Your search keyword '"Lambin P"' showing total 284 results

1. Overcoming radioresistance with the hypoxia-activated prodrug CP-506: A pre-clinical study of local tumour control probability

Author

Yaromina, A., Koi, L., Schuitmaker, L., Wiel, A. M.-M. A., Dubois, L. J., (0000-0003-1776-9556) Krause, M., Lambin, P., Yaromina, A., Koi, L., Schuitmaker, L., Wiel, A. M.-M. A., Dubois, L. J., (0000-0003-1776-9556) Krause, M., and Lambin, P.

Abstract

Background and purpose: Tumour hypoxia is an established radioresistance factor. A novel hypoxia-activated prodrug CP-506 has been proven to selectively target hypoxic tumour cells and to cause anti-tumour activity. The current study investigates whether CP-506 improves outcome of radiotherapy in vivo. Materials and methods: Mice bearing FaDu and UT-SCC-5 xenografts were randomized to receive 5 daily injections of CP-506/vehicle followed by single dose (SD) irradiation. In addition, CP-506 was combined once per week with fractionated irradiation (30 fractions/6 weeks). Animals were followed-up to score all recurrences. In parallel, tumours were harvested to evaluate pimonidazole hypoxia, DNA damage (cH2AX), expression of oxidoreductases. Results: CP-506 treatment significantly increased local control rate after SD in FaDu, 62% vs. 27% (p = 0.024). In UT-SCC-5, this effect was not curative and only marginally significant. CP-506 induced significant DNA damage in FaDu (p = 0.009) but not in UT- SCC-5. Hypoxic volume (HV) was significantly smaller (p = 0.038) after pretreatment with CP-506 as compared to vehicle in FaDu but not in less responsive UT-SCC-5. Adding CP-506 to fractionated radiotherapy in FaDu did not result in significant benefit. Conclusion: The results support the use of CP-506 in combination with radiation in particular using hypofractionation schedules in hypoxic tumours. The magnitude of effect depends on the tumour model, therefore it is expected that applying appropriate patient stratification strategy will further enhance the benefit of CP-506 treatment for cancer patients. A phase I-IIA clinical trial of CP-506 in monotherapy or in combination with carboplatin or a checkpoint inhibitor has been approved (NCT04954599).

Published

2023

2. Improving shared decision making for lung cancer treatment by developing and validating an open-source web based patient decision aid for stage I-II non-small cell lung cancer.

Author

Halilaj, I., Ankolekar, A., Lenaers, A., Chatterjee, Avishek, Oberije, C.J.G., Eppings, L., Smit, H.J., Hendriks, L.E.L., Jochems, A., Lieverse, R.I.Y., Timmeren, J.E. van, Wind, A., Lambin, P., Halilaj, I., Ankolekar, A., Lenaers, A., Chatterjee, Avishek, Oberije, C.J.G., Eppings, L., Smit, H.J., Hendriks, L.E.L., Jochems, A., Lieverse, R.I.Y., Timmeren, J.E. van, Wind, A., and Lambin, P.

Abstract

Contains fulltext : 305014.pdf (Publisher’s version ) (Open Access), The aim of this study was to develop and evaluate a proof-of-concept open-source individualized Patient Decision Aid (iPDA) with a group of patients, physicians, and computer scientists. The iPDA was developed based on the International Patient Decision Aid Standards (IPDAS). A previously published questionnaire was adapted and used to test the user-friendliness and content of the iPDA. The questionnaire contained 40 multiple-choice questions, and answers were given on a 5-point Likert Scale (1-5) ranging from "strongly disagree" to "strongly agree." In addition to the questionnaire, semi-structured interviews were conducted with patients. We performed a descriptive analysis of the responses. The iPDA was evaluated by 28 computer scientists, 21 physicians, and 13 patients. The results demonstrate that the iPDA was found valuable by 92% (patients), 96% (computer scientists), and 86% (physicians), while the treatment information was judged useful by 92%, 96%, and 95%, respectively. Additionally, the tool was thought to be motivating for patients to actively engage in their treatment by 92%, 93%, and 91% of the above respondents groups. More multimedia components and less text were suggested by the respondents as ways to improve the tool and user interface. In conclusion, we successfully developed and tested an iPDA for patients with stage I-II Non-Small Cell Lung Cancer (NSCLC).

Published

2023

3. A fully automatic artificial intelligence-based CT image analysis system for accurate detection, diagnosis, and quantitative severity evaluation of pulmonary tuberculosis

Author

Yan, C.G., Yan, C.G., Wang, L.F., Lin, J., Xu, J., Zhang, T.J., Qi, J., Li, X.Y., Ni, W., Wu, G.Y., Huang, J.B., Xu, Y.K., Woodruff, H.C., Lambin, P., Yan, C.G., Yan, C.G., Wang, L.F., Lin, J., Xu, J., Zhang, T.J., Qi, J., Li, X.Y., Ni, W., Wu, G.Y., Huang, J.B., Xu, Y.K., Woodruff, H.C., and Lambin, P.

Abstract

Objectives An accurate and rapid diagnosis is crucial for the appropriate treatment of pulmonary tuberculosis (TB). This study aims to develop an artificial intelligence (AI)-based fully automated CT image analysis system for detection, diagnosis, and burden quantification of pulmonary TB. Methods From December 2007 to September 2020, 892 chest CT scans from pathogen-confirmed TB patients were retrospectively included. A deep learning-based cascading framework was connected to create a processing pipeline. For training and validation of the model, 1921 lesions were manually labeled, classified according to six categories of critical imaging features, and visually scored regarding lesion involvement as the ground truth. A "TB score" was calculated based on a network-activation map to quantitively assess the disease burden. Independent testing datasets from two additional hospitals (dataset 2, n = 99; dataset 3, n = 86) and the NIH TB Portals (n = 171) were used to externally validate the performance of the AI model. Results CT scans of 526 participants (mean age, 48.5 +/- 16.5 years; 206 women) were analyzed. The lung lesion detection subsystem yielded a mean average precision of the validation cohort of 0.68. The overall classification accuracy of six pulmonary critical imaging findings indicative of TB of the independent datasets was 81.08-91.05%. A moderate to strong correlation was demonstrated between the AI model-quantified TB score and the radiologist-estimated CT score. Conclusions The proposed end-to-end AI system based on chest CT can achieve human-level diagnostic performance for early detection and optimal clinical management of patients with pulmonary TB.

Published

2022

4. The creation of a large set of realistic synthetic microcalcification clusters for simulation in (contrast-enhanced) mammography images

Author

Van Camp, A., Cockmartin, L., Beuque, M., Woodruff, H., Marshall, N., Lambin, P., Bosmans, H., Van Camp, A., Cockmartin, L., Beuque, M., Woodruff, H., Marshall, N., Lambin, P., and Bosmans, H.

