Longitudinal investigation of permeability and distribution of macromolecules in mouse malignant transformation using PET. Academic Article

abstract

• PURPOSE: We apply positron emission tomography (PET) to elucidate changes in nanocarrier extravasation during the transition from premalignant to malignant cancer, providing insight into the use of imaging to characterize early cancerous lesions and the utility of nanoparticles in early disease. EXPERIMENTAL DESIGN: Albumin and liposomes were labeled with (64)Cu (half-life 12.7 hours), and longitudinal PET and CT imaging studies were conducted in a mouse model of ductal carcinoma in situ. A pharmacokinetic model was applied to estimate the tumor vascular volume and permeability. RESULTS: From early time points characterized by disseminated hyperproliferation, the enhanced vascular permeability facilitated lesion detection. During disease progression, the vascular volume fraction increased 1.6-fold and the apparent vascular permeability to albumin and liposomes increased 2.5-fold to 6.6 10(-8) and 1.3 10(-8) cm/s, respectively, with the accumulation of albumin increasing earlier in the disease process. In the malignant tumor, both tracers reached similar mean intratumoral concentrations of 6% ID/cc but the distribution of liposomes was more heterogeneous, ranging from 1% to 18% ID/cc compared with 1% to 9% ID/cc for albumin. The tumor-to-muscle ratio was 17.9 8.1 and 7.1 0.5 for liposomes and albumin, respectively, indicating a more specific delivery of liposomes than with albumin. CONCLUSIONS: PET imaging of radiolabeled particles, validated by confocal imaging and histology, detected the transition from premalignant to malignant lesions and effectively quantified the associated changes in vascular permeability.

authors

• Even, Lisa

published proceedings

• Clin Cancer Res

author list (cited authors)

• Rygh, C. B., Qin, S., Seo, J. W., Mahakian, L. M., Zhang, H., Adamson, R., ... Ferrara, K. W.

citation count

• 32

complete list of authors

• Rygh, Cecilie B||Qin, Shengping||Seo, Jai W||Mahakian, Lisa M||Zhang, Hua||Adamson, Roger||Chen, Jane Q||Borowsky, Alexander D||Cardiff, Robert D||Reed, Rolf K||Curry, Fitz-Roy E||Ferrara, Katherine W

publication date

• February 2011

publisher

• American Association for Cancer Research (AACR)  Publisher

published in

• CLINICAL CANCER RESEARCH  Journal

keywords

• Animals
• Capillary Permeability
• Carcinoma In Situ
• Cell Transformation, Neoplastic
• Copper Radioisotopes
• Disease Progression
• Liposomes
• Mammary Neoplasms, Experimental
• Mice
• Nanoparticles
• Positron-Emission Tomography
• Serum Albumin

Digital Object Identifier (DOI)

• 10.1158/1078-0432.CCR-10-2049

start page

• 550

end page

• 559

volume

• 17

issue

• 3

URL

• http://dx.doi.org/10.1158/1078-0432.ccr-10-2049