CORona Drug InTEractions database

Potential inhibitors for 2019-nCoV coronavirus M protease from clinically approved medicines

Xin Liu, Xiu-Jie Wang

Abstract

Starting from December 2019, a novel coronavirus, named 2019-nCoV, was found to cause Severe Acute Respiratory (SARI) symptoms and rapid pandemic in China. With the hope to identify candidate drugs for 2019-nCoV, we adopted a computational approach to screen for available commercial medicines which may function as inhibitors for the Mpro of 2019-nCoV. Up to 10 commercial medicines that may form hydrogen bounds to key residues within the binding pocket of 2019-nCoV Mpro were identified, which may have higher mutation tolerance than lopinavir/ritonavir and may also function as inhibitors for other coronaviruses with similar Mpro binding sites and pocket structures.

Source: BioRxiv

Related molecules

Name	Synonyms	Genes
Epoprostenol
Vapreotide
Perphenazine
Caspofungin Acetate
Bepotastine
Epirubicin
Valrubicin
Colistin
3C-like protease	3CLpro, Mpro, SARS coronavirus main peptidase, 3CLpro-SARS-CoV-2	rep, ORF1a-1b
Aprepitant	Emend
Icatibant

Related interactions

Target	Drug	Type	Result
3C-like protease	Caspofungin Acetate
3C-like protease	Colistin
3C-like protease	Valrubicin
3C-like protease	Aprepitant
3C-like protease	Perphenazine
3C-like protease	Vapreotide
3C-like protease	Epoprostenol
3C-like protease	Epirubicin
3C-like protease	Bepotastine
3C-like protease	Icatibant

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

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Drugs

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Publications

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Clinical trials

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