Abstract

Characterization of microcalcification clusters in the breast and differentiation between benign and malignant structures on (contrast-enhanced) mammography (CEM) images is of great importance to determine cancerous lesions. Computer algorithms may help performing these tasks, but typically need large sets of data for model training. Therefore this paper develops a method to create synthetic microcalcification clusters that can later be used to overcome data sparsity problems. Starting from descriptors of the shape and size, both benign and malignant microcalcifications were created and then combined into 3-dimensional cluster models given realistic geometric properties. The distributions of the largest diameter and the number of microcalcifications per cluster in a set of 500 simulated clusters were set such that they agreed with those of real clusters. An existing simulation tool was then extended to insert the clusters into processed, low-energy CEM background images with appropriate contrast values. In a validation study comprised of 40 real and 40 synthetic cases, radiologists were asked to evaluate realism and malignancy. It was found that the shape and the structure of the individual microcalcifications as well as the complete clusters were realistic. Thus the descriptors were chosen correctly and enabled a good classification between benign and malignant cases. The realistic brightness and boundary smoothness proved the simulation tool can correctly insert the 3D clusters into real background images and is suitable of creating a large set of realistic microcalcification clusters simulated in existing (contrast-enhanced) mammography images. With improvements on the correspondence of insertion location in craniocaudal and mediolateral oblique view, which proved more challenging to simulate realistically, this promising method is expected to be applicable for modeling complete synthetic cases. Such a dataset can be used for data enrichment where data sources ar

Published

2022

5. A fully automatic artificial intelligence-based CT image analysis system for accurate detection, diagnosis, and quantitative severity evaluation of pulmonary tuberculosis

Author

Yan, C.G., Wang, L.F., Lin, J., Xu, J., Zhang, T.J., Qi, J., Li, X.Y., Ni, W., Wu, G.Y., Huang, J.B., Xu, Y.K., Woodruff, H.C., Lambin, P., Yan, C.G., Wang, L.F., Lin, J., Xu, J., Zhang, T.J., Qi, J., Li, X.Y., Ni, W., Wu, G.Y., Huang, J.B., Xu, Y.K., Woodruff, H.C., and Lambin, P.

Abstract

Objectives An accurate and rapid diagnosis is crucial for the appropriate treatment of pulmonary tuberculosis (TB). This study aims to develop an artificial intelligence (AI)-based fully automated CT image analysis system for detection, diagnosis, and burden quantification of pulmonary TB. Methods From December 2007 to September 2020, 892 chest CT scans from pathogen-confirmed TB patients were retrospectively included. A deep learning-based cascading framework was connected to create a processing pipeline. For training and validation of the model, 1921 lesions were manually labeled, classified according to six categories of critical imaging features, and visually scored regarding lesion involvement as the ground truth. A "TB score" was calculated based on a network-activation map to quantitively assess the disease burden. Independent testing datasets from two additional hospitals (dataset 2, n = 99; dataset 3, n = 86) and the NIH TB Portals (n = 171) were used to externally validate the performance of the AI model. Results CT scans of 526 participants (mean age, 48.5 +/- 16.5 years; 206 women) were analyzed. The lung lesion detection subsystem yielded a mean average precision of the validation cohort of 0.68. The overall classification accuracy of six pulmonary critical imaging findings indicative of TB of the independent datasets was 81.08-91.05%. A moderate to strong correlation was demonstrated between the AI model-quantified TB score and the radiologist-estimated CT score. Conclusions The proposed end-to-end AI system based on chest CT can achieve human-level diagnostic performance for early detection and optimal clinical management of patients with pulmonary TB.

Published

2022

6. MRI-based delta-radiomics predicts pathologic complete response in high-grade soft-tissue sarcoma patients treated with neoadjuvant therapy

Author

Peeken, J.C., Peeken, J.C., Asadpour, R., Specht, K., Chen, E.Y., Klymenko, O., Akinkuoroye, V., Hippe, D.S., Spraker, M.B., Schaub, S.K., Dapper, H., Knebel, C., Mayr, N.A., Gersing, A.S., Woodruff, H.C., Lambin, P., Nyflot, M.J., Combs, S.E., Peeken, J.C., Peeken, J.C., Asadpour, R., Specht, K., Chen, E.Y., Klymenko, O., Akinkuoroye, V., Hippe, D.S., Spraker, M.B., Schaub, S.K., Dapper, H., Knebel, C., Mayr, N.A., Gersing, A.S., Woodruff, H.C., Lambin, P., Nyflot, M.J., and Combs, S.E.

Abstract

Purpose: In high-grade soft-tissue sarcomas (STS) the standard of care encompasses multimodal therapy regimens. While there is a growing body of evidence for prognostic pretreatment radiomic models, we hypothesized that temporal changes in radiomic features following neoadjuvant treatment ("delta-radio mics") may be able to predict the pathological complete response (pCR). Methods: MRI scans (T1-weighted with fat-saturation and contrast-enhancement (T1FSGd) and T2 weighted with fat-saturation (T2FS)) of patients with STS of the extremities and trunk treated with neoadjuvant therapy were gathered from two independent institutions (training: 103, external testing: 53 patients). pCR was defined as <5% viable cells. After segmentation and preprocessing, 105 radiomic features were extracted. Delta-radiomic features were calculated by subtraction of features derived from MRI scans obtained before and after neoadjuvant therapy. After feature reduction, machine learning modeling was performed in 100 iterations of 3-fold nested cross-validation. Delta-radiomic models were compared with single timepoint models in the testing cohort. Results: The combined delta-radiomic models achieved the best area under the receiver operating characteristic curve (AUC) of 0.75. Pre-therapeutic tumor volume was the best conventional predictor (AUC 0.70). The T2FS-based delta-radiomic model had the most balanced classification performance with a balanced accuracy of 0.69. Delta-radiomic models achieved better reproducibility than single timepoint radiomic models, RECIST or the peri-therapeutic volume change. Delta-radiomic models were significantly associated with survival in multivariate Cox regression. Conclusion: This exploratory analysis demonstrated that MRI-based delta-radiomics improves prediction of pCR over tumor volume and RECIST. Delta-radiomics may one day function as a biomarker for personalized treatment adaptations. (c) 2021 Elsevier B.V. All rights reserved. Radiotherapy and

Published

2021

7. Exploratory Radiomic Analysis of Conventional vs. Quantitative Brain MRI: Toward Automatic Diagnosis of Early Multiple Sclerosis

Author

Lavrova, E., Lavrova, E., Lommers, E., Woodruff, H.C., Chatterjee, A., Maquet, P., Salmon, E., Lambin, P., Phillips, C., Lavrova, E., Lavrova, E., Lommers, E., Woodruff, H.C., Chatterjee, A., Maquet, P., Salmon, E., Lambin, P., and Phillips, C.

