BAY 73-6691 is an inhibitor of brain penetrant PDE9A.

BAY 73-6691 dose-dependently attenuates oxidative stress induced by Aβ25-35. The BAY 73-6691 dose-dependently alleviates cell viability loss due to Aβ25-35 treatment. The BAY 73-6691 attenuates Aβ25-35-induced increase of apoptosis cells[1]. It is found that when SH-SY5Y cells are cultured by Aβ25-35, a high degree of cell apoptosis is observed, while additional stimulation with BAY 73-6691 causes attenuation of cell apoptosis. BAY 73-6691 at 200 μg/mL almost neutralizes Aβ25-35-induced oxidative damage.

BAY 73-6691 dose-dependently improves the acquisition performance in the Aβ25-35-injected mice on days 7 to 10 (day 7, F(5,54)=65.153; day 8, F(5,54)=62.340; day 9, F(5,54)=37.529; day 10, F(5,54)=38.624; P<0.001) and it also dose-dependently elevates the Aβ25-35-induced decrease of the dwell time on the 10th day post Aβ25-35 injection (day 10, F(5,54)=27.360, P<0.001). BAY 73-6691 at 3 mg/kg can almost completely abolish the prolongation of escape-latency on days 9 to 10. Results reveal that the Aβ25-35 injection. BAY 73-6691 alleviates Aβ25-35-induced abnormalities of the above indices. BAY 73-6691 treatment cause no influence on the swimming speed. Treatment with BAY 73-6691 does not cause detectable alteration of spatial memory in sham mice. The BAY 73-6691 causes no influence on the four indices mentioned above in sham mice and it has no significant effect on the apoptosis of hippocampal neurons in sham mice[1].

794568-92-6

C15H12ClF3N4O

356.73

(R)-BAY 73-6691;BAY 73-6691

DMSO:160 mg/mL (448.52 mM),Need ultrasonic and warming
Powder: -20°C for 3 years
In solvent: -80°C for 2 years