In-vivo high-resolution X-ray microtomography for liver and spleen tumor assessment in mice

The present study sought to validate the use of glycery1‐2‐oley‐1,3‐bis‐[7‐(3‐amino‐2,4,6‐triiodophenyl)‐ heptanoate] (DHOG) contrast agent for mouse spleen tumor and liver metastasis imaging by high‐resolution X‐ray microtomography. Three groups of female nude mice were compared: controls (n = 5),...

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Veröffentlicht in:Contrast media and molecular imaging 2007-03, Vol.2 (2), p.88-93
Hauptverfasser: Almajdub, M., Nejjari, M., Poncet, G., Magnier, L., Chereul, E., Roche, C., Janier, M.
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container_issue 2
container_start_page 88
container_title Contrast media and molecular imaging
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creator Almajdub, M.
Nejjari, M.
Poncet, G.
Magnier, L.
Chereul, E.
Roche, C.
Janier, M.
description The present study sought to validate the use of glycery1‐2‐oley‐1,3‐bis‐[7‐(3‐amino‐2,4,6‐triiodophenyl)‐ heptanoate] (DHOG) contrast agent for mouse spleen tumor and liver metastasis imaging by high‐resolution X‐ray microtomography. Three groups of female nude mice were compared: controls (n = 5), and mice injected with 2.5 × 106 STC1 tumor cells in the spleen, imaged at 15 days (group G15, n = 5) and at 30 days (group G30, n = 5, of which one died before imaging). Micro‐CT scans (X‐ray voltage, 50 kVp; anode current, 200 µA; exposure time, 632 ms; 180 rotational steps resulting in 35 µm isotropic spatial resolution) were acquired at 0, 0.75, 2 and 4 h after i.v. injection of DHOG. CT number (Hounsfield units: HU) and contrast‐to‐noise ratios (CNR) were determined in three organs. Statistical analysis was performed by Mann–Whitney U‐test. Contrast enhancement in normal spleen and liver increased, respectively to 1020 ± 159 and 351 ± 27 HU over baseline at 4 h, and 482 ± 3 and 203 ± 14 HU on day 6 after a single contrast injection. Automated three‐dimensional reconstruction and modeling of the spleen provided accurate and quantifiable images. Spleen tumor and liver metastases did not take up DHOG, making them detectable in contrast to the increased signal in normal tissue. The smallest liver metastasis detected measured 0.3 mm in diameter. High‐resolution X‐ray micro‐CT in living mice using DHOG contrast agent allowed visualization and volume quantification of normal spleen and of spleen tumor and its liver metastases. Copyright © 2007 John Wiley & Sons, Ltd. The present study sought to validate the use of a specific contrast agent (DHOG) with high‐resolution X‐ray microtomography for the evaluation of liver and spleen tumors in mice. Signal intensity dramatically increased in normal spleen and liver, while no uptake was observed in the respective tumors. Spleen and tumor segmentation was easily obtained. The smallest liver metastasis detected measured 0.3 mm in diameter. Furthermore, it was possible to observe an increased signal in the liver and spleen 15 days after injection of DHOG. This finding may facilitate follow‐up of the tumor growth.
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Three groups of female nude mice were compared: controls (n = 5), and mice injected with 2.5 × 106 STC1 tumor cells in the spleen, imaged at 15 days (group G15, n = 5) and at 30 days (group G30, n = 5, of which one died before imaging). Micro‐CT scans (X‐ray voltage, 50 kVp; anode current, 200 µA; exposure time, 632 ms; 180 rotational steps resulting in 35 µm isotropic spatial resolution) were acquired at 0, 0.75, 2 and 4 h after i.v. injection of DHOG. CT number (Hounsfield units: HU) and contrast‐to‐noise ratios (CNR) were determined in three organs. Statistical analysis was performed by Mann–Whitney U‐test. Contrast enhancement in normal spleen and liver increased, respectively to 1020 ± 159 and 351 ± 27 HU over baseline at 4 h, and 482 ± 3 and 203 ± 14 HU on day 6 after a single contrast injection. Automated three‐dimensional reconstruction and modeling of the spleen provided accurate and quantifiable images. 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Three groups of female nude mice were compared: controls (n = 5), and mice injected with 2.5 × 106 STC1 tumor cells in the spleen, imaged at 15 days (group G15, n = 5) and at 30 days (group G30, n = 5, of which one died before imaging). Micro‐CT scans (X‐ray voltage, 50 kVp; anode current, 200 µA; exposure time, 632 ms; 180 rotational steps resulting in 35 µm isotropic spatial resolution) were acquired at 0, 0.75, 2 and 4 h after i.v. injection of DHOG. CT number (Hounsfield units: HU) and contrast‐to‐noise ratios (CNR) were determined in three organs. Statistical analysis was performed by Mann–Whitney U‐test. Contrast enhancement in normal spleen and liver increased, respectively to 1020 ± 159 and 351 ± 27 HU over baseline at 4 h, and 482 ± 3 and 203 ± 14 HU on day 6 after a single contrast injection. Automated three‐dimensional reconstruction and modeling of the spleen provided accurate and quantifiable images. Spleen tumor and liver metastases did not take up DHOG, making them detectable in contrast to the increased signal in normal tissue. The smallest liver metastasis detected measured 0.3 mm in diameter. High‐resolution X‐ray micro‐CT in living mice using DHOG contrast agent allowed visualization and volume quantification of normal spleen and of spleen tumor and its liver metastases. Copyright © 2007 John Wiley &amp; Sons, Ltd. The present study sought to validate the use of a specific contrast agent (DHOG) with high‐resolution X‐ray microtomography for the evaluation of liver and spleen tumors in mice. Signal intensity dramatically increased in normal spleen and liver, while no uptake was observed in the respective tumors. Spleen and tumor segmentation was easily obtained. The smallest liver metastasis detected measured 0.3 mm in diameter. Furthermore, it was possible to observe an increased signal in the liver and spleen 15 days after injection of DHOG. This finding may facilitate follow‐up of the tumor growth.</abstract><cop>Chichester, UK</cop><pub>John Wiley &amp; Sons, Ltd</pub><pmid>17444558</pmid><doi>10.1002/cmmi.130</doi><tpages>6</tpages></addata></record>
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subjects Animals
contrast agent
Contrast Media - pharmacology
Diagnostic Imaging - methods
Female
Image Processing, Computer-Assisted
liver metastasis
Liver Neoplasms - pathology
Mice
Micro-CT
Models, Statistical
Neoplasm Metastasis
Neoplasm Transplantation
spleen tumor
Splenic Neoplasms - pathology
Tomography, X-Ray Computed - methods
title In-vivo high-resolution X-ray microtomography for liver and spleen tumor assessment in mice
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