Abstract

Conventional magnetic resonance imaging (cMRI) is poorly sensitive to pathological changes related to multiple sclerosis (MS) in normal-appearing white matter (NAWM) and gray matter (GM), with the added difficulty of not being very reproducible. Quantitative MRI (qMRI), on the other hand, attempts to represent the physical properties of tissues, making it an ideal candidate for quantitative medical image analysis or radiomics. We therefore hypothesized that qMRI-based radiomic features have added diagnostic value in MS compared to cMRI. This study investigated the ability of cMRI (T1w) and qMRI features extracted from white matter (WM), NAWM, and GM to distinguish between MS patients (MSP) and healthy control subjects (HCS). We developed exploratory radiomic classification models on a dataset comprising 36 MSP and 36 HCS recruited in CHU Liege, Belgium, acquired with cMRI and qMRI. For each image type and region of interest, qMRI radiomic models for MS diagnosis were developed on a training subset and validated on a testing subset. Radiomic models based on cMRI were developed on the entire training dataset and externally validated on open-source datasets with 167 HCS and 10 MSP. Ranked by region of interest, the best diagnostic performance was achieved in the whole WM. Here the model based on magnetization transfer imaging (a type of qMRI) features yielded a median area under the receiver operating characteristic curve (AUC) of 1.00 in the testing sub-cohort. Ranked by image type, the best performance was achieved by the magnetization transfer models, with median AUCs of 0.79 (0.69-0.90, 90% CI) in NAWM and 0.81 (0.71-0.90) in GM. The external validation of the T1w models yielded an AUC of 0.78 (0.47-1.00) in the whole WM, demonstrating a large 95% CI and a low sensitivity of 0.30 (0.10-0.70). This exploratory study indicates that qMRI radiomics could provide efficient diagnostic information using NAWM and GM analysis in MSP. T1w radiomics could be useful for a fast

Published

2021

8. A Prospectively Validated Prognostic Model for Patients with Locally Advanced Squamous Cell Carcinoma of the Head and Neck Based on Radiomics of Computed Tomography Images

Author

Keek, S.A., Keek, S.A., Wesseling, F.W.R., Woodruff, H.C., van Timmeren, J.E., Nauta, I.H., Hoffmann, T.K., Cavalieri, S., Calareso, G., Primakov, S., Leijenaar, R.T.H., Licitra, L., Ravanelli, M., Scheckenbach, K., Poli, T., Lanfranco, D., Vergeer, M.R., Leemans, C.R., Brakenhoff, R.H., Hoebers, F.J.P., Lambin, P., Keek, S.A., Keek, S.A., Wesseling, F.W.R., Woodruff, H.C., van Timmeren, J.E., Nauta, I.H., Hoffmann, T.K., Cavalieri, S., Calareso, G., Primakov, S., Leijenaar, R.T.H., Licitra, L., Ravanelli, M., Scheckenbach, K., Poli, T., Lanfranco, D., Vergeer, M.R., Leemans, C.R., Brakenhoff, R.H., Hoebers, F.J.P., and Lambin, P.

Abstract

Simple Summary Patients that suffer from advanced head and neck cancer have a low average survival chance. Improving prognosis could improve this survival rate as it may help in clinical decision making. Radiomics features calculated from images of the tumour describe tumour size, shape, and pattern. These characteristics may be linked to patient survival, which is investigated in this paper. We combined radiomics features with other biomarkers of survival of 809 patients to make a prognosis before treatment. We then compared the predicted prognosis with the actual outcome to see how well our model performs. Our model was able to make three distinct risk groups of low-, medium-, and high-survival patients. With these findings, doctors may make a better judgement of treatment and follow-up per patient, which might improve clinical outcomes. Background: Locoregionally advanced head and neck squamous cell carcinoma (HNSCC) patients have high relapse and mortality rates. Imaging-based decision support may improve outcomes by optimising personalised treatment, and support patient risk stratification. We propose a multifactorial prognostic model including radiomics features to improve risk stratification for advanced HNSCC, compared to TNM eighth edition, the gold standard. Patient and methods: Data of 666 retrospective- and 143 prospective-stage III-IVA/B HNSCC patients were collected. A multivariable Cox proportional-hazards model was trained to predict overall survival (OS) using diagnostic CT-based radiomics features extracted from the primary tumour. Separate analyses were performed using TNM8, tumour volume, clinical and biological variables, and combinations thereof with radiomics features. Patient risk stratification in three groups was assessed through Kaplan-Meier (KM) curves. A log-rank test was performed for significance (p-value < 0.05). The prognostic accuracy was reported through the concordance index (CI). Results: A model combining an 11-feature rad

Published

2021

9. MRI-Based Radiomics Analysis for the Pretreatment Prediction of Pathologic Complete Tumor Response to Neoadjuvant Systemic Therapy in Breast Cancer Patients: A Multicenter Study

Author

Granzier, R.W.Y., Granzier, R.W.Y., Ibrahim, A., Primakov, S.P., Samiei, S., van Nijnatten, T.J.A., de Boer, M., Heuts, E.M., Hulsmans, F.J., Chatterjee, A., Lambin, P., Lobbes, M.B.I., Woodruff, H.C., Smidt, M.L., Granzier, R.W.Y., Granzier, R.W.Y., Ibrahim, A., Primakov, S.P., Samiei, S., van Nijnatten, T.J.A., de Boer, M., Heuts, E.M., Hulsmans, F.J., Chatterjee, A., Lambin, P., Lobbes, M.B.I., Woodruff, H.C., and Smidt, M.L.

Abstract

Simple SummaryThe prediction of pathologic complete response (pCR) to neo-adjuvant systemic therapy (NST) based on radiological assessment of pretreatment MRI exams in breast cancer patients is not possible to date. In this study, we investigated the value of pretreatment MRI-based radiomics analysis for the prediction of pCR to NST. Radiomics, clinical, and combined models were developed and validated based on MRI exams containing 320 tumors collected from two hospitals. The clinical models significantly outperformed the radiomics models for the prediction of pCR to NST and were of similar or better performance than the combined models. This indicates poor performance of the radiomics features and that in these scenarios the radiomic features did not have an added value for the clinical models developed. Due to previous and current work, we tentatively attribute the lack of significant improvement in clinical models following the addition of radiomics features to the effects of variations in acquisition and reconstruction parameters. The lack of reproducibility data meant this effect could not be analyzed. These results indicate the need for reproducibility studies to preselect reproducible features in order to properly assess the potential of radiomics.This retrospective study investigated the value of pretreatment contrast-enhanced Magnetic Resonance Imaging (MRI)-based radiomics for the prediction of pathologic complete tumor response to neoadjuvant systemic therapy in breast cancer patients. A total of 292 breast cancer patients, with 320 tumors, who were treated with neo-adjuvant systemic therapy and underwent a pretreatment MRI exam were enrolled. As the data were collected in two different hospitals with five different MRI scanners and varying acquisition protocols, three different strategies to split training and validation datasets were used. Radiomics, clinical, and combined models were developed using random forest classifiers in each strategy. The analy

Published

2021

10. Structural and functional radiomics for lung cancer

Author

Wu, G.Y., Wu, G.Y., Jochems, A., Refaee, T., Ibrahim, A., Yan, C.G., Sanduleanu, S., Woodruff, H.C., Lambin, P., Wu, G.Y., Wu, G.Y., Jochems, A., Refaee, T., Ibrahim, A., Yan, C.G., Sanduleanu, S., Woodruff, H.C., and Lambin, P.

