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Development and Validation of a Deep-Learning Network for Detecting Congenital Heart Disease from Multi-View Multi-Modal Transthoracic Echocardiograms
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Mingmei Cheng1, , Jing Wang2, 3, , Xiaofeng Liu4, Yanzhong Wang5, Qun Wu2, Fangyun Wang2, Pei Li2, Binbin Wang6, 7, *, Xin Zhang2, *, Wanqing Xie1, 8, *
Research. Vol 7 Article ID 0319
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Research. Vol 7 Article ID 0319
Research Article
Development and Validation of a Deep-Learning Network for Detecting Congenital Heart Disease from Multi-View Multi-Modal Transthoracic Echocardiograms
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Mingmei Cheng1, , Jing Wang2, 3, , Xiaofeng Liu4, Yanzhong Wang5, Qun Wu2, Fangyun Wang2, Pei Li2, Binbin Wang6, 7, *, Xin Zhang2, *, Wanqing Xie1, 8, *
Affiliations
  • 1Department of Intelligent Medical Engineering, School of Biomedical Engineering, Department of Psychology, School of Mental Health and Psychological Sciences, Anhui Medical University, Hefei 230011, China.
  • 2 Heart Center, Beijing Children's Hospital, Capital Medical University, National Center for Children's Health, Beijing 10045, China.
  • 3 School of Basic Medical Sciences, Capital Medical University, Beijing 10069, China.
  • 4 Gordon Center for Medical Imaging, Harvard Medical School, and Massachusetts General Hospital, Boston, MA 02114, USA.
  • 5 School of Life Course and Population Sciences, Faculty of Life Science and Medicine, King's College London, London, UK.
  • 6Center for Genetics, National Research Institute for Family Planning, Beijing 100730, China.
  • 7Graduated School, Peking Union Medical College, Beijing 100730, China.
  • 8Beth Israel Deaconess Medical Center, Harvard Medical School, Harvard University, Boston, MA 02215, USA.
Published: 2024-03-06 doi: 10.34133/research.0319
Outline
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Early detection and treatment of congenital heart disease (CHD) can significantly improve the prognosis of children. However, inexperienced sonographers often face difficulties in recognizing CHD through transthoracic echocardiogram (TTE) images. In this study, 2-dimensional (2D) and Doppler TTEs of children collected from 2 clinical groups from Beijing Children's Hospital between 2018 and 2022 were analyzed, including views of apical 4 chamber, subxiphoid long-axis view of 2 atria, parasternal long-axis view of the left ventricle, parasternal short-axis view of aorta, and suprasternal long-axis view. A deep learning (DL) framework was developed to identify cardiac views, integrate information from various views and modalities, visualize the high-risk region, and predict the probability of the subject being normal or having an atrial septal defect (ASD) or a ventricular septaldefect (VSD). A total of 1,932 children (1,255 healthy controls, 292 ASDs, and 385 VSDs) were collected from 2 clinical groups. For view classification, the DL model reached a mean [SD] accuracy of 0.989 [0.001]. For CHD screening, the model using both 2D and Doppler TTEs with 5 views achieved a mean [SD] area under the receiver operating characteristic curve (AUC) of 0.996 [0.000] and an accuracy of 0.994 [0.002] for within-center evaluation while reaching a mean [SD] AUC of 0.990 [0.003] and an accuracy of 0.993 [0.001] for cross-center test set. For the classification of healthy, ASD, and VSD, the model reached the mean [SD] accuracy of 0.991 [0.002] and 0.986 [0.001] for within- and cross-center evaluation, respectively. The DL models aggregating TTEs with more modalities and scanning views attained superior performance to approximate that of experienced sonographers. The incorporation of multiple views and modalities of TTEs in the model enables accurate identification of children with CHD in a noninvasive manner, suggesting the potential to enhance CHD detection performance and simplify the screening process.

