Histogram Analysis of Diffusion Weighted Imaging in Low-Grade Gliomas: in vivo Characterization of Tumor Architecture and Corresponding Neuropathology

Georg Alexander Gihr; Diana Horvath-Rizea; Elena Hekeler; Oliver Ganslandt; Hans Henkes; Karl-Titus Hoffmann; Cordula Scherlach; Stefan Schob

doi:10.3389/fonc.2020.00206

Histogram Analysis of Diffusion Weighted Imaging in Low-Grade Gliomas: in vivo Characterization of Tumor Architecture and Corresponding Neuropathology

Front Oncol. 2020 Feb 25:10:206. doi: 10.3389/fonc.2020.00206. eCollection 2020.

Authors

Georg Alexander Gihr¹, Diana Horvath-Rizea¹, Elena Hekeler², Oliver Ganslandt³, Hans Henkes¹, Karl-Titus Hoffmann⁴, Cordula Scherlach⁴, Stefan Schob⁴

Affiliations

¹ Katharinenhospital Stuttgart, Clinic for Neuroradiology, Stuttgart, Germany.
² Department for Pathology, Katharinenhospital Stuttgart, Stuttgart, Germany.
³ Katharinenhospital Stuttgart, Clinic for Neurosurgery, Stuttgart, Germany.
⁴ Department for Neuroradiology, University Hospital Leipzig, Leipzig, Germany.

Abstract

Background: Low-grade gliomas (LGG) in adults are usually slow growing and frequently asymptomatic brain tumors, originating from glial cells of the central nervous system (CNS). Although regarded formally as "benign" neoplasms, they harbor the potential of malignant transformation associated with high morbidity and mortality. Their complex and unpredictable tumor biology requires a reliable and conclusive presurgical magnetic resonance imaging (MRI). A promising and emerging MRI approach in this context is histogram based apparent diffusion coefficient (ADC) profiling, which recently proofed to be capable of providing prognostic relevant information in different tumor entities. Therefore, our study investigated whether histogram profiling of ADC distinguishes grade I from grade II glioma, reflects the proliferation index Ki-67, as well as the IDH (isocitrate dehydrogenase) mutation and MGMT (methylguanine-DNA methyl-transferase) promotor methylation status. Material and Methods: Pre-treatment ADC volumes of 26 LGG patients were used for histogram-profiling. WHO-grade, Ki-67 expression, IDH mutation, and MGMT promotor methylation status were evaluated. Comparative and correlative statistics investigating the association between histogram-profiling and neuropathology were performed. Results: Almost the entire ADC profile (p25, p75, p90, mean, median) was significantly lower in grade II vs. grade I gliomas. Entropy, as second order histogram parameter of ADC volumes, was significantly higher in grade II gliomas compared with grade I gliomas. Mean, maximum value (ADCmax) and the percentiles p10, p75, and p90 of ADC histogram were significantly correlated with Ki-67 expression. Furthermore, minimum ADC value (ADCmin) was significantly associated with MGMT promotor methylation status as well as ADC entropy with IDH-1 mutation status. Conclusions: ADC histogram-profiling is a valuable radiomic approach, which helps differentiating tumor grade, estimating growth kinetics and probably prognostic relevant genetic as well as epigenetic alterations in LGG.

Keywords: apparent diffusion coefficient; histogram analysis; histopathology; imaging biomarker; low-grade glioma; radiomics.