Abstract

Introduction Lung cancer ranks second in new cancer cases and first in cancer-related deaths worldwide. Precision medicine is working on altering treatment approaches and improving outcomes in this patient population. Radiological images are a powerful non-invasive tool in the screening and diagnosis of early-stage lung cancer, treatment strategy support, prognosis assessment, and follow-up for advanced-stage lung cancer. Recently, radiological features have evolved from solely semantic to include (handcrafted and deep) radiomic features. Radiomics entails the extraction and analysis of quantitative features from medical images using mathematical and machine learning methods to explore possible ties with biology and clinical outcomes. Methods Here, we outline the latest applications of both structural and functional radiomics in detection, diagnosis, and prediction of pathology, gene mutation, treatment strategy, follow-up, treatment response evaluation, and prognosis in the field of lung cancer. Conclusion The major drawbacks of radiomics are the lack of large datasets with high-quality data, standardization of methodology, the black-box nature of deep learning, and reproducibility. The prerequisite for the clinical implementation of radiomics is that these limitations are addressed. Future directions include a safer and more efficient model-training mode, merge multi-modality images, and combined multi-discipline or multi-omics to form "Medomics."

Published

2021

11. Cycle-Consistent Generative Adversarial Network: Effect on Radiation Dose Reduction and Image Quality Improvement in Ultralow-Dose CT for Evaluation of Pulmonary Tuberculosis

Author

Yan, C.G., Yan, C.G., Lin, J., Li, H.X., Xu, J., Zhang, T.J., Chen, H., Woodruff, H.C., Wu, G.Y., Zhang, S.Q., Xu, Y.K., Lambin, P., Yan, C.G., Yan, C.G., Lin, J., Li, H.X., Xu, J., Zhang, T.J., Chen, H., Woodruff, H.C., Wu, G.Y., Zhang, S.Q., Xu, Y.K., and Lambin, P.

Abstract

Objective: To investigate the image quality of ultralow-dose CT (ULDCT) of the chest reconstructed using a cycle-consistent generative adversarial network (CycleGAN)-based deep learning method in the evaluation of pulmonary tuberculosis. Materials and Methods: Between June 2019 and November 2019, 103 patients (mean age, 40.8 +/- 13.6 years; 61 men and 42 women) with pulmonary tuberculosis were prospectively enrolled to undergo standard-dose CT (120 kVp with automated exposure control), followed immediately by ULDCT (80 kVp and 10 mAs). The images of the two successive scans were used to train the CycleGAN framework for image-to-image translation. The denoising efficacy of the CycleGAN algorithm was compared with that of hybrid and model-based iterative reconstruction. Repeated-measures analysis of variance and Wilcoxon signed-rank test were performed to compare the objective measurements and the subjective image quality scores, respectively. Results: With the optimized CycleGAN denoising model, using the ULDCT images as input, the peak signal-to-noise ratio and structural similarity index improved by 2.0 dB and 0.21, respectively. The CycleGAN-generated denoised ULDCT images typically provided satisfactory image quality for optimal visibility of anatomic structures and pathological findings, with a lower level of image noise (mean +/- standard deviation [SD], 19.5 +/- 3.0 Hounsfield unit [HU]) than that of the hybrid (66.3 +/- 10.5 HU, p < 0.001) and a similar noise level to model-based iterative reconstruction (19.6 +/- 2.6 HU, p > 0.908). The CycleGAN-generated images showed the highest contrast-to-noise ratios for the pulmonary lesions, followed by the model-based and hybrid iterative reconstruction. The mean effective radiation dose of ULDCT was 0.12 mSv with a mean 93.9% reduction compared to standard-dose CT. Conclusion: The optimized CycleGAN technique may allow the synthesis of diagnostically acceptable images from ULDCT of the chest for the evaluation

Published

2021

12. Machine learning for grading and prognosis of esophageal dysplasia using mass spectrometry and histological imaging

Author

Beuque, M., Beuque, M., Martin-Lorenzo, M., Balluff, B., Woodruff, H.C., Lucas, M., de Bruin, D.M., van Timmeren, J.E., de Boer, O.J., Heeren, R.M.A., Meijer, S.L., Lambin, P., Beuque, M., Beuque, M., Martin-Lorenzo, M., Balluff, B., Woodruff, H.C., Lucas, M., de Bruin, D.M., van Timmeren, J.E., de Boer, O.J., Heeren, R.M.A., Meijer, S.L., and Lambin, P.

Abstract

Background: Barrett's esophagus (BE) is a precursor lesion of esophageal adenocarcinoma and may progress from non-dysplastic through low-grade dysplasia (LGD) to high-grade dysplasia (HGD) and cancer. Grading BE is of crucial prognostic value and is currently based on the subjective evaluation of biopsies. This study aims to investigate the potential of machine learning (ML) using spatially resolved molecular data from mass spectrometry imaging (MSI) and histological data from microscopic hematoxylin and eosin (H&E)-stained imaging for computer-aided diagnosis and prognosis of BE. Methods: Biopsies from 57 patients were considered, divided into non-dysplastic (n = 15), LGD non-progressive (n = 14), LGD progressive (n = 14), and HGD (n = 14). MSI experiments were conducted at 50 x 50 mu m spatial resolution per pixel corresponding to a tile size of 96x96 pixels in the co-registered H&E images, making a total of 144,823 tiles for the whole dataset. Results: ML models were trained to distinguish epithelial tissue from stroma with area-under-the-curve (AUC) values of 0.89 (MSI) and 0.95 (H&E)) and dysplastic grade (AUC of 0.97 (MSI) and 0.85 (H&E)) on a tile level, and low-grade progressors from non-progressors on a patient level (accuracies of 0.72 (MSI) and 0.48 (H&E)). Conclusions: In summary, while the H&E-based classifier was best at distinguishing tissue types, the MSI-based model was more accurate at distinguishing dysplastic grades and patients at progression risk, which demonstrates the complementarity of both approaches. Data are available via ProteomeXchange with identifier PXD028949.

Published

2021

13. Reproducibility of CT-Based Hepatocellular Carcinoma Radiomic Features across Different Contrast Imaging Phases: A Proof of Concept on SORAMIC Trial Data

Author

Ibrahim, A., Ibrahim, A., Widaatalla, Y., Refaee, T., Primakov, S., Miclea, R.L., Ocal, O., Fabritius, M.P., Ingrisch, M., Ricke, J., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Seidensticker, M., Lambin, P., Ibrahim, A., Ibrahim, A., Widaatalla, Y., Refaee, T., Primakov, S., Miclea, R.L., Ocal, O., Fabritius, M.P., Ingrisch, M., Ricke, J., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Seidensticker, M., and Lambin, P.

