Application of phospholipid complex technique to improve the dissolution and pharmacokinetic of probucol by solvent-evaporation and co-grinding methods

Application of phospholipid complex technique to improve the dissolution and pharmacokinetic of probucol by solvent-evaporation and co-grinding methods

[Display omitted] To enhance the aqueous solubility and thus oral bioavailability of a poorly water-soluble drug, probucol (PB), probucol–phospholipid complex (PB–PC) was formulated by solvent-evaporation or co-grinding methods. The complexes were characterized by differential scanning calorimetry (...

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Veröffentlicht in:International journal of pharmaceutics 2014-10, Vol.474 (1-2), p.50-56
Hauptverfasser: Guo, Bei, Liu, Hongzhuo, Li, Yun, Zhao, Juanhang, Yang, Dan, Wang, Xianglin, Zhang, Tianhong
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Co-grinding method
Male
Molecular Structure
Oral bioavailability
Phospholipid complex
Phospholipids - blood
Phospholipids - chemistry
Phospholipids - pharmacokinetics
Probucol
Probucol - blood
Probucol - chemistry
Probucol - pharmacokinetics
Rats
Rats, Sprague-Dawley
Solubility
Solvent-evaporation method
Solvents - chemistry
Water - chemistry
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container_issue 1-2
container_start_page 50
container_title International journal of pharmaceutics
container_volume 474
creator Guo, Bei
Liu, Hongzhuo
Li, Yun
Zhao, Juanhang
Yang, Dan
Wang, Xianglin
Zhang, Tianhong
description [Display omitted] To enhance the aqueous solubility and thus oral bioavailability of a poorly water-soluble drug, probucol (PB), probucol–phospholipid complex (PB–PC) was formulated by solvent-evaporation or co-grinding methods. The complexes were characterized by differential scanning calorimetry (DSC), infrared spectroscopy (IR), powder X-ray diffraction (PXRD), solubility, oil–water partition coefficient and in vitro dissolution. The DSC, IR and PXRD data confirmed the formation of phospholipid complex. Furthermore, the results indicated hydrogen bond formation between PB and PC molecules play an important role in the formation of PB–PC without the formation of a new compound. The water solubility of PB in the complexes was improved from 0.005 to 17.76 or 1.65μg/mL (by solvent-evaporation or co-grinding methods respectively). As a result of it, the improved dissolution was shown in the prepared complexes. The PB–PC complexes by both solvent-evaporation and co-grinding methods exhibited higher peak plasma concentration (16,625.7 or 5343.3 vs. 2628.4ngmL−1), increased AUC0–48h (145,863.2 or 77,477.0 vs. 34,435.9ngmL−1h) when compared with the commercial product, suggesting improved bioavailability of the drug. The study therefore suggests that the phospholipid complexes have possibilities in enhancing the therapeutic efficacy of PB which may be due to its improved aqueous solubility, dissolution behavior and thus bioavailability.
doi_str_mv 10.1016/j.ijpharm.2014.08.006
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The PB–PC complexes by both solvent-evaporation and co-grinding methods exhibited higher peak plasma concentration (16,625.7 or 5343.3 vs. 2628.4ngmL−1), increased AUC0–48h (145,863.2 or 77,477.0 vs. 34,435.9ngmL−1h) when compared with the commercial product, suggesting improved bioavailability of the drug. 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The complexes were characterized by differential scanning calorimetry (DSC), infrared spectroscopy (IR), powder X-ray diffraction (PXRD), solubility, oil–water partition coefficient and in vitro dissolution. The DSC, IR and PXRD data confirmed the formation of phospholipid complex. Furthermore, the results indicated hydrogen bond formation between PB and PC molecules play an important role in the formation of PB–PC without the formation of a new compound. The water solubility of PB in the complexes was improved from 0.005 to 17.76 or 1.65μg/mL (by solvent-evaporation or co-grinding methods respectively). As a result of it, the improved dissolution was shown in the prepared complexes. The PB–PC complexes by both solvent-evaporation and co-grinding methods exhibited higher peak plasma concentration (16,625.7 or 5343.3 vs. 2628.4ngmL−1), increased AUC0–48h (145,863.2 or 77,477.0 vs. 34,435.9ngmL−1h) when compared with the commercial product, suggesting improved bioavailability of the drug. 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The complexes were characterized by differential scanning calorimetry (DSC), infrared spectroscopy (IR), powder X-ray diffraction (PXRD), solubility, oil–water partition coefficient and in vitro dissolution. The DSC, IR and PXRD data confirmed the formation of phospholipid complex. Furthermore, the results indicated hydrogen bond formation between PB and PC molecules play an important role in the formation of PB–PC without the formation of a new compound. The water solubility of PB in the complexes was improved from 0.005 to 17.76 or 1.65μg/mL (by solvent-evaporation or co-grinding methods respectively). As a result of it, the improved dissolution was shown in the prepared complexes. The PB–PC complexes by both solvent-evaporation and co-grinding methods exhibited higher peak plasma concentration (16,625.7 or 5343.3 vs. 2628.4ngmL−1), increased AUC0–48h (145,863.2 or 77,477.0 vs. 34,435.9ngmL−1h) when compared with the commercial product, suggesting improved bioavailability of the drug. The study therefore suggests that the phospholipid complexes have possibilities in enhancing the therapeutic efficacy of PB which may be due to its improved aqueous solubility, dissolution behavior and thus bioavailability.</abstract><cop>Netherlands</cop><pub>Elsevier B.V</pub><pmid>25108049</pmid><doi>10.1016/j.ijpharm.2014.08.006</doi><tpages>7</tpages></addata></record>
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subjects Animals
Co-grinding method
Male
Molecular Structure
Oral bioavailability
Phospholipid complex
Phospholipids - blood
Phospholipids - chemistry
Phospholipids - pharmacokinetics
Probucol
Probucol - blood
Probucol - chemistry
Probucol - pharmacokinetics
Rats
Rats, Sprague-Dawley
Solubility
Solvent-evaporation method
Solvents - chemistry
Water - chemistry
title Application of phospholipid complex technique to improve the dissolution and pharmacokinetic of probucol by solvent-evaporation and co-grinding methods
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