Mingmei Cheng, Jing Wang, Xiaofeng Liu, Yanzhong Wang, Qun Wu, Fangyun Wang, Pei Li, Binbin Wang, Xin Zhang, Wanqing Xie. Development and Validation of a Deep-Learning Network for Detecting Congenital Heart Disease from Multi-View Multi-Modal Transthoracic Echocardiograms[J]. Research, 2024 , 7 (3) : 0319 . DOI: 10.34133/research.0319
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Introduction
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Congenital heart disease (CHD) is typically defined as a great vessel disease at birth caused by abnormal development of the embryonic heart and vascular tissue. With a prevalence of approximately 4 to 50 per 1,000 live births, it is one of the most common congenital anomalies worldwide [1,2] and can bring a heavy health and financial burden to patients. Early CHD screening and treatment can significantly improve children's prognosis and quality of life and prevent irreversible pulmonary vascular disease [1,3]. Among the subtypes of CHD, atrial septal defect (ASD) and ventricular septal defect (VSD) are the most common, accounting for about 10% and 40% of CHDs, respectively [4,5]. In China, the prevalence of CHD is about 0.4% to 0.7% [6]. With the advancement of medical technology and the increased dissemination of medical knowledge, CHD has gained increasing attention in China, and most simple CHDs can now be effectively treated with prompt surgery [7]. However, the medical accessibility and service quality for CHD is still low in China [8,9]. Thus, an auxiliary CHD screening system that allows inexperienced sonographers and general practitioners to perform transthoracic echocardiogram (TTE) in a simple and easy-to-use way, thereby improving the CHD screening rate and scope, is urgently needed.
Two-dimensional (2D) and Doppler ultrasound techniques reflect distinct echocardiographic information crucial for understanding cardiac structure and blood flow dynamics [10]. CHD often manifests prominent features in both 2D and Doppler TTEs, facilitating the diagnosis of CHD. However, for those inexperienced cardiac sonographers, the detection of CHD can be difficult, leading to misdiagnosis and missed diagnosis.
Deep learning (DL), one of the most advanced technologies in artificial intelligence, has been applied to various tasks in medical fields, such as disease diagnosis [11,12], lesion location [13,14], target region segmentation [1517], abnormality detection [18], data analysis [19], measurement [20], biomedicine [21,22], and emotion recognition [23,24]. Some attempts have also tried to apply DL to the diagnosis or treatment planning for CHD [2529]. However, developing a DL model that can comprehensively analyze multi-modal TTE images from different views to achieve more accurate identification of CHD remains a significant challenge currently under exploration.
The 2D and Doppler TTEs of 5 cardiac views from 1,932 subjects are collected in this study. Though rich information can be expected in multi-modal and multi-view depictions, it also poses challenges to exploiting the meaningful features in this high-dimensional data. In addition, some of the TTE modalities or views may be corrupted with noise or unstable motion in scanning or lost in the electronic health record transition. The regular multi-modal and multi-view TTE is often unavailable in real-world implementation while rescanning can be costly or even prohibitive. Toward the above difficulties, we integrate different TTEs to generate better diagnostic predictions through a hierarchical architecture while retaining the feasibility of flexibly handling the TTEs available. By considering more comprehensive TTE data, we hypothesized that the DL network could produce high-quality diagnostic predictions close to those of experienced clinical experts, providing richer information and better auxiliary diagnostic service.
Results
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We analyzed the TTE data of 1,308 (823 healthy controls, 209 ASDs, and 276 VSDs) and 624 children (432 healthy controls, 83 ASDs, and 109 VSDs) from the within- and cross-center datasets, respectively. More characteristics of the children in each group are summarized in Table 1. For within-center validation, the training data are randomly sampled from the within-center dataset, and the remaining data constitute the within-center test set. Instead of a fixed ratio, we used different ratios of training and testing datasets to assess the performance of the CHD detection model. To further validate the performance of our framework, the cross-center dataset is employed to test the model,s recognition results and generalization ability. The training and test data of the within-center dataset and the validation data of the cross-center dataset are randomly shuffled before being fed into the AI network.
