We found a match
Your institution may have access to this item. Find your institution then sign in to continue.
- Title
Systemic and brain bioavailabilities of D-Phenylglycine-L-Dopa, a sustained dopamine-releasing prodrug.
- Authors
Chun-Li Wang; Yang-Bin Fan; Shi-En Lee; Jang-Feng Lian; Jing-Ping Liou; Hui-Po Wang
- Abstract
D-Phenylglycine-L-Dopa (D-PhG-L-Dopa), designed as a dipeptide mimetic prodrug of dopamine, has been proven to have 31-fold higher oral bioavailability than L-Dopa in rats. To further investigate if this dipeptide enters the brain, a single-dose pharmacokinetic study by i.v. administration, in comparison with L-Dopa, was conducted to monitor brain availability. The dopamine level in the brain was also determined. The results indicated that both D-PhG-L-Dopa and L-Dopa entered the brain rapidly (Tmax 1 minute) with similar degrees of penetration (AUCbrain/AUCplasma 8.83% vs. 7.61%). As D-PhG-L-Dopa had higher systemic exposure than L-Dopa (AUCplasma 23.79 µmol*min/mL vs. 12.09 µmol*min/mL), it thus had higher brain availability (AUCbrain 2.0 µmol*min/mL vs. 0.92 µmol*min/mL). Although the AUCbrain dopamine after D-PhG-L-Dopa treatment was only 24% of that from L-Dopa treatment, it however exhibited higher anti-Parkinsonism activity than L-Dopa (reduction in rotation number 47.9 ± 5.5% vs. 27.3 ± 4.8%). Higher brain dopamine residual properties of D-PhG-L-Dopa treatment compared to L-Dopa treatment, namely 3.2 times longer MRTbrain dopamine (172.15 vs. 53.78 minutes), 10 times longer Tmax brain dopamine (30 vs. 3 minutes) and 8.36 times longer half-life (... (min) 112.51 vs. 13.46 minutes), may explain the result. Moreover, the long terminal half-life of brain dopamine upon D-PhG-L-Dopa treatment indicated its slow dopamine-releasing property compared with L-Dopa treatment (112.51 vs. 44.85 minutes). It is also important to note that brain dopamine level was better controlled in the D-PhG-L-Dopa group than in the L-Dopa group (Cmax/Cmin 1.62 vs. 9.85). In conclusion, this study demonstrated that D-PhG-L-Dopa is an intrinsic dopamine-sustained-releasing prodrug. The limited concentration fluctuation of released dopamine in the brain is beneficial for the clinical management of Parkinson's disease.
- Subjects
ANIMAL experimentation; ANTIPARKINSONIAN agents; BIOAVAILABILITY; BIOPHYSICS; DOPAMINE; HIGH performance liquid chromatography; RESEARCH methodology; PRODRUGS; RATS; RESEARCH funding; T-test (Statistics); RECEIVER operating characteristic curves; DATA analysis software; DESCRIPTIVE statistics; IN vitro studies
- Publication
Journal of Food & Drug Analysis, 2013, Vol 21, Issue 2, p136
- ISSN
1021-9498
- Publication type
Article
- DOI
10.1016/j.jfda.2013.05.001