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Dual-modality NIRF-MRI cubosomes and hexosomes: High throughput formulation and in vivo biodistribution

journal contribution
posted on 2024-11-02, 03:59 authored by Nhiem TranNhiem Tran, Nicole Bye, Bradford Moffat, David Wright, Andrew Cuddihy, Tracey Hinton, Adrian Hawley, Nicholas Reynolds, Lynne Waddington, Xavier MuletXavier Mulet, Ann Turnley, Cristina Morganti-Kossmann, Benjamin Muir
Engineered nanoparticles with multiple complementary imaging modalities are of great benefit to the rapid treatment and diagnosis of disease in various organs. Herein, we report the formulation of cubosomes and hexosomes that carry multiple amphiphilic imaging contrast agents in their self-assembled lipid bilayers. This is the first report of the use of both near infrared fluorescent (NIRF) imaging and gadolinium lipid based magnetic resonance (MR) imaging modalities in cubosomes and hexosomes. High-throughput screening was used to rapidly optimize formulations with desirable nano-architectures and low in vitro cytotoxicity. The dual-modal imaging nanoparticles in vivo biodistribution and organ specific contrast enhancement were then studied. The NIRF in vivo imaging results indicated accumulation of both cubosomes and hexosomes in the liver and spleen of mice up to 20 h post-injection. Remarkably, the biodistribution of the nanoparticle formulations was affected by the mesophase (i.e. cubic or hexagonal), a finding of significant importance for the future use of these compounds, with hexosomes showing higher accumulation in the spleen than the liver compared to cubosomes. Furthermore, in vivo MRI data of animals injected with either type of lyotropic liquid crystal nanoparticle displayed enhanced contrast in the liver and spleen.

History

Journal

Materials Science and Engineering C

Volume

71

Start page

584

End page

593

Total pages

10

Publisher

Elsevier

Place published

Netherlands

Language

English

Copyright

© 2016 Elsevier B.V.

Former Identifier

2006071139

Esploro creation date

2020-06-22

Fedora creation date

2017-03-07

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