Automatic view classification of TTEs
Our view classification model determines which of the 5 views (the apical 4 chambers view [A4C], the subxiphoid long-axis view [SXLAX] of 2 atria, the parasternal long-axis view [PSLAX] of the left ventricle, the parasternal short-axis view [PSSAX] of aorta, and the suprasternal long-axis view [SSLAX]) each image belongs to. When the ratio for training and testing in the first dataset is 8:2, the accuracy of the view classification model is 0.989, with a mean average precision (mAP) of 0.990 and a mean intersection over union (mIoU) of 0.979. The corresponding confusion matrix is shown in Fig. S1. With the training and test set ratio of 2:8, our view classifier can still reach an accuracy (ACC) of 0.978, an mAP of 0.978, and an mIoU of 0.957. The performance on the second evaluation dataset is 0.983 for ACC, 0.989 for mAP, and 0.973 for mIoU based on the model using 80% of data in the first dataset for training, which shows the same tendency as those in the first dataset.
To further analyze the influence of the automatic view classifier on the final CHD classification, we performed the CHD classification based on the automatic view classification results (Table S1). For the first dataset, the 5-view multi-modal CHD classifier achieved 0.992 AUC for CHD screening (normal/patient), reaching 0.984 accuracy for the classification of negative/ASD/VSD. Compared with the CHD classification results based on the view recognition identified by the clinical experts (Table S2), the computer-aided diagnostic framework with automatic view identification achieved comparable results on both within- and cross-center evaluation sets.
CHD detection performance
CHD detection with multi-view TTEs
We conducted CHD identification based on each scanning view as well as the fusion of various views. For brevity, we refer to the fusion of A4C, SXLAX, and PSLAX as “3 view” for short and the fusion of 5 scanning views as “5 view” in our paper. The test results of the first dataset are shown in Table S2. When using only a single data modality, the 5-view model exhibited a 10.20% to 20.70% higher performance compared to the single-view model (training set proportion = 80%). When fusing 2 modalities of TTEs, the 5-view model exhibited a 7.00% to 12.7% higher performance than the single-view model. Furthermore, the receiver operating characteristic (ROC) curves presented in Fig. 1 provide additional evidence that the model utilizing multiple views of TTE data exhibits a significantly improved performance in recognizing CHD. The cross-center evaluation results present the consistent performance of our model (Table S2).
CHD detection with multi-modal TTEs
We conducted CHD detection using the 2D-TTE model, Doppler-TTE model, and multi-modal-TTE model. The prediction results are presented in Fig. 1 and Table S2. For the first dataset, when considering single-view TTEs, the multi-modal model achieved an accuracy improvement of 1.80% to 13.7% over the single-modal model (training set percentage = 80%). For 3-view and 5-view TTEs, the multi-modal model yielded higher accuracy than the single-modal model, with improvements ranging from 0.30% to 1.70% (training set percentage = 80%). The cross-center evaluation results (Table S2) also demonstrated that the fusion of modalities improves the performance of the model.
Comparison of CHD detection performance between the multi-view multi-modal model and human readers
One can see that the multi-view multi-modal models realized much superior discriminative performance compared to single-view or single-modal models on both test sets (Fig. 1 and Table S2). Confusion matrices of classification and violin plots of the prediction confidences of the multi-view multi-modal models are presented in Fig. 2. For the 5-view multi-modal model, the sensitivity and specificity both exceed 0.980 for distinguishing the healthy from CHD and the precision of each class are all higher than 0.940 for classifying the healthy/ASD/VSD (Fig. 2A). The mean probability of the correct predictions was almost 1.0, which was remarkably higher than that of incorrect predictions (Fig. 2B). Besides, to evaluate the feature discrimination between classes and the relationships between training and test data, we utilized 2D t-distributed stochastic neighbor embedding (tSNE) analysis (Fig. 2C and Fig. S4). Clear clustering of embeddings among healthy controls, ASDs, and VSDs was observed, along with high consistency in features between the training and testing sets. These findings provide insights into the model's ability to distinguish between healthy controls and various subtypes of CHD.
