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PET Imaging of Tumor Uptake of a Biocompatible C60 Fullerene Drug Delivery Vector

Tuesday, 15 May 2018: 08:40
Room 203 (Washington State Convention Center)
N. G. Zaibaq, M. J. Collins (Rice University), M. D. Pagel (University of Texas MD Anderson Cancer Center), and L. J. Wilson (Rice University Department of Chemistry)
Traditional chemotherapy is one of the standards in cancer treatment, but the delivery of drugs and biologics is hindered by various barriers throughout the cancer microenvironment. Recently, nanoparticles have been of great interest as drug vectors because they can be tailored for specific functions to increase the amount of administered drug in the tumor microenvironment. In particular, biocompatible C60 fullerene has potential as a drug delivery scaffold since it has been shown to penetrate very restrictive physiological membranes (e.g. blood-brain-barrier and nuclear membrane)1. Our long-term goal is to determine the biodistribution of a biocompatible C60 material, as well as other pharmacokinetic data in both small and large animal models in order to evaluate its potential as a clinical drug vector for anti-cancer drugs. In this work, we have synthesized a C60 derivative with a metal chelating agent covalently bound to the C60 cage. The chelating agent of this material can be easily radiolabeled with 64Cu2++ emitter; t1/2 = 12 h) and tracked in vivo using positron emission tomography (PET) imaging. Because of its extreme sensitivity and routine clinical use, PET is an ideal imaging technique for studying pharmacokinetic properties and tumor accumulation of a C60 fullerene delivery vector, for both preclinical and possible future clinical studies. The material has been synthesized following an optimized six-step synthesis and the stability of the 64Cu2+ ion in the chelate has been evaluated by challenge with biological media. Animal biodistribution data will be determined using PET imaging in tumor- and non-tumor-bearing murine models.

Acknowledgements:

We gratefully acknowledge The Welch Foundation (C-0627) for support of this work, as well as the Department of Chemistry and the Smalley-Curl Institute at Rice University and the Department of Cancer Systems Imaging at UT MD Anderson Cancer Center. Additionally, the work is supported by the National Science Foundation Graduate Research Fellowship Program under Grant No. 1450681 (N.G.Z.).

References:

(1) Raoof, M.; Mackeyev, Y.; Cheney, M. A.; Wilson, L. J.; Curley, S. A. Biomaterials 2012, 33 (10), 2952–2960.