Quantitative characterization of the imaging limits of diffuse low-grade oligodendrogliomas

TL;DR

This study quantitatively compares histological tumor cell and edema fractions inside and outside MRI abnormalities in low-grade gliomas, revealing that edema mainly defines MRI margins and tumor activity varies across patients.

Contribution

It provides detailed histological validation of MRI-defined tumor margins, highlighting the role of edema and variable tumor cell cycling at tumor borders.

Findings

Edema fraction is higher inside MRI abnormalities.

Tumor cell concentration is higher inside MRI abnormalities.

Cycling tumor cell fraction varies at tumor borders.

Abstract

Background : Supratentorial diffuse low-grade gliomas in adults extend beyond maximal visible MRI-defined abnormalities, and a gap exists between the imaging signal changes and the actual tumor margins. Direct quantitative comparisons between imaging and histological analyses are lacking to date. However, they are of the utmost importance if one wishes to develop realistic models for diffuse glioma growth. Methods : In this study, we quantitatively compare the cell concentration and the edema fraction from human histological biopsy samples (BSs) performed inside and outside imaging abnormalities during serial imaging-based stereotactic biopsy of diffuse low-grade gliomas. Results : The cell concentration was significantly higher in BSs located inside (1189 $\pm$ 378 cell/mm$^2$) than outside (740 $\pm$ 124 cell/mm$^2$) MRI-defined abnormalities (p=0.0003). The edema fraction was significantly higher in BSs located inside (mean, 45 $\pm$ 23%) than outside (mean, 5 $\pm$ 9%) MRI-defined abnormalities (p<0.0001). At borders of the MRI-defined abnormalities, 20% of the tissue surface area was occupied by edema, and only 3% by tumor cells. The cycling cell concentration was significantly higher in BSs located inside (10 $\pm$ 12 cell/mm$^2$) compared to outside (0.5 $\pm$ 0.9 cell/mm$^2$) MRI-defined abnormalities (p=0.0001). Conclusions : We show that the margins of T2-weighted signal changes are mainly correlated with the edema fraction. In 62.5% of patients, the cycling tumor cell fraction (defined as the ratio of the cycling tumor cell concentration to the total number of tumor cells) was higher at the limits of the MRI-defined abnormalities than closer to the center of the tumor. In the remaining patients, the cycling tumor cell fraction increased towards the center of the tumor.