Four primary clinicians (under 3 years of clinical experience) at Beijing Children,s Hospital also conducted CHD recognition with the same testing images. The results of primary clinicians exceed 0.910 accuracy (mean) for distinguishing the healthy from CHD and 0.860 accuracy (mean) for the classification of healthy/ASD/VSD. To further evaluate the model's assistance for primary clinicians, these 4 doctors performed diagnosis on another 50 prospective children,s dataset with and without system support (Table 2). Whether for CHD screening or subtype determination, the accuracy of AI is much higher than that of primary doctors. With the support of the AI system, the accuracy and sensitivity of diagnosis by primary doctors have increased to about 0.95. It can be observed that our multi-view multi-modal DL framework exhibited better discriminative performance in CHD recognition compared to that of primary clinicians.
Diagnostic stability
We explored the model with training data percentages varying from 80% to 40% and conducted diagnostic classification experiments within the first dataset (Fig. 1, Tables S2 and S3). As the training ratio increased from 60% to 80%, the accuracy of the single-view single-modal models increased by 0.13% to 5.89%, while the performance of the multi-view and multi-modal models was boosted by 0.61% to 1.34%. As the volume of training data decreases, the diagnostic performance also decreases, particularly for the single-view single-modal models. However, the impact of decreased training data on multi-view and multi-modal models is significantly less pronounced. When the training set proportion drops to 40%, the 5-view multi-modal model can still perform effectively with an AUC of 0.983 for normal/patient classification and an accuracy of 0.968 for negative/ASD/VSD classification.
To investigate the recognition stability of the CHD diagnostic framework based on different DL models, we employed AlexNet [30], Vgg13 [31], and ResNet50 [32] for CHD detection. Descriptions of these network structures can be found in Fig. S2 and Appendix S6, and the corresponding results and analysis are shown in Table S4 and Appendix S7.
High-risk region visualization
By employing the gradient-weighted class activation mapping approach [33], we can visualize the regions in the images that are most relevant for distinguishing ASD and VSD in the DL models (Fig. 3). For instance, in the A4C view of 2D TTE, the model,s attention to ASD was focused on the location of the defect of the atrial septum, the right atrium with an enlarged inner diameter, and the left atrium with a reduced inner diameter. In the PSLAX view of Doppler TTE, the model,s identification of VSD was focused on the location of the defect and its left-to-right shunt signal, and the left atrium with an enlarged inner diameter. More visual results and detailed analysis are presented in Fig. S3 and Appendix S8. It is evident that the regions of interest identified by the DL model exhibited strong similarities to those identified by clinicians.
Discussion
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Early screening and intervention for CHD are of significant importance [34]. However, due to the complexity of CHD, the limitations of screening technology, and the limited experience of doctors in some underdeveloped areas, diagnosis of CHD remains a great challenge in many regions of the world. Although there is a great demand for an accurate, flexible, and stable CHD recognition system, developing an effective AI auxiliary diagnostic model that integrates multiple types of TTEs to attain the diagnostic proficiency of an experienced clinician remains a challenge. In this study, we collected 2D and Doppler TTEs with 5 views from 1,932 children, providing a new opportunity to investigate the performance of a DL recognition model in identifying pathology patterns across different views and modalities.
Our comprehensive multi-view multi-modal CHD recognition model showed superior performance in CHD screening on both within- and cross-center test sets. Our model reached an AUC of 0.996 and an accuracy of 0.991 for negative/ASD/VSD classification (using a training data proportion of 80% on the first dataset), which approximates the diagnostic accuracy of experienced sonographers. This performance demonstrated that the framework has the potential to assist not only in the early and large-scale screening for CHD but also in clinical diagnosis and may aid in the discrimination of more subtypes. Furthermore, the multi-view multi-modal model exhibited significantly higher diagnostic performance than the single-view single-modal model. This demonstrated that the diagnostic model based on deep-learning technology not only can efficiently process a large amount of data, but also can fully mine and analyze the information in multiple TTE images, so as to reach the diagnostic proficiency of experienced clinicians. As a systematic detection system, our model extracts images from each view and modality separately, and then generates prediction information through feature fusion. Therefore, when only single-modal or single-view TTE data are available, our model can also provide clinical diagnostic information, such as prediction probability and high-risk region saliency map. This reveals the framework,s flexible detection capability to adapt to different clinical scenarios. For instance, even in the event of partial loss of TTE data during storage and transmission, our system is still capable of diagnostic prediction, which provides great convenience for clinical data collection and computer-aided CHD screening.
