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Literature DB >> 31170464

Formulation and manufacturing of lymphatic targeting liposomes using microfluidics.

Swapnil Khadke¹, Carla B Roces², Allan Cameron³, Andrew Devitt³, Yvonne Perrie⁴.

Abstract

The lymphatics are a target for a range of therapeutic purposes, including cancer therapy and vaccination, and both vesicle size and charge have been considered as factors controlling lymphatic targeting. Within this work, a range of liposomal formulations were investigated to develop a liposomal lymphatic targeting system. Initial screening of formulations considered the effect of charge, with neutral, cationic and anionic liposomes being investigated. Biodistribution studies demonstrated that after intramuscular injection, anionic liposomes offered the most rapid clearance to the draining lymphatics with cationic liposomes forming a depot at the injection site. Anionic liposomes containing phosphatidylserine showed higher clearance to the lymphatics and this may result form preferential uptake by macrophages. In terms of vesicle size, smaller unilamellar vesicles gave high lymphatic targeting and a 10-fold increase in concentration was achieved in dose escalation studies. Given that effective trafficking to the lymphatics was achieved, the next step was to enhance retention of the liposomes within the lymphatics, therefore the liposome formulation was combined with an avidin/biotin complex mechanism. The affinity of avidin for biotin allows biotinylated liposomes to complex in the presence of avidin. By pre-dosing with avidin, the biotin-avidin complex can be exploited to promote longer retention of the liposomes at the draining lymphatics. To load these small, biotinylated liposomes with protein, microfluidics manufacturing was used. Using microfluidics, protein could easily be incorporated in these small (~90nm) biotinylated liposomes. Both liposome and protein retention at the local draining lymph nodes was demonstrated with the liposome-biotin-avidin system. These results demonstrate that microfluidics can be used to prepare protein-loaded liposomes that offer enhanced lymphatic targeting and retention of both the liposomes and entrapped antigen.

Entities: Chemical

Keywords: Avidin; Biotin; Liposomes; Lymphatic targeting; Microfluidics; Protein delivery; Vaccines

Mesh：

Substances：

Year: 2019 PMID： 31170464 DOI： 10.1016/j.jconrel.2019.06.002

Source DB: PubMed Journal: J Control Release ISSN： 0168-3659 Impact factor: 9.776

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Cited

9 in total

1. The Impact of Solvent Selection: Strategies to Guide the Manufacturing of Liposomes Using Microfluidics.

Authors: Cameron Webb; Swapnil Khadke; Signe Tandrup Schmidt; Carla B Roces; Neil Forbes; Gillian Berrie; Yvonne Perrie
Journal: Pharmaceutics Date: 2019-12-04 Impact factor: 6.321

2. Optimization of Liposomes for Antigen Targeting to Splenic CD169⁺ Macrophages.

Authors: Maarten K Nijen Twilhaar; Lucas Czentner; Joanna Grabowska; Alsya J Affandi; Chun Yin Jerry Lau; Katarzyna Olesek; Hakan Kalay; Cornelus F van Nostrum; Yvette van Kooyk; Gert Storm; Joke M M den Haan
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4. Translating a Thin-Film Rehydration Method to Microfluidics for the Preparation of a SARS-CoV-2 DNA Vaccine: When Manufacturing Method Matters.

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Journal: Pharmaceutics Date: 2022-07-07 Impact factor: 6.525

5. Comparison of Physicochemical Properties of LipoParticles as mRNA Carrier Prepared by Automated Microfluidic System and Bulk Method.

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Review 6. Nanomaterial-Based Drug Delivery System Targeting Lymph Nodes.

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Review 7. Mimicking Pathogens to Augment the Potency of Liposomal Cancer Vaccines.

Authors: Maarten K Nijen Twilhaar; Lucas Czentner; Cornelus F van Nostrum; Gert Storm; Joke M M den Haan
Journal: Pharmaceutics Date: 2021-06-24 Impact factor: 6.321

Review 8. Evolution of drug delivery system from viewpoint of controlled intracellular trafficking and selective tissue targeting toward future nanomedicine.

Authors: Yuma Yamada; Yusuke Sato; Takashi Nakamura; Hideyoshi Harashima
Journal: J Control Release Date: 2020-09-08 Impact factor: 9.776

Review 9. Vaccine delivery systems toward lymph nodes.

Authors: Yingyue Ding; Zhaoting Li; Ana Jaklenec; Quanyin Hu
Journal: Adv Drug Deliv Rev Date: 2021-08-04 Impact factor: 17.873