Table 2.
In-silico ADMET screening of the selected compounds.
| Compounds | aCNS | bQPlogKhsa | cSASA | dQPlogPo/w | eQPlogS | fQPlogBB | g%Human oral absorption | hRule of five |
|---|---|---|---|---|---|---|---|---|
| Daunorubicin | − 2 | − 0.32 | 716.74 | 0.49 | − 2.30 | − 1.88 | 9.34 | 3 |
| Onalespib | 1 | 0.58 | 763.23 | 3.03 | − 3.92 | − 0.3 | 74.42 | 0 |
| ABBV-744 | − 2 | 0.95 | 798.91 | 4.83 | − 7.15 | − 1.42 | 100.0 | 0 |
| αk-13b inhibitor | − 2 | − 0.07 | 960.42 | 3.11 | − 5.15 | − 2.91 | 33.40 | 3 |
aPredicted central nervous system activity from − 2 (inactive) to + 2 (active). bPrediction of binding to human serum albumin (acceptable range: − 1.5–1.5). cTotal Solvent Accessible Surface Area: SASA (acceptable range: 300–1000). dPredicted octanol/water partition coefficient (acceptable range: − 2–6.5). ePredicted aqueous solubility, S in mol/dm−3 (acceptable range: − 6.5–0.5). fPredicted brain/blood partition coefficient (acceptable range: − 3.0–1.2). gPredicted percentage human oral absorption (< 25% is poor and > 80% is high). hNumber of violations of Lipinski’s rule of five, Compounds that satisfy these rules are considered druglike (maximum 4).