模态(人机交互)
计算机科学
人工智能
特征(语言学)
分割
模式识别(心理学)
模式
特征学习
稳健性(进化)
掷骰子
深度学习
缺少数据
机器学习
数学
基因
哲学
社会学
生物化学
语言学
化学
社会科学
几何学
作者
Yueqin Diao,Fan Li,Zhiyuan Li
标识
DOI:10.1016/j.compbiomed.2023.107234
摘要
Multimodal Magnetic Resonance Imaging (MRI) can provide valuable complementary information and substantially enhance the performance of brain tumor segmentation. However, it is common for certain modalities to be absent or missing during clinical diagnosis, which can significantly impair segmentation techniques that rely on complete modalities. Current advanced methods attempt to address this challenge by developing shared feature representations via modal fusion to handle different missing modality situations. Considering the importance of missing modality information in multimodal segmentation, this paper utilize a feature reconstruction method to recover the missing information, and proposes a joint learning-based feature reconstruction and enhancement method for incomplete modality brain tumor segmentation. The method leverages an information learning mechanism to transfer information from the complete modality to a single modality, enabling it to obtain complete brain tumor information, even without the support of other modalities. Additionally, the method incorporates a module for reconstructing missing modality features, which recovers fused features of the absent modality through utilizing the abundant potential information obtained from the available modalities. Furthermore, the feature enhancement mechanism improves shared feature representation by utilizing the information obtained from the missing modalities that have been reconstructed. These processes enable the method to obtain more comprehensive information regarding brain tumors in various missing modality circumstances, thereby enhancing the model's robustness. The performance of the proposed model was evaluated on BraTS datasets and compared with other deep learning algorithms using Dice similarity scores. On the BraTS2018 dataset, the proposed algorithm achieved a Dice similarity score of 86.28%, 77.02%, and 59.64% for whole tumors, tumor cores, and enhanced tumors, respectively. These results demonstrate the superiority of our framework over state-of-the-art methods in missing modalities situations.
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