Spatial correlation between in vivo imaging and immunohistochemical biomarkers: A methodological study

体内成像与免疫组织化学生物标志物之间的空间相关性:一项方法学研究

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Abstract

In this study, we present a method that enables voxel-by-voxel comparison of in vivo imaging to immunohistochemistry (IHC) biomarkers. As a proof of concept, we investigated the spatial correlation between dynamic contrast enhanced (DCE-)CT parameters and IHC biomarkers Ki-67 (proliferation), HIF-1α (hypoxia), and CD45 (immune cells). 54 whole-mount tumor slices of 15 laryngeal and hypopharyngeal carcinomas were immunohistochemically stained and digitized. Heatmaps of biomarker positivity were created and registered to DCE-CT parameter maps. The adiabatic approximation to the tissue homogeneity model was used to fit the following DCE parameters: K(trans) (transfer constant), V(e) (extravascular and extracellular space), and V(i) (intravascular space). Both IHC and DCE maps were downsampled to 4 × 4 × 3 mm[3] voxels. The mean values per tumor were used to calculate the between-subject correlations between parameters. For the within-subject (spatial) correlation, values of all voxels within a tumor were compared using the repeated measures correlation (r(rm)). No between-subject correlations were found between IHC biomarkers and DCE parameters, whereas we found multiple significant within-subject correlations: V(e) and Ki-67 (r(rm) = -0.17, P < .001), V(e) and HIF-1α (r(rm) = -0.12, P < .001), K(trans) and CD45 (r(rm) = 0.13, P < .001), V(i) and CD45 (r(rm) = 0.16, P < .001), and V(i) and Ki-67 (r(rm) = 0.08, P = .003). The strongest correlation was found between IHC biomarkers Ki-67 and HIF-1α (r(rm) = 0.35, P < .001). This study shows the technical feasibility of determining the 3 dimensional spatial correlation between histopathological biomarker heatmaps and in vivo imaging. It also shows that between-subject correlations do not reflect within-subject correlations of parameters.

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