Abstract

Simple Summary Radiomics has been reported to have potential for correlating with clinical outcomes. However, handcrafted radiomic features (HRFs)-the quantitative features extracted from medical images-are limited by their sensitivity to variations in scanning parameters. Furthermore, radiomics analyses require big data with good quality to achieve desirable performances. In this study, we investigated the reproducibility of HRFs between scans acquired with the same scanning parameters except for the imaging phase (arterial and portal venous phases) to assess the possibilities of merging scans from different phases or replacing missing scans from a phase with other phases to increase data entries. Additionally, we assessed the potential of ComBat harmonization to remove batch effects attributed to this variation. Our results show that the majority of HRFs were not reproducible between the arterial and portal venous phases before or after ComBat harmonization. We provide a guide for analyzing scans of different imaging phases. Handcrafted radiomic features (HRFs) are quantitative imaging features extracted from regions of interest on medical images which can be correlated with clinical outcomes and biologic characteristics. While HRFs have been used to train predictive and prognostic models, their reproducibility has been reported to be affected by variations in scan acquisition and reconstruction parameters, even within the same imaging vendor. In this work, we evaluated the reproducibility of HRFs across the arterial and portal venous phases of contrast-enhanced computed tomography images depicting hepatocellular carcinomas, as well as the potential of ComBat harmonization to correct for this difference. ComBat harmonization is a method based on Bayesian estimates that was developed for gene expression arrays, and has been investigated as a potential method for harmonizing HRFs. Our results show that the majority of HRFs are not reproducible between the arterial a

Published

2021

14. Reply to Orlhac, F.; Buvat, I. Comment on 'Ibrahim et al. The Effects of In-Plane Spatial Resolution on CT-Based Radiomic Features' Stability with and without ComBat Harmonization. Cancers 2021, 13, 1848'

Author

Ibrahim, A., Ibrahim, A., Refaee, T., Primakov, S., Barufaldi, B., Acciavatti, R.J., Granzier, R.W.Y., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Wildberger, J.E., Lambin, P., Maidment, A.D.A., Ibrahim, A., Ibrahim, A., Refaee, T., Primakov, S., Barufaldi, B., Acciavatti, R.J., Granzier, R.W.Y., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Wildberger, J.E., Lambin, P., and Maidment, A.D.A.

Published

2021

15. Making Radiomics More Reproducible across Scanner and Imaging Protocol Variations: A Review of Harmonization Methods

Author

Mali, S.A., Mali, S.A., Ibrahim, A., Woodruff, H.C., Andrearczyk, V., Muller, H., Primakov, S., Salahuddin, Z., Chatterjee, A., Lambin, P., Mali, S.A., Mali, S.A., Ibrahim, A., Woodruff, H.C., Andrearczyk, V., Muller, H., Primakov, S., Salahuddin, Z., Chatterjee, A., and Lambin, P.

Abstract

Radiomics converts medical images into mineable data via a high-throughput extraction of quantitative features used for clinical decision support. However, these radiomic features are susceptible to variation across scanners, acquisition protocols, and reconstruction settings. Various investigations have assessed the reproducibility and validation of radiomic features across these discrepancies. In this narrative review, we combine systematic keyword searches with prior domain knowledge to discuss various harmonization solutions to make the radiomic features more reproducible across various scanners and protocol settings. Different harmonization solutions are discussed and divided into two main categories: image domain and feature domain. The image domain category comprises methods such as the standardization of image acquisition, post-processing of raw sensor-level image data, data augmentation techniques, and style transfer. The feature domain category consists of methods such as the identification of reproducible features and normalization techniques such as statistical normalization, intensity harmonization, ComBat and its derivatives, and normalization using deep learning. We also reflect upon the importance of deep learning solutions for addressing variability across multi-centric radiomic studies especially using generative adversarial networks (GANs), neural style transfer (NST) techniques, or a combination of both. We cover a broader range of methods especially GANs and NST methods in more detail than previous reviews.

Published

2021

16. Toxicity of L19-Interleukin 2 combined with Stereotactic Body Radiation Therapy: A phase I study

Author

Limbergen Ej, H. A., Lieverse, R., Houben, R., Overhof, C., Jacobi, L., Postma, A., Zindler, J., Verhelst, F., Dubois, L., De, R. D., (0000-0001-9550-9050) Troost, E. G. C., Lambin, P., Limbergen Ej, H. A., Lieverse, R., Houben, R., Overhof, C., Jacobi, L., Postma, A., Zindler, J., Verhelst, F., Dubois, L., De, R. D., (0000-0001-9550-9050) Troost, E. G. C., and Lambin, P.

Abstract

Introduction The immunocytokine L19-IL2 delivers interleukin-2 to the tumor by exploiting the selective L19-dependent binding of extradomain B of fibronectin on tumor blood vessels. In preclinical models, L19-IL2 has been shown to enhance the local and abscopal effects of radiotherapy. The clinical safety of L19-IL2 monotherapy has been established previously. In this study, the safety and tolerability of L19-IL2 following Stereotactic Body Radiotherapy (SBRT) was assessed. Materials and methods Patients with oligometastatic solid tumors received radical SBRT to all visible metastases. Within one week following SBRT, intravenous L19-IL2 using a 3+3 dose escalation design was administered. Safety and tolerability were analyzed as the primary endpoint using the CTCAE4.03 scoring system, progression-free and overall survival as secondary endpoints. Results A total of 6 patients in two L19-IL2 dose levels were included. The 15 Mio International Units (IU) dose level was well tolerated with no dose limiting toxicity. The most frequently reported adverse events were chills, noninfectious fever, fatigue, edema, erythema, pruritus, nausea/vomiting as well as cough and dyspnea. Blood analysis revealed abnormalities in liver function tests, anemia, hypoalbuminemia, and hypokalemia. At the second dose level (i.e., 22.5 Mio IU), which is the recommended dose for L19-IL2 monotherapy, all three included patients experienced dose-limiting toxicity, but toxicities recovered without sequelae. We documented two long-term progression-free responders both having non-small cell lung cancer as primary tumor. Conclusion Based in the results of this phase I clinical trial, the recommended phase II dose for SBRT combined with L19-IL2 is 15 Mio IU. The therapeutic efficacy of this combination is currently being evaluated in the multicentric EU-funded phase II clinical trial, ImmunoSABR.

Published

2021

17. Reproducibility of CT-Based Hepatocellular Carcinoma Radiomic Features across Different Contrast Imaging Phases: A Proof of Concept on SORAMIC Trial Data

Author

Ibrahim, A., Widaatalla, Y., Refaee, T., Primakov, S., Miclea, R.L., Ocal, O., Fabritius, M.P., Ingrisch, M., Ricke, J., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Seidensticker, M., Lambin, P., Ibrahim, A., Widaatalla, Y., Refaee, T., Primakov, S., Miclea, R.L., Ocal, O., Fabritius, M.P., Ingrisch, M., Ricke, J., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Seidensticker, M., and Lambin, P.

