Species | Potential target | Raw | Global | Species |
---|---|---|---|---|
Loa Loa (eye worm) | DOMON domain-containing protein | 0.1386 | 0.4902 | 0.4129 |
Loa Loa (eye worm) | hypothetical protein | 0.2067 | 1 | 1 |
Loa Loa (eye worm) | TK/ROR protein kinase | 0.2067 | 1 | 1 |
Brugia malayi | Muscle positioning protein 4 | 0.1561 | 0.6213 | 0.2571 |
Plasmodium falciparum | cysteine repeat modular protein 1 | 0.2067 | 1 | 0.5 |
Onchocerca volvulus | 0.2067 | 1 | 1 | |
Toxoplasma gondii | kringle domain-containing protein | 0.2067 | 1 | 0.5 |
Schistosoma mansoni | hypothetical protein | 0.1386 | 0.4902 | 0.4902 |
Plasmodium vivax | cysteine repeat modular protein 1, putative | 0.2067 | 1 | 0.5 |
Brugia malayi | Kringle domain containing protein | 0.2067 | 1 | 1 |
Trypanosoma cruzi | hypothetical protein, conserved | 0.2067 | 1 | 0.5 |
Loa Loa (eye worm) | hypothetical protein | 0.1386 | 0.4902 | 0.4129 |
Schistosoma mansoni | subfamily S1A unassigned peptidase (S01 family) | 0.0984 | 0.189 | 0.189 |
Leishmania major | hypothetical protein, conserved | 0.2067 | 1 | 0.5 |
Echinococcus multilocularis | tissue type plasminogen activator | 0.2067 | 1 | 0.5 |
Onchocerca volvulus | 0.1561 | 0.6213 | 0.2571 | |
Loa Loa (eye worm) | hypothetical protein | 0.1561 | 0.6213 | 0.5638 |
Echinococcus granulosus | tissue type plasminogen activator | 0.2067 | 1 | 0.5 |
Schistosoma mansoni | hypothetical protein | 0.2067 | 1 | 1 |
Activity type | Activity value | Assay description | Source | Reference |
---|---|---|---|---|
Potency (functional) | 23.0999 uM | PUBCHEM_BIOASSAY: qHTS screen for small molecules that inhibit ELG1-dependent DNA repair in human embryonic kidney (HEK293T) cells expressing luciferase-tagged ELG1. (Class of assay: confirmatory) [Related pubchem assays (depositor defined):AID493107, AID493125] | ChEMBL. | No reference |
Potency (functional) | 89.1251 uM | PUBCHEM_BIOASSAY: qHTS for Inhibitors of Polymerase Iota. (Class of assay: confirmatory) [Related pubchem assays (depositor defined):AID588623] | ChEMBL. | No reference |
Many chemical entities in TDR Targets come from high-throughput screenings with whole cells or tissue samples, and not all assayed compounds have been tested against a single a single target protein, probably because they get ruled out during screening process. Even if these compounds may have not been of interest in the original screening, they may come as interesting leads for other screening assays. Furthermore, we may be able to propose drug-target associations using chemical similarities and network patterns.