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Pharmaceutical Development and Technology Volume 24, 2019 - Issue 5
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Research Article

Effects of formulation development methods on the stability of model protein pharmaceuticals embedded in solid lipid matrices

Misbah TabbassumDepartment of Chemistry, Faculty of Science, University of Malaya (UM), Kuala Lumpur, Malaysia;
&
Farrukh ZeeshanSchool of Pharmacy, University of Otago, Dunedin, New Zealand; ;School of Pharmacy, International Medical University (IMU), Kuala Lumpur, MalaysiaCorrespondence[email protected]
Pages 649-662 | Received 26 Apr 2018, Accepted 19 Nov 2018, Published online: 27 Jan 2019
 
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Abstract

This study was conducted to investigate the influence of formulation development methods on the stability (secondary structure, aggregation, and biological activity) of protein drugs embedded in lipid matrices. Catalase, horseradish peroxidase, and α-chymotrypsin were employed as model proteins, while Precirol® AT05 (glyceryl palmitostearate) was used as lipid matrix. Protein-loaded lipid matrices were prepared using melting and mixing and wet granulation methods. Attenuated total reflectance Fourier transform infrared (ATR FT-IR) spectroscopy, size exclusion chromatography (SEC) and biological activity analyses were performed. ATR FT-IR analysis indicated significant interference of the lipid with the protein amide-I band, which was eliminated using spectral subtraction. Wet granulation method induced more changes in protein secondary structure compared to melting and mixing method. SEC analysis gave evidence of protein aggregation for catalase upon adopting the wet granulation method. The biological activity of catalase was found to reduce significantly than other two proteins upon using wet granulation method, which might be ascribed to both secondary structure alterations and the formation of aggregates. Horseradish peroxidase and α-chymotrypsin did not form any soluble aggregates. In conclusion, melting and mixing method emerged as a better incorporation method compared to wet granulation because of better stability shown by the formulated proteins.

Acknowledgement

The authors would like to thank University of Otago, Dunedin, New Zealand for providing the PhD funding and all other necessary facilities and University of Malaya, Kuala Lumpur, Malaysia for rendering analytical instruments that made this study possible.

Disclosure statement

No potential conflict of interest was reported by the authors.

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