ADV368

Bispecific Sigma-1 Agonist and Sigma-2 Antagonist

Candidate Profile:

  • ADV368 is an achiral compound ​
  • The compound shows a good profile regarding Lipinski’s rule compliance
  • logP 1.44; MW 478.6 g/mol
  • Max. kinetic solubility: 300 µM (pH 7.4) ​
  • Good stability in neutral and acidic conditions
  • Free base thermodynamic solubility of 5237 µM (pH 2) and 901 µM (pH 7.4) and a mp of 168 ºC
  • The free base has been selected for development
  • Synthesis has 4 steps with a 70% overall yield
  • The process is suitable for scale-up
  • Good affinity for σ1 receptor, Ki = 46 nM ​
  • Good affinity for σ2 receptor, Ki = 14 nM ​
  • S1R-BIP interaction is not modified and, therefore, behaves as an S1R agonist
  • Functional profile corresponding to σ1 agonist and σ2 antagonist based on the effect in capsaicin 1µg i.pl. in WT and KO mice
  • Selective vs 164 targets panel (inhib.<50% at 10 µM)
  • No alerts on genotoxicity in vitro: SOS/umu, Ames, and CHO micronucleus tests negative​
  • No alerts on mitochondrial toxicity
  • No alerts on in vitro cytotoxicity (up to 100 µM)
  • Cardiac hERG potassium channel: IC50 > 10 µM
  • No in vitro alert on electrophysiological assays of ion channels related to cardiovascular function up to 10 µM​
  • Irwin’s test: no relevant effects (60 mg/kg po, rat)
  • High metabolic stability expected in humans
  • Metabolic Stability in liver microsomes HRMDoMoMp=96/84/92/93/61/73% (1h)
  • Metabolic Stability in hepatocytes HRMDoMoMp=94/82/–/99/22/48% (1h)
  • Metabolic Stability in mouse t½=871 min​ at 1μM
  • CYPs IC50 µM (HLM) >250 (1A2,2D6,3A4)
  • Low potential for metabolism-based drug-drug interactions​
  • Moderate permeability (human Caco-2 cells): Papp 106nm/s. ER 3.3
  • Plasma protein binding in humans similar to rodents (37% vs 48-51%)
  • Good oral exposure in rodents (AUC > 2000 ng.h/mL)
  • Bioavailability in rats: F=117%
  • Brain distribution in rats after oral dosing: AUCbrain/AUCplasma = 0.5​
  • Urinary excretion in the rat is a minor route of elimination (12% of unchanged compound excreted)
  • Fast oral absorption in dogs
  • High exposure after oral administration in dogs, with no clinical signs observed
  • Moderate elimination rate with t1/2 of 3h after iv administration in dogs
  • Medium hepatic extraction ratio in dogs, suggesting that clearance could be limited by and dependent upon liver blood flow
  • Volume of distribution higher than the total body wate in dogs, indicating a good distribution of the compound
  • Good bioavailability in dogs (67%)
  • Max Non Lethal Dose in mouse:​ 2000 mg/kg M & F
  • Genotoxicity in vivo (micronuclei): Negative
  • No alert and well-tolerated in 7-day oral rat toxicity (RDT) at 10 (F) & 50 (M) mg/kg/d​

Current Indications: