using previously published data from HTS campaigns or data available in public databases, can enable the selection of compounds with desirable bioactivity and absorption, distribution, metabolism, and excretion profiles. In this study, we have collated cell-based assay data for yellow fever virus from the literature and public databases. The data were used to build predictive models with several machine learning methods that could prioritize compounds for in vitro testing. Five molecules were prioritized and tested in vitro from which we have identified a new pyrazolesulfonamide derivative with EC50 3.2 μM and CC50 24 μM, which represents a new scaffold suitable for hit-to-lead optimization that can expand the available drug discovery candidates for YF.

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