Increase in tumour permeability following TGF-Β type i receptor-inhibitor treatment observed by dynamic contrast-enhanced MRI

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Abstract

Background:To enhance the success rate of nanocarrier-mediated chemotherapy combined with an anti-angiogenic agent, it is crucial to identify parameters for tumour vasculature that can predict a response to the treatment of the anti-angiogenic agent.Methods:To apply transforming growth factor (TGF)-Β type I receptor (TΒR-I) inhibitor, A-83-01, to combined therapy, dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI) was carried out in mice bearing colon 26 cells using gadolinium (Gd)-DTPA and for its liposomal formulation to evaluate changes in tumour microvasculature following A-83-01. Tumour vascular parameters from DCE-MRI were compared with histological assessment and apparent diffusion coefficient of water in tumour generated by diffusion-weighted MRI.Results:Contrary to evaluations reported for anti-angiogenic agents, A-83-01 treatment increased the initial area under the Gd concentration-time curve (IAUGC 60), volume transfer constant (K trans) and fractional plasma volume (v p) significantly within 24 h, that was positively related to α-smooth muscle actin-positive pericyte coverage and tumour cell proliferation, and was correlated inversely with the apparent diffusion coefficient. The vascular function of the tumour improved by A-83-01 treatment was well assessed on post-liposomal Gd-DTPA-enhanced MR images, which predicted delivery of a liposomal drug to the tumour.Conclusion:These findings suggest that DCE-MRI and, in particular, K trans and v p quantitation, provide important additional information about tumour vasculature by A-83-01 treatment. © 2009 Cancer Research UK.

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Minowa, T., Kawano, K., Kuribayashi, H., Shiraishi, K., Sugino, T., Hattori, Y., … Maitani, Y. (2009). Increase in tumour permeability following TGF-Β type i receptor-inhibitor treatment observed by dynamic contrast-enhanced MRI. British Journal of Cancer, 101(11), 1884–1890. https://doi.org/10.1038/sj.bjc.6605367

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