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Liposomes As Drug Delivery Vehicles for Boron Agents

Overview
Journal J Neurooncol
Publisher Springer
Date 1997 May 1
PMID 9151223
Citations 10
Authors
M F Hawthorne
K Shelly
Affiliations
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Abstract

The successful treatment of cancer by boron neutron capture therapy (BNCT) requires the selective concentration of boron-10 within malignant tumors. The potential of liposomes to deliver boron-rich compounds to tumors has been assessed by examination of the biodistribution of boron delivered by liposomes in tumor-bearing mice. Small unilamellar vesicles have been found to stably encapsulate high concentrations of water-soluble ionic boron compounds. Alternatively, lipophilic boron-containing species have been embedded within the phospholipid bilayer of liposomes, and both hydrophilic and lipophilic boron compounds have been incorporated within the same liposome formulation. The biodistribution of boron was determined at several time points over 48 hr after i.v. injection of liposomal suspensions in BALB/c mice bearing EMT6 tumors. The tumor-selective delivery of boron by the liposomes was demonstrated as tumor-boron concentrations increased for several hours post-injection. Even at the low injected doses employed (6-18 mg boron/kg body weight) therapeutic tumor boron concentrations were observed (> 30 micrograms boron/g tissue) and high tumor/blood ratios were achieved (> 5). The most favorable results were obtained with the polyhedral borane Na3[a2-B20H1-NH2CH2CH2NH2]. Liposomes encapsulating this species produced a tumor boron concentration of 45 micrograms/g tissue at 30 hr post-injection, at which time the tumor/blood boron ratio was 9.3.

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A Novel Boron Lipid to Modify Liposomal Surfaces for Boron Neutron Capture Therapy.

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BNCT induced immunomodulatory effects contribute to mammary tumor inhibition.

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Synthesis and Applications of Perfunctionalized Boron Clusters.

Axtell J, Saleh L, Qian E, Wixtrom A, Spokoyny A Inorg Chem. 2018; 57(5):2333-2350.

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Validation and Comparison of the Therapeutic Efficacy of Boron Neutron Capture Therapy Mediated By Boron-Rich Liposomes in Multiple Murine Tumor Models.

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