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Evaluation of Nonradiative Clinical Imaging Techniques for the Longitudinal Assessment of Tumour Growth in Murine CT26 Colon Carcinoma
Author(s) -
Johanne Séguin,
BichThuy Doan,
Heldmuth Latorre Ossa,
Lauriane Jugé,
JeanLuc Gennisson,
Mickaël Tanter,
Daniel Scherman,
Guy G. Chabot,
Nathalie Mignet
Publication year - 2013
Publication title -
international journal of molecular imaging
Language(s) - English
Resource type - Journals
eISSN - 2090-1712
pISSN - 2090-1720
DOI - 10.1155/2013/983534
Subject(s) - medicine , colon carcinoma , carcinoma , colorectal cancer , pathology , cancer research , medical physics , oncology , cancer
Background and Objectives . To determine the most appropriate technique for tumour followup in experimental therapeutics, we compared ultrasound (US) and magnetic resonance imaging (MRI) to characterize ectopic and orthotopic colon carcinoma models. Methods . CT26 tumours were implanted subcutaneously (s.c.) in Balb/c mice for the ectopic model or into the caecum for the orthotopic model. Tumours were evaluated by histology, spectrofluorescence, MRI, and US. Results . Histology of CT26 tumour showed homogeneously dispersed cancer cells and blood vessels. The visualization of the vascular network using labelled albumin showed that CT26 tumours were highly vascularized and disorganized. MRI allowed high-resolution and accurate 3D tumour measurements and provided additional anatomical and functional information. Noninvasive US imaging allowed good delineation of tumours despite an hypoechogenic signal. Monitoring of tumour growth with US could be accomplished as early as 5 days after implantation with a shorter acquisition time (<5 min) compared to MRI. Conclusion . MRI and US afforded excellent noninvasive imaging techniques to accurately follow tumour growth of ectopic and orthotopic CT26 tumours. These two techniques can be appropriately used for tumour treatment followup, with a preference for US imaging, due to its short acquisition time and simplicity of use.

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