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Synthesis and evaluation of dapagliflozin ester prodrugs with improved hygroscopicity and thermal stability
  • Sung, Si Young ;
  • Chae, Yu Na ;
  • Lee, Dae Young ;
  • Kim, Kyeong Min ;
  • Kim, Eun Jung ;
  • Han, Ji Hye ;
  • Kim, Wook ;
  • Yoon, Sung Hwa
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Publication Year
2020-01-01
Publisher
Bentham Science Publishers
Citation
Letters in Drug Design and Discovery, Vol.17, pp.1409-1421
Keyword
DapagliflozinDiabetesFarxiga®ProdrugSGLT-2 inhibitorThermal stability
All Science Classification Codes (ASJC)
Molecular MedicinePharmaceutical ScienceDrug Discovery
Abstract
Background: Dapagliflozin, developed as an SGLT-2 inhibitor, has a low melting point and high hygroscopicity, which needs extreme care during pharmaceutical production to keep the active pharmacological property. Various attempts have been made to overcome these problematic properties. Objective: To develop dapagliflozin prodrugs that have similar pharmacological effects with improved hygroscopicity and thermal stability. Method: The novel dapagliflozin ester prodrugs containing pharmaceutically acceptable moieties were synthesized and their pharmacokinetics (PK) and physical properties were compared with dapagliflozin propanediol hydrate (DPD, Farxiga®). The PK in dog and rat, in vitro stability, hygroscopicity, and physical property studies in accelerated conditions (40°C, 75 % RH) were performed with prodrugs. Results and Discussions: Among the eight synthesized prodrugs, Cmax and AUC0-48h values of prodrug 8b (1.35 µg/ml and 14.78 µg·h/ml, respectively) were similar to those of DPD (1.67 µg/ml and 14.27 µg·h/ml, respectively). However, the rest of the prodrugs 8a, 8c, 8d, 8e, 8f, 8g and 8h showed significantly lower Cmax and AUC0-48h values than DPD. Prodrug 8b completely converted into parent drug in the body. Conclusion: The novel prodrug 8b exhibited comparative PK profile to that of DPD, but with low hygroscopic property and better thermal stability than DPD.
Language
eng
URI
https://dspace.ajou.ac.kr/dev/handle/2018.oak/31571
DOI
https://doi.org/10.2174/1570180817999200618162949
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Type
Article
Funding
This study was supported by Dong-A ST Research Institute of South Korea (Grant No. DA-2811).This study was supported by Dong-A ST Research Institute fooSuth oKrea G(rntaNo. DA-2811).
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College of Bio-convergence Engineering
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