The framework can also be used as standalone software to analyze data for studies, as well as online software to perform real-time detection of CHD, benefiting from its high performance and quick inference speed (lower than 2.3 ms for CHD classification per subject). Based on the keyframe selection scheme, the multi-view multi-modal CHD classification model not only obtains effective information for detection but also reduces the computational speed and memory space occupation, thereby reducing the system's requirements for hardware devices and improving the practicality and scope of clinical application. Furthermore, the excellent implantability and scalability of our model allow it to be embedded in many clinical devices and process diverse data, thereby facilitating the implementation of telemedicine.
Generally, in most studies, the test set proportion ranges from 10% to 20%. However, in this study, we used various test set ratios ranging from 20% to 60% to observe the stability of the model. When the test set size was 1.5 times that of the training set, our multi-view multi-modal recognition framework still achieved superior results, with an AUC of 0.983 for screening and an ACC of 0.968 for classifying negative/ASD/VSD. In addition, there are many reasons that can lead to low-quality TTEs in real-life clinical environments. Therefore, an AI model trained with manually selected high-quality data cannot offer reliable prediction facing real-life data. The dataset in this study was all collected from real clinical settings, and the isovolumic relaxation phase TTEs were obtained through an automatic keyframe selection rather than a manual selection. The multi-view and multi-modal model architecture greatly enhances the model's resistance to noise and interference in the data, improves the model's robustness, and allows it to be performed more reliably in clinical applications.
The number of images in each 2D and Doppler study can already reach as many as thousands, not to mention the huge amount of video data of 2 modalities from 5 views. It is necessary to free observers from the repetitive work of manually identifying the keyframe TTE for diagnosis and distinguishing different views of images, which is very time-consuming. The experimental results demonstrate the superior performance of our scanning view discriminability and simultaneously illustrate how our overall framework for CHD detection can serve clinical diagnosis in multiple aspects. By fusing the view classifier with CHD detection into a systematic framework, it provides support for computer-aided recognition systems to adaptively fuse various types of TTE data for more flexible and accurate diagnosis, as well as further promote the generalization for the screening of other subtypes of CHD and even other rare heart diseases.
The CAM figures showed the region in images that contributed the most to diagnostic prediction, giving a deep insight into the inference scheme of the DL model, which highly correlated with the structural information of the heart that is of clinical concern in CHD. Considering the complexities of CHD and clinical courses, it is crucial to identify and visually represent regions that signify high-risk information, providing more detailed information on the location of interest in each TTE image and facilitating subsequent surgical planning.
Our study has several limitations. ASD and VSD are the most common subtypes of CHD; it is promising to collect more data subtypes for a more comprehensive detection of CHD. In addition, TTE is widely used in clinical assessment of cardiac-related symptoms. Thus, other rare heart diseases can be incorporated into our study, providing convenience for early screening of more heart diseases. Besides, more diverse and detailed information needs to be explored, such as target location, distance, and area size, so that the system can provide more comprehensive information to serve clinical needs, especially by offering better support for the surgical plan of CHD, which is the direction of our future work. In addition, data from other vendors of ultrasound equipment need to be considered, which is the future work that we will keep working on.
Our study has developed and validated a comprehensive framework for CHD detection using 2D and Doppler TTE images from various scanning views, including A4C, SXLAX, PSLAX, PSSAX, and SSLAX. The system exhibited excellent performance in classifying scanning views and identifying healthy individuals, as well as those with ASD or VSD. The results suggest that the model has the potential to facilitate and improve widespread screening and the distinguishing of CHD subtypes in children.
