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Liposome-based mucus-penetrating particles (MPP) for mucosal theranostics: demonstration of diamagnetic chemical exchange saturation transfer (diaCEST) magnetic resonance imaging (MRI)

Authors :
Michael T. McMahon
Benjamin S. Schuster
Himatkumar V. Patel
Qingguo Xu
Peter C.M. van Zjil
Tao Yu
Kannie W. Y. Chan
Abraham Anonuevo
Laura M. Ensign
Nikita Oskolkov
Sumon Chattopadhyay
Xiaolei Song
Justin Hanes
Source :
Nanomedicine : nanotechnology, biology, and medicine. 11(2)
Publication Year :
2014

Abstract

Mucus barriers lining mucosal epithelia reduce the effectiveness of nanocarrier-based mucosal drug delivery and imaging (“theranostics”). Here, we describe liposome-based mucus-penetrating particles (MPP) capable of loading hydrophilic agents, e.g., the diaCEST MRI contrast agent barbituric acid (BA). We observed that polyethylene glycol (PEG)-coated liposomes containing ≥ 7 mol% PEG diffused only ~ 10-fold slower in human cervicovaginal mucus (CVM) compared to their theoretical speeds in water. 7 mol%-PEG liposomes contained sufficient BA loading for diaCEST contrast, and provided improved vaginal distribution compared to 0 and 3 mol%-PEG liposomes. However, increasing PEG content to ~ 12 mol% compromised BA loading and vaginal distribution, suggesting that PEG content must be optimized to maintain drug loading and stability. Non-invasive diaCEST MRI illustrated uniform vaginal coverage and longer retention of BA-loaded 7 mol%-PEG liposomes compared to unencapsulated BA. Liposomal MPP with optimized PEG content hold promise for drug delivery and imaging at mucosal surfaces. From the Clinical Editor This team of authors characterized liposome-based mucus-penetrating particles (MPP) capable of loading hydrophilic agents, such as barbituric acid (a diaCEST MRI contrast agent) and concluded that liposomal MPP with optimized PEG coating enables drug delivery and imaging at mucosal surfaces.

Details

ISSN :
15499642
Volume :
11
Issue :
2
Database :
OpenAIRE
Journal :
Nanomedicine : nanotechnology, biology, and medicine
Accession number :
edsair.doi.dedup.....a7641b35d3aacd2ae54ed7f9a0783d40