A DiaCEST MRI Approach for Monitoring Liposomal Accumulation in Tumors

Overview

Journal J Control Release

Specialty Pharmacology

Date 2014 Feb 20

PMID 24548481

Citations 33

Authors

Kannie W Y Chan

Tao Yu

Yuan Qiao

Qiang Liu

Ming Yang

Himatkumar Patel

Guanshu Liu

Kenneth W Kinzler

Bert Vogelstein

Jeff W M Bulte

Peter C M van Zijl

Justin Hanes

Shibin Zhou

Michael T McMahon

Affiliations

Soon will be listed here.

Abstract

Nanocarrier-based chemotherapy allows preferential delivery of therapeutics to tumors and has been found to improve the efficacy of cancer treatment. However, difficulties in tracking nanocarriers and evaluating their pharmacological fates in patients have limited judicious selection of patients to those who might most benefit from nanotherapeutics. To enable the monitoring of nanocarriers in vivo, we developed MRI-traceable diamagnetic Chemical Exchange Saturation Transfer (diaCEST) liposomes. The diaCEST liposomes were based on the clinical formulation of liposomal doxorubicin (i.e. DOXIL®) and were loaded with barbituric acid (BA), a small, organic, biocompatible diaCEST contrast agent. The optimized diaCEST liposomal formulation with a BA-to-lipid ratio of 25% exhibited 30% contrast enhancement at B1=4.7μT in vitro. The contrast was stable, with ~80% of the initial CEST signal sustained over 8h in vitro. We used the diaCEST liposomes to monitor the response to tumor necrosis factor-alpha (TNF-α), an agent in clinical trials that increases vascular permeability and uptake of nanocarriers into tumors. After systemic administration of diaCEST liposomes to mice bearing CT26 tumors, we found an average diaCEST contrast at the BA frequency (5ppm) of 0.4% at B1=4.7μT while if TNF-α was co-administered the contrast increased to 1.5%. This novel approach provides a non-radioactive, non-metallic, biocompatible, semi-quantitative, and clinically translatable approach to evaluate the tumor targeting of stealth liposomes in vivo, which may enable personalized nanomedicine.

Citing Articles

Going Above and Beyond: Achieving High Contrast and Higher Offset through Carbon Dot-Based diaCEST MRI Contrast Agent.

Pandey S, Ghosh A Chem Biomed Imaging. 2025; 3(2):123-131.

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Design Chemical Exchange Saturation Transfer Contrast Agents and Nanocarriers for Imaging Proton Exchange .

Su H, Chan K ACS Nano. 2024; 18(50):33775-33791.

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Contrasting Properties of Polymeric Nanocarriers for MRI-Guided Drug Delivery.

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Monitor Tumor pHe and Response Longitudinally during Treatment Using CEST MRI-Detectable Alginate Microbeads.

Xiao P, Huang J, Han X, Cheu J, Liu Y, Law L ACS Appl Mater Interfaces. 2022; 14(49):54401-54410.

PMID: 36448714 PMC: 9756293. DOI: 10.1021/acsami.2c10493.

Preparation of Hydrothermal Carbon Quantum Dots as a Contrast Amplifying Technique for the diaCEST MRI Contrast Agents.

Pandey S, Ghosh R, Ghosh A ACS Omega. 2022; 7(38):33934-33941.

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