Materials and Methods
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Study design and data collection
This study utilized 2D and Doppler TTE images of 1,932 children (1,255 healthy controls, 292 ASDs, and 385 VSDs) from 2 clinical groups from Beijing Children's Hospital between 2018 and 2022. The first dataset contained 1,308 children (823 healthy controls, 209 ASDs, and 276 VSDs), and the second dataset included 624 children (432 healthy controls, 83 ASDs, and 109 VSDs) collected from different sonographers in Beijing Children's Hospital. The study protocol was approved by the Ethics Committee of Beijing Children's Hospital (No. 2019-k-342), and all samples recruited in the present study were from outpatients or inpatients of the heart center. After the TTE examination, the TTE data from a total of 1,932 individuals with no cardiac structural abnormalities were used as healthy control data. The individuals diagnosed with ASD or VSD were recruited as positive cases. All subjects were determined by at least 2 experienced senior sonographers (chief physician, over 15 years of experience, over 150,000 ultrasound examinations) or intraoperative final diagnosis. Among CHD patients, we also recorded the following treatment: 196 ASD and 70 VSD patients were treated with transcatheter closure, while 96 ASD and 315 VSD patients were treated with surgical closure. More detailed statistics of the within- or cross-center dataset are shown in Table 1.
PHILIPS iE 33, iE Elite, and EPIQ 7C (Philips Electronics Nederland B.V.) with transducer frequency ranging from 3 to 8 MHz were adopted as data acquisition equipment. Given the analysis of the atrial septum and ventricular septum, the heart defect was identified, and cavity or pulmonary venous return was noted [19]. Each patient was placed in the supine position and captured with 1 to 5 views of 2D and Doppler-TTE data, providing sufficient information for clinical AI-assisted detection. According to the recommendation of clinical experts, we collected 5 standard views: A4C, SXLAX, PSLAX, PSSAX, and SSLAX, which provide sufficient information for the diagnosis of most CHDs. To facilitate the TTE data collection, processing, and analysis, we adopted a keyframe selection method [5], which selects the isovolumic relaxation phase as the keyframe when the ventricles finish contracting and start to relax. More description of data collection, data pre-processing, and the strategies for handling class imbalance can be found in Appendix S1, Appendix S2, and Fig. S5.
Framework development
The overall CHD detection framework consists of scanning view and modality recognition, CHD diagnostic prediction, and high-risk region visualization. The diagnostic part first explores the information from every 5 scanning images of 2 modalities with 10 sub-models. It then comprehensively investigates the coupling relationships in the high-dimensional embedding space of hidden layers of the DL model to provide the diagnostic classifier with more reliable features. This hierarchical architecture helps generate more accurate probability predictions of whether each subject is normal, has ASD, or has VSD. The overview of our framework is shown in Fig. 4.
Concretely, the distinction between 2D and Doppler TTE can be directly realized through the color channel measurement. For view classification, the classic DL network ResNet18 [23] was adopted to recognize which scanning view the image belongs to. To detect CHD using TTEs, we constructed a feature extraction module for each modality with a particular view using ResNet18. We also built a multi-level feature fusion network with a fully connected neural network (FCNN) to fuse the features. Finally, we employed a small FCNN module to construct the diagnostic classifier, which computes the probability of each subject being normal, having ASD, or having VSD. More details of the models, technical settings, and the training and inference time can be found in Appendix S3 and Appendix S4.
Statistical analysis
The ACC and area under the receiver operating characteristic curve (AUC) were chosen as the primary outcomes for CHD screening. We also employed the metrics of precision, sensitivity, and specificity, which provided further insights into the model,s ability to detect positive and negative samples. To assess the performance of our DL model in identifying the subtypes of CHD, we adopted ACC as the primary outcome. Additionally, we calculated the confusion matrix, mAP, and the mIoU to gain detailed information on the classification of each subtype and the model,s subtype recognition performance. Cross-center test was further conducted to evaluate the generality of our CHD identification framework, and the same metrics as those of within-center evaluation were adopted for the cross-center evaluation. All experiments were implemented 10 times to compute the standard deviation.
