Evolutionary Multi-Objective Design of SARS-CoV-2 Protease Inhibitor
  Candidates

A Alhossary; CA Lipinski; CA Nicolaou; D Douguet; D Weininger; E van der Horst; E Zitzler; GR Bickerton; H Nguyen; HG Beyer; K Deb; L Zhang; N Brown; N Brown; O Trott; P Ertl; P Ertl; RF de Freitas; RV Devi; SCH Pegg; SS Kaplan; T Gaillard; T Krause; TT Wager; W Dai

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Evolutionary Multi-Objective Design of SARS-CoV-2 Protease Inhibitor Candidates

Authors: A Alhossary
CA Lipinski
CA Nicolaou
D Douguet
D Weininger
E van der Horst
E Zitzler
GR Bickerton
H Nguyen
HG Beyer
K Deb
L Zhang
N Brown
N Brown
O Trott
P Ertl
P Ertl
RF de Freitas
RV Devi
SCH Pegg
SS Kaplan
T Gaillard
T Krause
TT Wager
W Dai
Publication date: 18 May 2020
Publisher: 'Springer Science and Business Media LLC'
Doi

Abstract

Computational drug design based on artificial intelligence is an emerging research area. At the time of writing this paper, the world suffers from an outbreak of the coronavirus SARS-CoV-2. A promising way to stop the virus replication is via protease inhibition. We propose an evolutionary multi-objective algorithm (EMOA) to design potential protease inhibitors for SARS-CoV-2's main protease. Based on the SELFIES representation the EMOA maximizes the binding of candidate ligands to the protein using the docking tool QuickVina 2, while at the same time taking into account further objectives like drug-likeliness or the fulfillment of filter constraints. The experimental part analyzes the evolutionary process and discusses the inhibitor candidates.Comment: 15 pages, 7 figures, submitted to PPSN 202

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