CORona Drug InTEractions database

Potentially highly potent drugs for 2019-nCoV

Duc Duy Nguyen, Kaifu Gao, Jiahui Chen, Rui Wang, Guo-Wei Wei

Abstract

The World Health Organization (WHO) has declared the 2019 novel coronavirus (2019-nCoV) infection outbreak a global health emergency. Currently, there is no effective anti-2019-nCoV medication. The sequence identity of the 3CL proteases of 2019-nCoV and SARS is 96%, which provides a sound foundation for structural-based drug repositioning (SBDR). Based on a SARS 3CL protease X-ray crystal structure, we construct a 3D homology structure of 2019-nCoV 3CL protease. Based on this structure and existing experimental datasets for SARS 3CL protease inhibitors, we develop an SBDR model based on machine learning and mathematics to screen 1465 drugs in the DrugBank that have been approved by the U.S. Food and Drug Administration (FDA). We found that many FDA approved drugs are potentially highly potent to 2019-nCoV.

Source: BioRxiv

Related molecules

Name	Synonyms	Genes
Flurazepam	Dalmane, Dalmadorm, Fluzepam
Paramethasone	Cortidene Depot, Dilar, Dilarmine
Clocortolone	Victrelis
Flucloxacillin	Flora, Flox, Floxapen
Sertindole	Serdolect and Serlect
Clevidipine	Cleviprex
Cinolazepam	Gerodorm
Ponatinib	Iclusig
Fosaprepitant	Emend, Ivemend
Clofazimine	Lamprene
3C-like protease	3CLpro, Mpro, SARS coronavirus main peptidase, 3CLpro-SARS-CoV-2	rep, ORF1a-1b
Dasatinib	Sprycel, Dasanix
Aprepitant	Emend
Atorvastatin	Lipitor, Sortis
Bortezomib	Velcade, Chemobort, Bortecad
Sorafenib	Nexavar

Related interactions

Target	Drug	Type	Result
3C-like protease	Flurazepam
3C-like protease	Ponatinib
3C-like protease	Sorafenib
3C-like protease	Paramethasone
3C-like protease	Clocortolone
3C-like protease	Flucloxacillin
3C-like protease	Sertindole
3C-like protease	Clevidipine
3C-like protease	Cinolazepam
3C-like protease	Clofazimine
3C-like protease	Fosaprepitant
3C-like protease	Dasatinib
3C-like protease	Aprepitant
3C-like protease	Atorvastatin
3C-like protease	Bortezomib

Target	Target affiliation	Drug	Type	Result
Target	Target affiliation	Drug	Type	Result

Name	Synonyms	Genes	Origin
Name	Synonyms	Genes	Origin

Name	Synonyms	PubChem	DrugBank	RCSB PDB	ATC
Name	Synonyms	PubChem	DrugBank	RCSB PDB	ATC

Title	Authors	DOI	Source	Article type	Date
Title	Authors	DOI	Source	Article type	Date

Title	Status	Phases	Start Date	Prim. Comp. Date	Comp. Date	First Post. Date
Title	Status	Phases	Start Date	Prim. Comp. Date	Comp. Date	First Post. Date

CORDITE (CORona Drug InTEractions database) collects and aggregates data from PubMed, MedRxiv, BioRxiv, ChemRxiv and PMC for SARS-CoV-2. Its main focus is set on drug interactions either addressing viral proteins or human proteins that could be used to treat COVID. It collects and provides up-to-date information on computational predictions, in vitro, as well as in vivo study data.

The information provided is for research only and we cannot guarantee the correctness of the data.

Please contact dominik.heider@uni-muenster.de for further information.

Programmable access

There is an open API for access programmatically to the database. The API will print a JSON output:

Interactions

https://cordite-api.uni-muenster.de/api.php?action=list&table=interaction

Targets

https://cordite-api.uni-muenster.de/api.php?action=list&table=target

Drugs

https://cordite-api.uni-muenster.de/api.php?action=list&table=drug

Publications

https://cordite-api.uni-muenster.de/api.php?action=list&table=publication

Clinical trials

https://cordite-api.uni-muenster.de/api.php?action=list&table=clinical_trial