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Comparison of Computed Tomography– and Optical Image–Based Assessment of Liposome Distribution
Author(s) -
Huang Huang,
Michael Dunne,
J.T. Lo,
David A. Jaffray,
Christine Allen
Publication year - 2013
Publication title -
molecular imaging
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.815
H-Index - 60
eISSN - 1536-0121
pISSN - 1535-3508
DOI - 10.2310/7290.2012.00028
Subject(s) - liposome , biodistribution , nanocarriers , optical coherence tomography , in vivo , iohexol , biomedical engineering , fluorescence lifetime imaging microscopy , molecular imaging , preclinical imaging , positron emission tomography , medicine , materials science , drug delivery , radiology , nanotechnology , fluorescence , optics , biology , physics , microbiology and biotechnology , renal function
The use of multimodal imaging as a tool to assess the in vivo pharmacokinetics and biodistribution of nanocarriers is important in understanding the nature of their in vivo transport. The current study reports the development of a nano-sized liposomal computed tomographic (CT)/optical imaging probe carrying iohexol and Cy5.5 and its use in micro-CT and optical imaging to quantitatively assess the whole-body (macroscopic), intratumoral, and microscopic distribution over a period of 8 days. These multimodal liposomes have a vascular half-life of 30.3 ± 8.9 hours in mice bearing subcutaneous H520 non-small cell lung cancer tumors, with the maximum liposome accumulation in tumor achieved 48 hours postinjection. The in vivo liposome distribution and stability were quantitatively assessed using both micro-CT and fluorescence molecular tomography. The combination of CT and optical imaging enables visualization of the liposomes at the whole-body, tumor, and cellular scales with high sensitivity. Such noninvasive tracking of therapeutic vehicles at the macro- and microscale is important for informed and rational development of novel nanocarrier systems

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