Background: Intestinal expression of Abcg2/breast cancer resistance protein (BCRP) exhibits circadian oscillation, but the mechanism is unknown. Results: ATF4, a molecular component of the circadian clock, induced circadian expression of Abcg2 in mouse small intestine.
Conclusion:The circadian clock-ATF4 pathway causes the oscillation of BCRP function and induces the circadian change in intestinal drug absorption. Significance: ATF4 constitutes a novel molecular link connecting the circadian clock to xenobiotic detoxification.
Background/Purpose
Blonanserin is an atypical antipsychotic, a potent selective antagonist of dopamine D
2
receptor (D
2
), prescribed as oral formulations in patients with schizophrenia. Blonanserin transdermal patch was developed to provide a new treatment option, but the corresponding dose to oral blonanserin was not clear. The aims of this study were to clarify the pharmacokinetic (PK)-pharmacodynamic characteristics of blonanserin after transdermal patch application and to evaluate the corresponding dose to oral formulation based on striatal D
2
occupancy.
Methods
The relationship between D
2
occupancy and plasma blonanserin concentration was analyzed using an
E
max
model based on data from positron emission tomography study with oral and transdermal blonanserin. D
2
occupancy was simulated using
E
max
models based on the observed plasma concentrations and the simulated plasma concentrations obtained from population PK model.
Results
Plasma blonanserin concentration levels after repeated patch applications were nearly stable throughout the day and no effect of sex, advanced age, or application site was detected. The concentration at half maximal D
2
occupancy during transdermal patch applications, 0.857 ng/mL, was higher than that after oral doses, 0.112 ng/mL, suggesting metabolite contribution after oral doses. The median predicted D
2
occupancy during blonanserin patch applications at doses of 40 and 80 mg/d was 48.7% and 62.5%, respectively, and the distribution of D
2
occupancy at these doses could cover most of that at oral doses of 8 to 24 mg/d.
Conclusions
Predicted D
2
occupancy suggested that a 40- to 80-mg/d blonanserin transdermal patch dose corresponds to an 8- to 24-mg/d oral dose for the treatment of schizophrenia.
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