In general, to train and test the performance of a model, the dataset is partitioned into training and testing sets at a fixed ratio, such as 8:2. However, for many AI models, the size of the training dataset has a significant impact on the model,s detection ability, which may sharply decline as the proportion of the training set decreases. To evaluate the stability of our CHD detection model under different training set ratios, we trained and tested our CHD recognition framework using the within-center dataset with various training set proportions ranging from 80% to 40% and the remaining data for testing. We used the ACC and AUC for CHD screening and the ACC for CHD subtype discrimination to observe whether the CHD recognition framework can maintain effective and stable detection results with a reduced amount of training data. Furthermore, we used the same metrics to investigate the influence of different DL architectures on the performance of the CHD detection framework using multi-view and multi-modal TTEs.
The performance of scanning view distinguishing was evaluated using ACC, mAP, mIoU, and the confusion matrix. More details of the statistical analysis are described in Appendix S5.
Funding
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  • Beijing Natural Science Foundation(JQ21037)
  • Beijing Municipal Administration of Hospitals Youth Programme(QML20191208)
  • Science Foundation for Youths of Anhui Medical University(2022xkj012)
  • University Natural Science Research Project of Anhui Province (2022AH050696)
  • Research Fund for the Doctoral Program of Anhui Medical University(1401020201)
  • Research Fund for the Doctoral Program of Anhui Medical University(1401038201)
  • National Natural Science Foundation of China (62306012)
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Article Info
doi: 10.34133/research.0319
  • Receive Date:2023-08-14
  • Online Date:2025-07-24
  • Published:2024-03-06
Article Data
Affiliations
History
  • Received:2023-08-14
  • Accepted:2024-01-26
Funding
Beijing Natural Science Foundation(JQ21037)
Beijing Municipal Administration of Hospitals Youth Programme(QML20191208)
Science Foundation for Youths of Anhui Medical University(2022xkj012)
University Natural Science Research Project of Anhui Province (2022AH050696)
Research Fund for the Doctoral Program of Anhui Medical University(1401020201)
Research Fund for the Doctoral Program of Anhui Medical University(1401038201)
National Natural Science Foundation of China (62306012)
Affiliations
    1Department of Intelligent Medical Engineering, School of Biomedical Engineering, Department of Psychology, School of Mental Health and Psychological Sciences, Anhui Medical University, Hefei 230011, China.
    2 Heart Center, Beijing Children's Hospital, Capital Medical University, National Center for Children's Health, Beijing 10045, China.
    3 School of Basic Medical Sciences, Capital Medical University, Beijing 10069, China.
    4 Gordon Center for Medical Imaging, Harvard Medical School, and Massachusetts General Hospital, Boston, MA 02114, USA.
    5 School of Life Course and Population Sciences, Faculty of Life Science and Medicine, King's College London, London, UK.
    6Center for Genetics, National Research Institute for Family Planning, Beijing 100730, China.
    7Graduated School, Peking Union Medical College, Beijing 100730, China.
    8Beth Israel Deaconess Medical Center, Harvard Medical School, Harvard University, Boston, MA 02215, USA.

Corresponding:

* Address correspondence to: (X.Z.); (B.W.) (W.X.)
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表12种不同金属材料的力学参数

Family		 属数
Number of
genus		 种数
Number of
species		 占总种数比例
Percentage of
total species (%)
Genus		 种数
Number of
species		 占总种数比例
Percentage of total
species (%)
鹅膏菌科Amanitaceae 2 11 5.26 鹅膏菌属 Amanita 10 4.78
小菇科 Mycenaceae 2 12 5.74 丝盖伞属 Inocybe 5 2.39
多孔菌科 Polyporaceae 8 14 6.70 蜡蘑属 Laccaria 5 2.39
红菇科 Russulaceae 3 23 11.00 小皮伞属 Marasmius 6 2.87
小菇属 Mycena 11 5.26
光柄菇属 Pluteus 5 2.39
红菇属 Russula 17 8.13
栓菌属 Trametes 5 2.39
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