Abstract

Simple Summary Radiomics has been reported to have potential for correlating with clinical outcomes. However, handcrafted radiomic features (HRFs)-the quantitative features extracted from medical images-are limited by their sensitivity to variations in scanning parameters. Furthermore, radiomics analyses require big data with good quality to achieve desirable performances. In this study, we investigated the reproducibility of HRFs between scans acquired with the same scanning parameters except for the imaging phase (arterial and portal venous phases) to assess the possibilities of merging scans from different phases or replacing missing scans from a phase with other phases to increase data entries. Additionally, we assessed the potential of ComBat harmonization to remove batch effects attributed to this variation. Our results show that the majority of HRFs were not reproducible between the arterial and portal venous phases before or after ComBat harmonization. We provide a guide for analyzing scans of different imaging phases. Handcrafted radiomic features (HRFs) are quantitative imaging features extracted from regions of interest on medical images which can be correlated with clinical outcomes and biologic characteristics. While HRFs have been used to train predictive and prognostic models, their reproducibility has been reported to be affected by variations in scan acquisition and reconstruction parameters, even within the same imaging vendor. In this work, we evaluated the reproducibility of HRFs across the arterial and portal venous phases of contrast-enhanced computed tomography images depicting hepatocellular carcinomas, as well as the potential of ComBat harmonization to correct for this difference. ComBat harmonization is a method based on Bayesian estimates that was developed for gene expression arrays, and has been investigated as a potential method for harmonizing HRFs. Our results show that the majority of HRFs are not reproducible between the arterial a

Published

2021

18. Making Radiomics More Reproducible across Scanner and Imaging Protocol Variations: A Review of Harmonization Methods

Author

Mali, S.A., Ibrahim, A., Woodruff, H.C., Andrearczyk, V., Muller, H., Primakov, S., Salahuddin, Z., Chatterjee, A., Lambin, P., Mali, S.A., Ibrahim, A., Woodruff, H.C., Andrearczyk, V., Muller, H., Primakov, S., Salahuddin, Z., Chatterjee, A., and Lambin, P.

Abstract

Radiomics converts medical images into mineable data via a high-throughput extraction of quantitative features used for clinical decision support. However, these radiomic features are susceptible to variation across scanners, acquisition protocols, and reconstruction settings. Various investigations have assessed the reproducibility and validation of radiomic features across these discrepancies. In this narrative review, we combine systematic keyword searches with prior domain knowledge to discuss various harmonization solutions to make the radiomic features more reproducible across various scanners and protocol settings. Different harmonization solutions are discussed and divided into two main categories: image domain and feature domain. The image domain category comprises methods such as the standardization of image acquisition, post-processing of raw sensor-level image data, data augmentation techniques, and style transfer. The feature domain category consists of methods such as the identification of reproducible features and normalization techniques such as statistical normalization, intensity harmonization, ComBat and its derivatives, and normalization using deep learning. We also reflect upon the importance of deep learning solutions for addressing variability across multi-centric radiomic studies especially using generative adversarial networks (GANs), neural style transfer (NST) techniques, or a combination of both. We cover a broader range of methods especially GANs and NST methods in more detail than previous reviews.

Published

2021

19. MRI-based delta-radiomics predicts pathologic complete response in high-grade soft-tissue sarcoma patients treated with neoadjuvant therapy

Author

Peeken, J.C., Asadpour, R., Specht, K., Chen, E.Y., Klymenko, O., Akinkuoroye, V., Hippe, D.S., Spraker, M.B., Schaub, S.K., Dapper, H., Knebel, C., Mayr, N.A., Gersing, A.S., Woodruff, H.C., Lambin, P., Nyflot, M.J., Combs, S.E., Peeken, J.C., Asadpour, R., Specht, K., Chen, E.Y., Klymenko, O., Akinkuoroye, V., Hippe, D.S., Spraker, M.B., Schaub, S.K., Dapper, H., Knebel, C., Mayr, N.A., Gersing, A.S., Woodruff, H.C., Lambin, P., Nyflot, M.J., and Combs, S.E.

Abstract

Purpose: In high-grade soft-tissue sarcomas (STS) the standard of care encompasses multimodal therapy regimens. While there is a growing body of evidence for prognostic pretreatment radiomic models, we hypothesized that temporal changes in radiomic features following neoadjuvant treatment ("delta-radio mics") may be able to predict the pathological complete response (pCR). Methods: MRI scans (T1-weighted with fat-saturation and contrast-enhancement (T1FSGd) and T2 weighted with fat-saturation (T2FS)) of patients with STS of the extremities and trunk treated with neoadjuvant therapy were gathered from two independent institutions (training: 103, external testing: 53 patients). pCR was defined as <5% viable cells. After segmentation and preprocessing, 105 radiomic features were extracted. Delta-radiomic features were calculated by subtraction of features derived from MRI scans obtained before and after neoadjuvant therapy. After feature reduction, machine learning modeling was performed in 100 iterations of 3-fold nested cross-validation. Delta-radiomic models were compared with single timepoint models in the testing cohort. Results: The combined delta-radiomic models achieved the best area under the receiver operating characteristic curve (AUC) of 0.75. Pre-therapeutic tumor volume was the best conventional predictor (AUC 0.70). The T2FS-based delta-radiomic model had the most balanced classification performance with a balanced accuracy of 0.69. Delta-radiomic models achieved better reproducibility than single timepoint radiomic models, RECIST or the peri-therapeutic volume change. Delta-radiomic models were significantly associated with survival in multivariate Cox regression. Conclusion: This exploratory analysis demonstrated that MRI-based delta-radiomics improves prediction of pCR over tumor volume and RECIST. Delta-radiomics may one day function as a biomarker for personalized treatment adaptations. (c) 2021 Elsevier B.V. All rights reserved. Radiotherapy and

Published

2021

20. Machine learning for grading and prognosis of esophageal dysplasia using mass spectrometry and histological imaging

Author

Beuque, M., Martin-Lorenzo, M., Balluff, B., Woodruff, H.C., Lucas, M., de Bruin, D.M., van Timmeren, J.E., de Boer, O.J., Heeren, R.M.A., Meijer, S.L., Lambin, P., Beuque, M., Martin-Lorenzo, M., Balluff, B., Woodruff, H.C., Lucas, M., de Bruin, D.M., van Timmeren, J.E., de Boer, O.J., Heeren, R.M.A., Meijer, S.L., and Lambin, P.

Abstract

Background: Barrett's esophagus (BE) is a precursor lesion of esophageal adenocarcinoma and may progress from non-dysplastic through low-grade dysplasia (LGD) to high-grade dysplasia (HGD) and cancer. Grading BE is of crucial prognostic value and is currently based on the subjective evaluation of biopsies. This study aims to investigate the potential of machine learning (ML) using spatially resolved molecular data from mass spectrometry imaging (MSI) and histological data from microscopic hematoxylin and eosin (H&E)-stained imaging for computer-aided diagnosis and prognosis of BE. Methods: Biopsies from 57 patients were considered, divided into non-dysplastic (n = 15), LGD non-progressive (n = 14), LGD progressive (n = 14), and HGD (n = 14). MSI experiments were conducted at 50 x 50 mu m spatial resolution per pixel corresponding to a tile size of 96x96 pixels in the co-registered H&E images, making a total of 144,823 tiles for the whole dataset. Results: ML models were trained to distinguish epithelial tissue from stroma with area-under-the-curve (AUC) values of 0.89 (MSI) and 0.95 (H&E)) and dysplastic grade (AUC of 0.97 (MSI) and 0.85 (H&E)) on a tile level, and low-grade progressors from non-progressors on a patient level (accuracies of 0.72 (MSI) and 0.48 (H&E)). Conclusions: In summary, while the H&E-based classifier was best at distinguishing tissue types, the MSI-based model was more accurate at distinguishing dysplastic grades and patients at progression risk, which demonstrates the complementarity of both approaches. Data are available via ProteomeXchange with identifier PXD028949.

