[HTML][HTML] Semi-quantitative analyses of metabolic systems of human colon cancer metastatic xenografts in livers of superimmunodeficient NOG mice

A Kubo, M Ohmura, M Wakui, T Harada… - Analytical and …, 2011 - Springer
A Kubo, M Ohmura, M Wakui, T Harada, S Kajihara, K Ogawa, H Suemizu, M Nakamura…
Analytical and bioanalytical chemistry, 2011Springer
Analyses of energy metabolism in human cancer have been difficult because of rapid
turnover of the metabolites and difficulties in reducing time for collecting clinical samples
under surgical procedures. Utilization of xenograft transplantation of human-derived colon
cancer HCT116 cells in spleens of superimmunodeficient NOD/SCID/IL-2Rγ null (NOG)
mice led us to establish an experimental model of hepatic micrometastasis of the solid
tumor, whereby analyses of the tissue sections collected by snap-frozen procedures through …
Abstract
Analyses of energy metabolism in human cancer have been difficult because of rapid turnover of the metabolites and difficulties in reducing time for collecting clinical samples under surgical procedures. Utilization of xenograft transplantation of human-derived colon cancer HCT116 cells in spleens of superimmunodeficient NOD/SCID/IL-2Rγnull (NOG) mice led us to establish an experimental model of hepatic micrometastasis of the solid tumor, whereby analyses of the tissue sections collected by snap-frozen procedures through newly developed microscopic imaging mass spectrometry (MIMS) revealed distinct spatial distribution of a variety of metabolites. To perform intergroup comparison of the signal intensities of metabolites among different tissue sections collected from mice in fed states, we combined matrix-assisted laser desorption/ionization time-of-flight imaging mass spectrometry (MALDI–TOF-IMS) and capillary electrophoresis–mass spectrometry (CE–MS), to determine the apparent contents of individual metabolites in serial tissue sections. The results indicated significant elevation of ATP and energy charge in both metastases and the parenchyma of the tumor-bearing livers. To note were significant increases in UDP-N-acetyl hexosamines, and reduced and oxidized forms of glutathione in the metastatic foci versus the liver parenchyma. These findings thus provided a potentially important method for characterizing the properties of metabolic systems of human-derived cancer and the host tissues in vivo.
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