Electrospinning polymersomes into bead-on-string polyethylene oxide fibres for the delivery of biopharmaceuticals to mucosal epithelia

Jake G Edmans; Samuel Harrison; Paul V Hatton; Craig Murdoch; Sebastian G Spain; Helen E Colley

doi:10.1016/j.bioadv.2023.213734

Electrospinning polymersomes into bead-on-string polyethylene oxide fibres for the delivery of biopharmaceuticals to mucosal epithelia

Biomater Adv. 2024 Feb:157:213734. doi: 10.1016/j.bioadv.2023.213734. Epub 2023 Dec 12.

Authors

Jake G Edmans¹, Samuel Harrison², Paul V Hatton³, Craig Murdoch⁴, Sebastian G Spain², Helen E Colley³

Affiliations

¹ School of Clinical Dentistry, University of Sheffield, 19 Claremont Crescent, Sheffield S10 2TA, United Kingdom; Department of Chemistry, University of Sheffield, Brook Hill, Sheffield S3 7HF, United Kingdom.
² Department of Chemistry, University of Sheffield, Brook Hill, Sheffield S3 7HF, United Kingdom.
³ School of Clinical Dentistry, University of Sheffield, 19 Claremont Crescent, Sheffield S10 2TA, United Kingdom.
⁴ School of Clinical Dentistry, University of Sheffield, 19 Claremont Crescent, Sheffield S10 2TA, United Kingdom. Electronic address: c.murdoch@sheffield.ac.uk.

PMID: 38109830
DOI: 10.1016/j.bioadv.2023.213734

Abstract

Fibrous mucoadhesive polymer membranes prepared using electrospinning demonstrate many advantages for mucosal drug delivery compared to other formulations. Previous electrospun membrane formulations have been developed mainly for the delivery of small molecule drugs. There remains great potential to further develop the technology for the delivery of vesicular vectors that allow administration of advanced therapeutic agents. However, there are no previous reports demonstrating the release of intact drug delivery vesicles from electrospun materials. Here, we describe incorporation and release of protein-loaded polymersomes from polyethylene oxide (PEO)-based electrospun membranes. Polymersomes comprising a copolymer of glycerol monomethacrylate (GMA) and hydroxypropyl methacrylate (HPMA) were prepared using polymerization-induced self-assembly and incorporated within PEO membranes using bead-on-string electrospinning at approximately 40 % w/w by polymer mass. Super-resolution fluorescence imaging showed that the vesicles remained intact and retained their encapsulated protein load within the fibre beads. Transmission electron microscopy and dynamic light scattering demonstrated that polymersomes retained their morphology following release from the polymer fibres. F(ab) antibody fragments were encapsulated within polymersomes and then electrospun into membranes. 78 ± 13 % of the F(ab) remained encapsulated within polymersomes during electrospinning and retained functionality when released from electrospun membranes, demonstrating that the formulation is suitable for the delivery of biologics. Membranes were non-irritant to the oral epithelium and fluorescence microscopy detected accumulation of polymersomes within the epithelia following application. This innovative drug delivery approach represents a novel and potentially highly useful method for the administration of large molecular mass therapeutic molecules to diseased mucosal sites.

Keywords: Antibody; Drug delivery; Electrospinning; Mucosa; Polymersome.

MeSH terms

Biological Products*
Drug Delivery Systems
Epithelium
Polyethylene Glycols*
Polymers

Substances

Polyethylene Glycols
Biological Products
Polymers