Published

2021

21. A Prospectively Validated Prognostic Model for Patients with Locally Advanced Squamous Cell Carcinoma of the Head and Neck Based on Radiomics of Computed Tomography Images

Author

Keek, S.A., Wesseling, F.W.R., Woodruff, H.C., van Timmeren, J.E., Nauta, I.H., Hoffmann, T.K., Cavalieri, S., Calareso, G., Primakov, S., Leijenaar, R.T.H., Licitra, L., Ravanelli, M., Scheckenbach, K., Poli, T., Lanfranco, D., Vergeer, M.R., Leemans, C.R., Brakenhoff, R.H., Hoebers, F.J.P., Lambin, P., Keek, S.A., Wesseling, F.W.R., Woodruff, H.C., van Timmeren, J.E., Nauta, I.H., Hoffmann, T.K., Cavalieri, S., Calareso, G., Primakov, S., Leijenaar, R.T.H., Licitra, L., Ravanelli, M., Scheckenbach, K., Poli, T., Lanfranco, D., Vergeer, M.R., Leemans, C.R., Brakenhoff, R.H., Hoebers, F.J.P., and Lambin, P.

Abstract

Simple Summary Patients that suffer from advanced head and neck cancer have a low average survival chance. Improving prognosis could improve this survival rate as it may help in clinical decision making. Radiomics features calculated from images of the tumour describe tumour size, shape, and pattern. These characteristics may be linked to patient survival, which is investigated in this paper. We combined radiomics features with other biomarkers of survival of 809 patients to make a prognosis before treatment. We then compared the predicted prognosis with the actual outcome to see how well our model performs. Our model was able to make three distinct risk groups of low-, medium-, and high-survival patients. With these findings, doctors may make a better judgement of treatment and follow-up per patient, which might improve clinical outcomes. Background: Locoregionally advanced head and neck squamous cell carcinoma (HNSCC) patients have high relapse and mortality rates. Imaging-based decision support may improve outcomes by optimising personalised treatment, and support patient risk stratification. We propose a multifactorial prognostic model including radiomics features to improve risk stratification for advanced HNSCC, compared to TNM eighth edition, the gold standard. Patient and methods: Data of 666 retrospective- and 143 prospective-stage III-IVA/B HNSCC patients were collected. A multivariable Cox proportional-hazards model was trained to predict overall survival (OS) using diagnostic CT-based radiomics features extracted from the primary tumour. Separate analyses were performed using TNM8, tumour volume, clinical and biological variables, and combinations thereof with radiomics features. Patient risk stratification in three groups was assessed through Kaplan-Meier (KM) curves. A log-rank test was performed for significance (p-value < 0.05). The prognostic accuracy was reported through the concordance index (CI). Results: A model combining an 11-feature rad

Published

2021

22. Structural and functional radiomics for lung cancer

Author

Wu, G.Y., Jochems, A., Refaee, T., Ibrahim, A., Yan, C.G., Sanduleanu, S., Woodruff, H.C., Lambin, P., Wu, G.Y., Jochems, A., Refaee, T., Ibrahim, A., Yan, C.G., Sanduleanu, S., Woodruff, H.C., and Lambin, P.

Abstract

Introduction Lung cancer ranks second in new cancer cases and first in cancer-related deaths worldwide. Precision medicine is working on altering treatment approaches and improving outcomes in this patient population. Radiological images are a powerful non-invasive tool in the screening and diagnosis of early-stage lung cancer, treatment strategy support, prognosis assessment, and follow-up for advanced-stage lung cancer. Recently, radiological features have evolved from solely semantic to include (handcrafted and deep) radiomic features. Radiomics entails the extraction and analysis of quantitative features from medical images using mathematical and machine learning methods to explore possible ties with biology and clinical outcomes. Methods Here, we outline the latest applications of both structural and functional radiomics in detection, diagnosis, and prediction of pathology, gene mutation, treatment strategy, follow-up, treatment response evaluation, and prognosis in the field of lung cancer. Conclusion The major drawbacks of radiomics are the lack of large datasets with high-quality data, standardization of methodology, the black-box nature of deep learning, and reproducibility. The prerequisite for the clinical implementation of radiomics is that these limitations are addressed. Future directions include a safer and more efficient model-training mode, merge multi-modality images, and combined multi-discipline or multi-omics to form "Medomics."

Published

2021

23. Reply to Orlhac, F.; Buvat, I. Comment on 'Ibrahim et al. The Effects of In-Plane Spatial Resolution on CT-Based Radiomic Features' Stability with and without ComBat Harmonization. Cancers 2021, 13, 1848'

Author

Ibrahim, A., Refaee, T., Primakov, S., Barufaldi, B., Acciavatti, R.J., Granzier, R.W.Y., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Wildberger, J.E., Lambin, P., Maidment, A.D.A., Ibrahim, A., Refaee, T., Primakov, S., Barufaldi, B., Acciavatti, R.J., Granzier, R.W.Y., Hustinx, R., Mottaghy, F.M., Woodruff, H.C., Wildberger, J.E., Lambin, P., and Maidment, A.D.A.

Abstract

We would like to thank Orlhac and Buvat [...]

Published

2021

24. MRI-Based Radiomics Analysis for the Pretreatment Prediction of Pathologic Complete Tumor Response to Neoadjuvant Systemic Therapy in Breast Cancer Patients: A Multicenter Study

Author

Granzier, R.W.Y., Ibrahim, A., Primakov, S.P., Samiei, S., van Nijnatten, T.J.A., de Boer, M., Heuts, E.M., Hulsmans, F.J., Chatterjee, A., Lambin, P., Lobbes, M.B.I., Woodruff, H.C., Smidt, M.L., Granzier, R.W.Y., Ibrahim, A., Primakov, S.P., Samiei, S., van Nijnatten, T.J.A., de Boer, M., Heuts, E.M., Hulsmans, F.J., Chatterjee, A., Lambin, P., Lobbes, M.B.I., Woodruff, H.C., and Smidt, M.L.

