Uncertainty‐aware refinement framework for ovarian tumor segmentation in CECT volume

分割 计算机科学 豪斯多夫距离 雅卡索引 人工智能 卵巢癌 卵巢肿瘤 图像分割 模式识别(心理学) 医学 癌症 内科学
作者
Jiaqi Hu,Zhiming Cui,Xiao Zhang,Jiadong Zhang,Yuyan Ge,Honghe Zhang,Yan Lü,Dinggang Shen
出处
期刊:Medical Physics [Wiley]
卷期号:51 (4): 2678-2694
标识
DOI:10.1002/mp.16795
摘要

Abstract Background Ovarian cancer is a highly lethal gynecological disease. Accurate and automated segmentation of ovarian tumors in contrast‐enhanced computed tomography (CECT) images is crucial in the radiotherapy treatment of ovarian cancer, enabling radiologists to evaluate cancer progression and develop timely therapeutic plans. However, automatic ovarian tumor segmentation is challenging due to factors such as inhomogeneous background, ambiguous tumor boundaries, and imbalanced foreground‐background, all of which contribute to high predictive uncertainty for a segmentation model. Purpose To tackle these challenges, we propose an uncertainty‐aware refinement framework that aims to estimate and refine regions with high predictive uncertainty for accurate ovarian tumor segmentation in CECT images. Methods To this end, we first employ an approximate Bayesian network to detect coarse regions of interest (ROIs) of both ovarian tumors and uncertain regions. These ROIs allow a subsequent segmentation network to narrow down the search area for tumors and prioritize uncertain regions, resulting in precise segmentation of ovarian tumors. Meanwhile, the framework integrates two guidance modules that learn two implicit functions capable of mapping query features sampled according to their uncertainty to organ or boundary manifolds, guiding the segmentation network to facilitate information encoding of uncertain regions. Results Firstly, 367 CECT images are collected from the same hospital for experiments. Dice score, Jaccard, Recall, Positive predictive value (PPV), 95% Hausdorff distance (HD95) and Average symmetric surface distance (ASSD) for the testing group of 77 cases are 86.31%, 73.93%, 83.95%, 86.03%, 15.17 mm and 2.57 mm, all of which are significantly better than that of the other state‐of‐the‐art models. And results of visual comparison shows that the compared methods have more mis‐segmentation than our method. Furthermore, our method achieves a Dice score that is at least 20% higher than the Dice scores of other compared methods when tumor volumes are less than 20 cm, indicating better recognition ability to small regions by our method. And then, 38 CECT images are collected from another hospital to form an external testing group. Our approach consistently outperform the compared methods significantly, with the external testing group exhibiting substantial improvements across key evaluation metrics: Dice score (83.74%), Jaccard (69.55%), Recall (82.12%), PPV (81.61%), HD95 (12.31 mm), and ASSD (2.32 mm), robustly establishing its superior performance. Conclusions Experimental results demonstrate that the framework significantly outperforms the compared state‐of‐the‐art methods, with decreased under‐ or over‐segmentation and better small tumor identification. It has the potential for clinical application.
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