Development of flexible and dispersible oral formulations containing praziquantel for potential schistosomiasis treatment of pre-school age children

Ramona Trastullo; Luisa Stella Dolci; Nadia Passerini; Beatrice Albertini

doi:10.1016/j.ijpharm.2015.09.019

Development of flexible and dispersible oral formulations containing praziquantel for potential schistosomiasis treatment of pre-school age children

Int J Pharm. 2015 Nov 10;495(1):536-550. doi: 10.1016/j.ijpharm.2015.09.019. Epub 2015 Sep 16.

Authors

Ramona Trastullo¹, Luisa Stella Dolci², Nadia Passerini¹, Beatrice Albertini³

Affiliations

¹ Department of Pharmacy and BioTechnology, University of Bologna, Via S. Donato 19/2, 40127 Bologna, Italy.
² Department of Chemistry "G. Ciamician", University of Bologna, Via Selmi 2, 40126 Bologna, Italy.
³ Department of Pharmacy and BioTechnology, University of Bologna, Via S. Donato 19/2, 40127 Bologna, Italy. Electronic address: beatrice.albertini@unibo.it.

PMID: 26386139
DOI: 10.1016/j.ijpharm.2015.09.019

Abstract

Praziquantel (PZQ), an anthelmintic drug used in developing countries for the treatment of schistosome infections, was processed using the fluid bed wet granulation technology to prepare fast dispersible granules, as an appropriate and flexible dosage form for pre-school-aged children. Granulation experiments were performed incorporating PZQ either in the powder mixture, according to the traditional way, or in the liquid phase containing wetting agents. In the powder mixture several excipients were tested: Flowlac 100 as filler, Galeniq 721 (isomalt) and Neosorb P 100 T (D-sorbitol) as sweeteners and PVP K30 as binder; while in the liquid phase Lutrol F68, Cremophor RH 40 or Tween 80 as surfactants were investigated. Different formulations loaded with 10% w/w (batches 1-8) and 20% w/w of PZQ (batches 9-13) were produced The majority of granules displayed good flow properties and uniform drug content. X-ray powder diffraction showed that PZQ remained in its original crystalline state, while differential scanning calorimetry and Fourier transform-infrared analysis evidenced the formation of chemical interactions among the ingredients. The solubilisation test performed in non-sink condition to reproduce the actual condition in which a child of 4 years takes the medicine revealed that granules quickly formed a very fine suspension in water (dV90=39.9 μm). Although after the granulation process the solubility of raw PZQ was not increased, adding the aqueous suspension to 500 ml of buffer solution of pH 1.5, simulating the fasted state of a child, 50% of the drug was dissolved after 30 min. After granule manipulation with milk and fruit juices, no PZQ degradation was observed during time. Finally, the selected granule formulation provided evidence to be stable even at hot and very humid climate (30°C/75% RH), at least for the examined time.

Keywords: Extemporaneous aqueous suspensions; Neglected tropical diseases; Paediatric dosage form; Praziquantel; Solid-state characterization; Stability; Wet granulation.

MeSH terms

Administration, Oral
Anthelmintics / administration & dosage*
Anthelmintics / therapeutic use
Calorimetry, Differential Scanning
Chemistry, Pharmaceutical / methods*
Child, Preschool
Dose-Response Relationship, Drug
Drug Stability
Excipients / chemistry
Humans
Models, Biological
Particle Size
Praziquantel / administration & dosage*
Praziquantel / therapeutic use
Schistosomiasis / drug therapy
Solubility
Spectroscopy, Fourier Transform Infrared
Sweetening Agents / chemistry
Technology, Pharmaceutical / methods*
X-Ray Diffraction

Substances

Anthelmintics
Excipients
Sweetening Agents
Praziquantel