Abstract

It is a general assumption in deep learning that more training data leads to better performance, and that models will learn to generalize well across heterogeneous input data as long as that variety is represented in the training set. Segmentation of brain tumors is a well-investigated topic in medical image computing, owing primarily to the availability of a large publicly-available dataset arising from the long-running yearly Multimodal Brain Tumor Segmentation (BraTS) challenge. Research efforts and publications addressing this dataset focus predominantly on technical improvements of model architectures and less on properties of the underlying data. Using the dataset and the method ranked third in the BraTS 2018 challenge, we performed experiments to examine the impact of tumor type on segmentation performance. We propose to stratify the training dataset into high-grade glioma (HGG) and low-grade glioma (LGG) subjects and train two separate models. Although we observed only minor gains in overall mean dice scores by this stratification, examining case-wise rankings of individual subjects revealed statistically significant improvements. Compared to a baseline model trained on both HGG and LGG cases, two separately trained models led to better performance in 64.9% of cases (p < 0.0001) for the tumor core. An analysis of subjects which did not profit from stratified training revealed that cases were missegmented which had poor image quality, or which presented clinically particularly challenging cases (e.g., underrepresented subtypes such as IDH1-mutant tumors), underlining the importance of such latent variables in the context of tumor segmentation. In summary, we found that segmentation models trained on the BraTS 2018 dataset, stratified according to tumor type, lead to a significant increase in segmentation performance. Furthermore, we demonstrated that this gain in segmentation performance is evident in the case-wise ranking of individual subjects but not in summary statistics. We conclude that it may be useful to consider the segmentation of brain tumors of different types or grades as separate tasks, rather than developing one tool to segment them all. Consequently, making this information available for the test data should be considered, potentially leading to a more clinically relevant BraTS competition.

Highlights

  • Gliomas are primary brain tumors which arise from glial cells

  • While we agree on the whole tumor segmentation, we argue that the present T2-weighted hyperintensity indicates the presence of nonenhancing tumor rather than edema

  • We have proposed two ways of how to use data stratification to “conquer” brain tumor segmentation: First, the targeted application of a specialized model (HGG model) to the respective data (HGG test case)

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Summary

Introduction

Gliomas are primary brain tumors which arise from glial cells. According to the World Health Organization (WHO) classification of tumors of the central nervous system (CNS) (Louis et al, 2016), they can be grouped into different tumor grades based on the underlying histology and molecular characteristics. Glioma are managed depending on grade, with treatment strategies ranging from tumor resection followed by combined radio- and chemotherapy to a “watch and wait” approach (Stupp et al, 2005; Grier, 2006). The typical radiological appearance of a glioblastoma features a disrupted blood-brain barrier causing ring-enhancing lesions with central necrosis and peritumoral edema. Low-grade astrocytic tumors exhibit typically no contrast enhancement and are missing central necrosis (Pierallini et al, 1997)

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