Quantitative analysis of varying profiles of hypoxia in relation to functional vessels in different human glioma xenograft lines

PFJW Rijken, JPW Peters… - Radiation …, 2002 - meridian.allenpress.com
PFJW Rijken, JPW Peters, AJ Van der Kogel
Radiation research, 2002meridian.allenpress.com
Abstract Rijken, PFJW, Peters, JPW and van der Kogel, AJ Quantitative Analysis of Varying
Profiles of Hypoxia in Relation to Functional Vessels in Different Human Glioma Xenograft
Lines. Radiat. Res. 157, 626–632 (2002). Tissue oxygenation influences the radiation
response of tumors. To further investigate the underlying mechanisms of tumor hypoxia, the
spatial distribution of hypoxic cells in relation to the vasculature was studied. In a panel of
three human glioma xenograft lines (E2, E102, E106) with different growth characteristics …
Abstract
Rijken, P. F. J. W., Peters, J. P. W. and van der Kogel, A. J. Quantitative Analysis of Varying Profiles of Hypoxia in Relation to Functional Vessels in Different Human Glioma Xenograft Lines. Radiat. Res. 157, 626–632 (2002).
Tissue oxygenation influences the radiation response of tumors. To further investigate the underlying mechanisms of tumor hypoxia, the spatial distribution of hypoxic cells in relation to the vasculature was studied. In a panel of three human glioma xenograft lines (E2, E102, E106) with different growth characteristics, tumor line-specific patterns of hypoxia (pimonidazole) and (functional) vasculature (Hoechst 33342) were observed. Two of the three glioma lines showed a more homogeneous distribution of perfused vessels (E102 and E106) than the third glioma line (E2). Although all tumors showed hypoxia, the distance at which the steepest part of the gradient of the hypoxia marker was found varied significantly among the different glioma lines. The faster-growing E102 tumors had the longest distance (>300 μm). These results indicate that tumor line-specific factors, rather than vascular geometry alone, may determine the oxygenation status of a tumor. As a consequence, vascular density cannot be used as a surrogate parameter for tumor hypoxia when comparing different tumors. Additional hypoxia and perfusion markers will further improve our understanding of changes in tumor physiology at the microregional level explaining the relationship between the low oxygen levels and the response of tumors to treatment.
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