DrugRepV|Encyclopedia for antivirals

Chemical, Structural, Clinical and Biological details of Antiviral agents ID: DrugRepV_0692

Chemical Information
Antiviral agent ID DrugRepV_0692
Antiviral agent name Amodiaquine
IUPAC Name 4-[(7-chloroquinolin-4-yl)amino]-2-(diethylaminomethyl)phenol
SMILES (canonical) CCN(CC)CC1=C(C=CC(=C1)NC2=C3C=CC(=CC3=NC=C2)Cl)O
Molecular Formula C20H22ClN3O
Molecular Weight (g/mol) 355.87

InChl InChI=1S/C20H22ClN3O/c1-3-24(4-2)13-14-11-16(6-8-20(14)25)23-18-9-10-22-19-12-15(21)5-7-17(18)19/h5-12,25H,3-4,13H2,1-2H3,(H,22,23)

Common Name Amodiaquine

Synonyms Amodiaquina | Amodiaquine | Amodiaquinum
Structural Information

Clinical Information
Category Antiparasitic products, Insectisides and Repellents
Primary Indication (Clinical trial phases) Approved
Biological Information
Primary Indication (Disease Category) Infectious Disease
Primary Indication (Disease) Malaria
Primary Indication (Drug target/Mode of Action) Coagulation factor XIII B chain
Secondary Indication Ebola virus (EBOV) NA EBOLA-eGFP
Secondary Indication (Approaches) Experimental
Secondary Indication (Methods) In-vitro
Secondary Indication (Model system) [cell lines/ animal models] Vero76
Secondary Indication (Mode of viral infection) Adsorption
Secondary Indication (Viral titer) 1.0:0.5 MOI
Secondary Indication (Mode of drug delivery) Culture
Secondary Indication (Time of drug delivery) Pre infection (1 hour)
Secondary Indication (Duration of drug delivery) 48 hours
Secondary Indication (Cell based assay) Fluorescence-based assay
Secondary Indication (Change) No significant effect
Reference Madrid PB, Chopra S, Manger ID, Gilfillan L, Keepers TR, Shurtleff AC, Green CE, Iyer LV, Dilks HH,.A systematic screen of FDA-approved drugs for inhibitors of biological threat agents..PLoS One. 2013;8(4):e60579. doi: 10.1371/journal.pone.0060579. Epub 2013 Apr 5. PMID:23577127
Comment 1012 FDA-approved drugs for off-label broad-spectrum efficacy against Bacillus anthracis; Francisella tularensis; Coxiella burnetii; and Ebola, Marburg, and Lassa fever viruses using in vitro cell culture assays. Multiple virus-specific inhibitors were identified, the most noteworthy antiviral compound identified was chloroquine, which disrupted entry and replication of two or more viruses in vitro and protected mice against Ebola virus challenge in vivo. The feasibility of repurposing existing drugs to face novel threats is demonstrated and this represents the first effort to apply this approach to high containment bacteria and viruses.

Copyright © 2019. CSIR-Institute of Microbial Technology, Chandigarh, INDIA.

Chemical Information
Antiviral agent ID	DrugRepV_0692
Antiviral agent name	Amodiaquine
IUPAC Name	4-[(7-chloroquinolin-4-yl)amino]-2-(diethylaminomethyl)phenol
SMILES (canonical)	CCN(CC)CC1=C(C=CC(=C1)NC2=C3C=CC(=CC3=NC=C2)Cl)O
Molecular Formula	C20H22ClN3O
Molecular Weight (g/mol)	355.87
InChl	InChI=1S/C20H22ClN3O/c1-3-24(4-2)13-14-11-16(6-8-20(14)25)23-18-9-10-22-19-12-15(21)5-7-17(18)19/h5-12,25H,3-4,13H2,1-2H3,(H,22,23)
Common Name	Amodiaquine
Synonyms	Amodiaquina \| Amodiaquine \| Amodiaquinum
Structural Information

Clinical Information
Category	Antiparasitic products, Insectisides and Repellents
Primary Indication (Clinical trial phases)	Approved
Biological Information
Primary Indication (Disease Category)	Infectious Disease
Primary Indication (Disease)	Malaria
Primary Indication (Drug target/Mode of Action)	Coagulation factor XIII B chain
Secondary Indication	Ebola virus (EBOV) NA EBOLA-eGFP
Secondary Indication (Approaches)	Experimental
Secondary Indication (Methods)	In-vitro
Secondary Indication (Model system) [cell lines/ animal models]	Vero76
Secondary Indication (Mode of viral infection)	Adsorption
Secondary Indication (Viral titer)	1.0:0.5 MOI
Secondary Indication (Mode of drug delivery)	Culture
Secondary Indication (Time of drug delivery)	Pre infection (1 hour)
Secondary Indication (Duration of drug delivery)	48 hours
Secondary Indication (Cell based assay)	Fluorescence-based assay
Secondary Indication (Change)	No significant effect
Reference	Madrid PB, Chopra S, Manger ID, Gilfillan L, Keepers TR, Shurtleff AC, Green CE, Iyer LV, Dilks HH,.A systematic screen of FDA-approved drugs for inhibitors of biological threat agents..PLoS One. 2013;8(4):e60579. doi: 10.1371/journal.pone.0060579. Epub 2013 Apr 5. PMID:23577127
Comment	1012 FDA-approved drugs for off-label broad-spectrum efficacy against Bacillus anthracis; Francisella tularensis; Coxiella burnetii; and Ebola, Marburg, and Lassa fever viruses using in vitro cell culture assays. Multiple virus-specific inhibitors were identified, the most noteworthy antiviral compound identified was chloroquine, which disrupted entry and replication of two or more viruses in vitro and protected mice against Ebola virus challenge in vivo. The feasibility of repurposing existing drugs to face novel threats is demonstrated and this represents the first effort to apply this approach to high containment bacteria and viruses.