Compound Libraries 3CLpro-Targeted Compound Library (CADD)

3CLpro-Targeted Compound Library (CADD)

Catalog No. L1712
  Library Compound List   Excel SDF

The 3CLpro (Mpro), also known as Nsp5, is first automatically cleaved from poly-proteins to produce mature enzymes, and then further cleaves downstream Nsps at 11 sites to release Nsp4–Nsp1631. 3CLpro directly mediates the maturation of Nsps, which is essential in the life cycle of the virus. The detailed investigation on the structure and catalytic mechanism of 3CLpro makes 3CLpro an attractive target for anti-coronavirus drug development. Inhibitors targeting at SARS-CoV 3CLpro mainly include peptide inhibitors and small-molecule inhibitors.

Based on the protein structure of 3CLpro, we selected 161 top-ranked docked molecules into 3CLpro-Targeted Compound Library (CADD) by molecular docking virtual screening against 15,376 compound structures. To speed up the research and development of anti-SARS-CoV-2 drugs, we provide the virtual screening result for free!

Pack Size Price/USD
100 μL * 10 mM (in DMSO) 2660.00
If the above compound libraries do not match your needs,
please contact our compound library specialist for a customized compound library at [email protected]
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Product Description

  • A unique collection of 161 compounds having the potential of anti-SARS-CoV-2 activity, can be used for high throughput screening and high content screening;
  • Top-ranked docked compounds targeting 3CLpro will improve the hit success rate;
  • Detailed compound information with structure, target, and biological activity description;
  • NMR and HPLC validated to ensure high purity and quality.

Library Customization

Targetmol Compound Libraries can be highly customized! Learn More

Packaging And Storage

  • Powder or pre-dissolved DMSO solutions in 96/384 well plate with optional 2D barcode
  • Shipped with blue ice
Request Library Compound List (L1712)

Library Composition

Histone Methyltransferase (7)
Beta-lactamase AmpC (7)
HEK293 (5)
Nuclear factor erythroid 2-related factor 2 (5)
Mothers against decapentaplegic homolog 3 (5)
Thyroid hormone receptor beta-1 (4)
TAR DNA-binding protein 43 (4)
RAAS (3)
PDE (3)
Plasmodium falciparum (3)
Prelamin-A/C (3)
Prostaglandin Receptor (3)
Nonstructural protein 1 (3)
Microtubule-associated protein tau (3)
AChR (3)
Antibiotic (3)
Endogenous Metabolite (3)
Geminin (3)
Glucagon-like peptide 1 receptor (2)
GSK-3 (2)
Guanine nucleotide-binding protein G(s), subunit alpha (2)
Ataxin-2 (2)
ATPase family AAA domain-containing protein 5 (2)
DNA/RNA Synthesis (2)
Dopamine Receptor (2)
Antioxidant (2)
Cellular tumor antigen p53 (2)
5-HT Receptor (2)
Phospholipase (2)
Src (2)
TAM Receptor (2)
Topoisomerase (2)
Trk receptor (1)
Virus Protease (1)
Wnt/beta-catenin (1)
ribosome (1)
Short transient receptor potential channel 4 (1)
PKC (1)
PED (1)
Proteasome (1)
PPAR (1)
Histone Acetyltransferase (1)
HMG-CoA Reductase (1)
JAK (1)
Kinesin (1)
Lipase (1)
LTR (1)
Norepinephrine (1)
NF-κB (1)
Nuclear receptor ROR-gamma (1)
P450 (1)
p53 (1)
c-Met/HGFR (1)
COX (1)
CXCR (1)
Cysteine Protease (1)
Dehydrogenase (1)
DNA polymerase iota (1)
Bradykinin Receptor (1)
Calcium Channel (1)
Caspase (1)
CDK (1)
Arachidonate 15-lipoxygenase (1)
Ataxin (1)
ACK (1)
Adrenergic Receptor (1)
Amino Acids and Derivatives (1)
Antibacterial (1)
E1/E2/E3 Enzyme (1)
ATP-dependent Clp protease proteolytic subunit (1)
Epigenetic Reader Domain (1)
ERK (1)
Estrogen/progestogen Receptor (1)
Fatty Acid Synthase (1)
Guanylate cyclase (1)
HBV (1)
HCV Protease (1)
Glutaminase kidney isoform, mitochondrial (1)
Glycoprotein hormones alpha chain (1)
TGF-beta receptor type II (1)
Thrombin (1)