Application of Quality by Design to the robust preparation of a liposomal GLA formulation by DELOS-susp method

Fabry disease is a lysosomal storage disease arising from a deficiency of the enzyme α-galactosidase A (GLA). The enzyme deficiency results in an accumulation of glycolipids, which over time, leads to cardiovascular, cerebrovascular, and renal disease, ultimately leading to death in the fourth or fi...

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Authors: Merlo-Mas, Josep, Tomsen Melero, Judit|||0000-0002-2837-8107, Corchero Nieto, José Luis|||0000-0002-6109-144X, González Mira, Elisabet, Font, Albert|||0000-0003-3908-1111, Pedersen, Jannik N., García Aranda, Natalia|||0000-0003-3230-9881, Cristóbal-Lecina, Edgar, Alcaina Hernando, Marta, Mendoza Moreno, Rosa|||0000-0002-0488-4814, Garcia-Fruitos, Elena|||0000-0001-7498-4864, Lizarraga, Teresa, Resch, Susanne, Schimpel, Christa, Falk, Andreas, Pulido, Daniel|||0000-0002-2841-194X, Royo, Miriam|||0000-0001-5292-0819, Schwartz, Simon|||0000-0001-8297-7971, Abasolo, Ibane|||0000-0001-5970-6276, Pedersen, Jan Skov|||0000-0002-7768-0206, Danino, Dganit, Soldevila, Andreu, Veciana i Miró, Jaume|||0000-0003-1023-9923, Sala, Santi, Ventosa, Nora|||0000-0002-8008-4974, Córdoba, Alba
Format: article
Publication Date:2021
Country:España
Institution:Universitat Autònoma de Barcelona
Repository:Dipòsit Digital de Documents de la UAB
Language:English
OAI Identifier:oai:ddd.uab.cat:247506
Online Access:https://ddd.uab.cat/record/247506
https://dx.doi.org/urn:doi:10.1016/j.supflu.2021.105204
Access Level:Open access
Keyword:Quality by Design
DELOS
Scale-up
Protein-loaded liposomes
Fabry disease
α-galactosidase
Description
Summary:Fabry disease is a lysosomal storage disease arising from a deficiency of the enzyme α-galactosidase A (GLA). The enzyme deficiency results in an accumulation of glycolipids, which over time, leads to cardiovascular, cerebrovascular, and renal disease, ultimately leading to death in the fourth or fifth decade of life. Currently, lysosomal storage disorders are treated by enzyme replacement therapy (ERT) through the direct administration of the missing enzyme to the patients. In view of their advantages as drug delivery systems, liposomes are increasingly being researched and utilized in the pharmaceutical, food and cosmetic industries, but one of the main barriers to market is their scalability. Depressurization of an Expanded Liquid Organic Solution into aqueous solution (DELOS-susp) is a compressed fluid-based method that allows the reproducible and scalable production of nanovesicular systems with remarkable physicochemical characteristics, in terms of homogeneity, morphology, and particle size. The objective of this work was to optimize and reach a suitable formulation for in vivo preclinical studies by implementing a Quality by Design (QbD) approach, a methodology recommended by the FDA and the EMA to develop robust drug manufacturing and control methods, to the preparation of α-galactosidase-loaded nanoliposomes (nanoGLA) for the treatment of Fabry disease. Through a risk analysis and a Design of Experiments (DoE), we obtained the Design Space in which GLA concentration and lipid concentration were found as critical parameters for achieving a stable nanoformulation. This Design Space allowed the optimization of the process to produce a nanoformulation suitable for in vivo preclinical testing.