Modelling protein therapeutic co-formulation and co-delivery with PLGA nanoparticles continuously manufactured by microfluidics

Literature Information

Publication Date 2019-11-28
DOI 10.1039/C9RE00395A
Impact Factor 4.239
Authors

Veeren M. Chauhan, Amjad A. Selo, Mohammad Al-Natour, Jonathan W. Aylott


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Abstract

Formulating protein therapeutics into nanoparticles (NPs) of poly(lactic-co-glycolic acid) (PLGA) provides key features such as protection against clearance, sustained release and less side effects by possible attachment of targeting ligands. These NPs also offer the potential for protein combination therapy, which is expected to exploit synergetic bioresponses, avoid multiple dosage regimens and consequent mis-dosing. Since the conventional manufacture of protein-loaded PLGA NPs is still associated with low-throughput, new continuous manufacturing methods such as microfluidics have been established. Herein, PLGA NPs continuously manufactured through microfluidics are proposed for co-formulation and -delivery of two model proteins consisting of bovine serum albumin (BSA) conjugated to either fluorescein (FITC) or tetramethylrhodamine (TRITC) isothiocyanates. Protein co-formulated NPs of 100 nm, monodispersed and with 70% of association efficiency were obtained. The microfluidic setup allowed a production rate of around 7 g of particles per day and demonstrated scale-up capacity. Model proteins were released in a controlled manner and without significant changes in their secondary structure. Studies in macrophage-like cells proved that protein co-formulated PLGA NPs did not impair metabolic activity (>70%). The cellular association of the proteins was around 2-times higher when co-formulated into PLGA NPs, compared to the free protein controls. Moreover, the cellular association of the co-formulated proteins was 4-times higher than the physical mixture of NPs individually loaded with each protein type. This work has demonstrated the effectiveness of continuously manufactured PLGA NPs for co-formulating and enhancing the cellular association of co-delivered model proteins, providing a proof-of-concept foundation for future protein combination nanotherapies.

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Source Journal

Reaction Chemistry & Engineering

Reaction Chemistry & Engineering
CiteScore: 0
Self-citation Rate: 8.8%
Articles per Year: 284

Reaction Chemistry & Engineering is an interdisciplinary journal reporting cutting-edge research focused on enhancing the understanding and efficiency of reactions. Reaction engineering leverages the interface where fundamental molecular chemistry meets chemical engineering and technology. Challenges in chemistry can be overcome by the application of new technologies, while engineers may find improved solutions for process development from the latest developments in reaction chemistry. Reaction Chemistry & Engineering is a unique forum for researchers whose interests span the broad areas of chemical engineering and chemical sciences to come together in solving problems of importance to wider society. All papers should be written to be approachable by readers across the engineering and chemical sciences. Papers that consider multiple scales, from the laboratory up to and including plant scale, are particularly encouraged.

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