Effect of Cyclodextrin Complexation on the Aqueous Solubility and Solubility/Dose Ratio of Praziquantel

Maragos, Stratos; Archontaki, Helen; Macheras, Panos; Valsami, Georgia

doi:10.1208/s12249-009-9346-7

Cited by 26 publications

(21 citation statements)

References 23 publications

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“…1). These findings confirmed previous results of Arrua et al (Arrua et al, 2015) and Maragos et al (Maragos et al, 2009).…”

Section: Comparative Phase Solubility Study With Maltodextrin and Cycsupporting

confidence: 93%

“…A linear profile of the solubility increase of CDs indicated a stoichiometry of 1:1, a positive or negative deviation from linearity would be associated with a higher order interaction or a self-association of CDs (Loftsson et al, 2005). Whereas this conclusion is in line with Maragos et al (Maragos et al, 2009), de Jesus et al (de Jesus et al, 2006) and El-Arini et al (El-Arini and Leuenberger, 1996), other studies reported a stoichiometry of 1:2 (Arrua et al, 2015).…”

Section: Comparative Phase Solubility Study With Maltodextrin and Cycsupporting

confidence: 52%

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Comparative in vitro and in vivo taste assessment of liquid praziquantel formulations

Münster

Mohamed-Ahmed

Immohr

et al. 2017

International Journal of Pharmaceutics

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The taste of pharmaceuticals strongly affects the compliance of patients. This study investigated the applicability of the electronic tongue and rodent brief-access taste aversion (BATA) model for the bitter compound praziquantel (PZQ) and taste masked liquid formulations for PZQ. In a comparative study maltodextrin (MD) Kleptose linecaps 17 was selected as an alternative taste masking agent to two cyclodextrins; hydroxypropyl-beta-cyclodextrin (HP-β-CD) and sulfobutyl ether-beta-cyclodextrin (SBE-β-CD). A phase solubility study showed the highest affinity and solubilization capabilities for SBE-β-CD over HP-β-CD and MD, suggesting the highest taste masking ability for SBE-β-CD. No reliable results were achieved for PZQ with the Insent electronic tongue. Thus this system was not used for further evaluation of solutions with MD and CDs to confirm the results of the solubility study. In contrast the BATA model demonstrated conclusive responses for the aversiveness of PZQ. The concentration of PZQ inhibiting 50% of water lick numbers (called IC value) was 0.06mg/ml. In contrast to the phase solubility study, the MD enabled an equal taste masking effect in vivo in comparison to both CDs. Moreover HP-β-CD showed superior taste masking capabilities for PZQ compared to SBE-β-CD as the SBE-β-CD itself was less acceptable for the rodents than HP-β-CD. In conclusion, the BATA model was identified as a more efficient taste assessment tool for the pure PZQ and liquid formulations in contrast to the electronic tongue and the phase solubility study.

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“…1). These findings confirmed previous results of Arrua et al (Arrua et al, 2015) and Maragos et al (Maragos et al, 2009).…”

Section: Comparative Phase Solubility Study With Maltodextrin and Cycsupporting

confidence: 93%

Section: Comparative Phase Solubility Study With Maltodextrin and Cycsupporting

confidence: 52%

Comparative in vitro and in vivo taste assessment of liquid praziquantel formulations

Münster

Mohamed-Ahmed

Immohr

et al. 2017

International Journal of Pharmaceutics

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“…The interaction between PZQ and other excipients was also studied in order to improve the low solubility of the drug, for example, with calcium carbonate [ 18 , 19 , 20 ], β-cyclodextrins [ 21 , 22 , 23 ], polyvinyl-pyrrolidone [ 24 , 25 ], polyethylene glycols [ 26 , 27 , 28 ], sodium starch glycolate [ 29 ], phosphatidylcholine–containing liposomes [ 30 ], layered double hydroxides [ 31 ], among others. Specifically, the interaction between PZQ and montmorillonite in aqueous medium was previously studied, although no improvements of in vitro dissolution and absorption rates were observed [ 32 ].…”

Section: Introductionmentioning

confidence: 99%

Praziquantel–Clays as Accelerated Release Systems to Enhance the Low Solubility of the Drug

et al. 2020

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Praziquantel is an antiparasitic drug indicated for the treatment of the schistosomiasis disease. This drug has very low aqueous solubility, requiring high oral doses for its administration which gives rise to side effects, therapeutic noncompliance and the appearance of resistant forms of the parasite. Clay minerals, like sepiolite and montmorillonite, are innocuous, non-toxic, biocompatible and low-cost excipients. Additionally, clays have high adsorbent properties that allow them to encapsulate drugs in nanometric spaces present in the channels in the case of the sepiolite or between the layers in the case of the montmorillonite. The interactions between the drug and clay minerals are studied experimentally with the strategy for preparing interactions products in organic solvents (ethanol, acetonitrile and dichloromethane) so that the interaction will be more effective and will be enhanced the aqueous solubility of praziquantel. The results showed that in the interaction products, the drug interacted with both clay minerals, which produced the loss of the crystallinity of the drug demonstrated by different techniques. This led to a significant increase in the dissolution rate of the praziquantel in all the interaction products in the simulated gastrointestinal tract media, except for the praziquantel–montmorillonite product prepared in dichloromethane that presented a controlled release in acid medium. Moreover, in vitro cytotoxicity and cell cycle studies were performed in the interaction products prepared with ethanol. The interaction product with sepiolite was biocompatible with the HTC116 line cells, and it did not produce alterations in the cell cycle. However, interaction products with montmorillonite did not produce cell death, but they showed affectation and damage of cells in the cell cycle study at the highest concentration tested (20–100 µM). Therefore, the different organic solvents used are adequate for the improvement of the biopharmaceutical profile of praziquantel. Drug–clay interaction products, specifically with sepiolite, showed very promising results in which new accelerated oral release systems of the praziquantel were obtained.

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“…Thus, it suggested that the effect of non-inclusion complexation in the solubilization ability of HP-␤-CD was more evident than that of ␤-CD, resulting in the better solubilization ability of the former. It should be also taken into account that the low solubility of ␤-CD was attributed to the strong inter-and intra-molecular hydrogen bond formation between the secondary hydroxyl groups of CD molecules, while no such bonding was observed in the case of HP-␤-CD due to partial substitution of the secondary hydroxyl groups of the CD molecule with hydroxypropyl groups (Maragos et al, 2009). Similar to HP-␤-CD, the methyl groups of Me-␤-CD disrupted intra-molecular hydrogen bonding, but also enlarged the whole cavity of the molecule by extending the secondary hydroxyl side and narrowing the primary hydroxyl side of the cone.…”

Section: Comparison Of Various Cdsmentioning

confidence: 99%

Complex of 9-nitro-camptothecin in hydroxypropyl-β-cyclodextrin: In vitro and in vivo evaluation

Jiang¹,

Sha²,

Zhang³

et al. 2010

International Journal of Pharmaceutics

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Effect of Cyclodextrin Complexation on the Aqueous Solubility and Solubility/Dose Ratio of Praziquantel

Cited by 26 publications

References 23 publications

Comparative in vitro and in vivo taste assessment of liquid praziquantel formulations

Comparative in vitro and in vivo taste assessment of liquid praziquantel formulations

Praziquantel–Clays as Accelerated Release Systems to Enhance the Low Solubility of the Drug

Complex of 9-nitro-camptothecin in hydroxypropyl-β-cyclodextrin: In vitro and in vivo evaluation

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