Abstract

Simple SummaryThe prediction of pathologic complete response (pCR) to neo-adjuvant systemic therapy (NST) based on radiological assessment of pretreatment MRI exams in breast cancer patients is not possible to date. In this study, we investigated the value of pretreatment MRI-based radiomics analysis for the prediction of pCR to NST. Radiomics, clinical, and combined models were developed and validated based on MRI exams containing 320 tumors collected from two hospitals. The clinical models significantly outperformed the radiomics models for the prediction of pCR to NST and were of similar or better performance than the combined models. This indicates poor performance of the radiomics features and that in these scenarios the radiomic features did not have an added value for the clinical models developed. Due to previous and current work, we tentatively attribute the lack of significant improvement in clinical models following the addition of radiomics features to the effects of variations in acquisition and reconstruction parameters. The lack of reproducibility data meant this effect could not be analyzed. These results indicate the need for reproducibility studies to preselect reproducible features in order to properly assess the potential of radiomics.This retrospective study investigated the value of pretreatment contrast-enhanced Magnetic Resonance Imaging (MRI)-based radiomics for the prediction of pathologic complete tumor response to neoadjuvant systemic therapy in breast cancer patients. A total of 292 breast cancer patients, with 320 tumors, who were treated with neo-adjuvant systemic therapy and underwent a pretreatment MRI exam were enrolled. As the data were collected in two different hospitals with five different MRI scanners and varying acquisition protocols, three different strategies to split training and validation datasets were used. Radiomics, clinical, and combined models were developed using random forest classifiers in each strategy. The analy

Published

2021

25. Exploratory Radiomic Analysis of Conventional vs. Quantitative Brain MRI: Toward Automatic Diagnosis of Early Multiple Sclerosis

Author

Lavrova, E., Lommers, E., Woodruff, H.C., Chatterjee, A., Maquet, P., Salmon, E., Lambin, P., Phillips, C., Lavrova, E., Lommers, E., Woodruff, H.C., Chatterjee, A., Maquet, P., Salmon, E., Lambin, P., and Phillips, C.

Abstract

Conventional magnetic resonance imaging (cMRI) is poorly sensitive to pathological changes related to multiple sclerosis (MS) in normal-appearing white matter (NAWM) and gray matter (GM), with the added difficulty of not being very reproducible. Quantitative MRI (qMRI), on the other hand, attempts to represent the physical properties of tissues, making it an ideal candidate for quantitative medical image analysis or radiomics. We therefore hypothesized that qMRI-based radiomic features have added diagnostic value in MS compared to cMRI. This study investigated the ability of cMRI (T1w) and qMRI features extracted from white matter (WM), NAWM, and GM to distinguish between MS patients (MSP) and healthy control subjects (HCS). We developed exploratory radiomic classification models on a dataset comprising 36 MSP and 36 HCS recruited in CHU Liege, Belgium, acquired with cMRI and qMRI. For each image type and region of interest, qMRI radiomic models for MS diagnosis were developed on a training subset and validated on a testing subset. Radiomic models based on cMRI were developed on the entire training dataset and externally validated on open-source datasets with 167 HCS and 10 MSP. Ranked by region of interest, the best diagnostic performance was achieved in the whole WM. Here the model based on magnetization transfer imaging (a type of qMRI) features yielded a median area under the receiver operating characteristic curve (AUC) of 1.00 in the testing sub-cohort. Ranked by image type, the best performance was achieved by the magnetization transfer models, with median AUCs of 0.79 (0.69-0.90, 90% CI) in NAWM and 0.81 (0.71-0.90) in GM. The external validation of the T1w models yielded an AUC of 0.78 (0.47-1.00) in the whole WM, demonstrating a large 95% CI and a low sensitivity of 0.30 (0.10-0.70). This exploratory study indicates that qMRI radiomics could provide efficient diagnostic information using NAWM and GM analysis in MSP. T1w radiomics could be useful for a fast

Published

2021

26. Cycle-Consistent Generative Adversarial Network: Effect on Radiation Dose Reduction and Image Quality Improvement in Ultralow-Dose CT for Evaluation of Pulmonary Tuberculosis

Author

Yan, C.G., Lin, J., Li, H.X., Xu, J., Zhang, T.J., Chen, H., Woodruff, H.C., Wu, G.Y., Zhang, S.Q., Xu, Y.K., Lambin, P., Yan, C.G., Lin, J., Li, H.X., Xu, J., Zhang, T.J., Chen, H., Woodruff, H.C., Wu, G.Y., Zhang, S.Q., Xu, Y.K., and Lambin, P.

Abstract

Objective: To investigate the image quality of ultralow-dose CT (ULDCT) of the chest reconstructed using a cycle-consistent generative adversarial network (CycleGAN)-based deep learning method in the evaluation of pulmonary tuberculosis. Materials and Methods: Between June 2019 and November 2019, 103 patients (mean age, 40.8 +/- 13.6 years; 61 men and 42 women) with pulmonary tuberculosis were prospectively enrolled to undergo standard-dose CT (120 kVp with automated exposure control), followed immediately by ULDCT (80 kVp and 10 mAs). The images of the two successive scans were used to train the CycleGAN framework for image-to-image translation. The denoising efficacy of the CycleGAN algorithm was compared with that of hybrid and model-based iterative reconstruction. Repeated-measures analysis of variance and Wilcoxon signed-rank test were performed to compare the objective measurements and the subjective image quality scores, respectively. Results: With the optimized CycleGAN denoising model, using the ULDCT images as input, the peak signal-to-noise ratio and structural similarity index improved by 2.0 dB and 0.21, respectively. The CycleGAN-generated denoised ULDCT images typically provided satisfactory image quality for optimal visibility of anatomic structures and pathological findings, with a lower level of image noise (mean +/- standard deviation [SD], 19.5 +/- 3.0 Hounsfield unit [HU]) than that of the hybrid (66.3 +/- 10.5 HU, p < 0.001) and a similar noise level to model-based iterative reconstruction (19.6 +/- 2.6 HU, p > 0.908). The CycleGAN-generated images showed the highest contrast-to-noise ratios for the pulmonary lesions, followed by the model-based and hybrid iterative reconstruction. The mean effective radiation dose of ULDCT was 0.12 mSv with a mean 93.9% reduction compared to standard-dose CT. Conclusion: The optimized CycleGAN technique may allow the synthesis of diagnostically acceptable images from ULDCT of the chest for the evaluation

Published

2021

27. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., Lambin, P., Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., and Lambin, P.

Abstract

Contains fulltext : 220477.pdf (publisher's version ) (Open Access), BACKGROUND: About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). METHODS: This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised to the experimental-arm (E-arm) or the control-arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). The accrual period will be 2.5-years, starting after the first centre is initiated and active. Primary endpoint is PFS at 1.5-years based on blinded radiological review, and secondary endpoints are overall survival, toxicity, quality of life and abscopal response. Associative biomarker studies, immune monitoring, CT-based radiomics, stool collection, iRECIST and tumour growth rate will be performed. DISCUSSION: The combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd li

Published

2020

28. Exploring imaging features of molecular subtypes of large cell neuroendocrine carcinoma (LCNEC)

Author

Hermans, B.C.M. (B. C.M.), Sanduleanu, S. (S.), Derks, J.L. (Jules L.), Woodruff, H. (H.), Hillen, L.M. (L. M.), Casale, R. (R.), Hoesein, F.A.M. (Firdaus A Mohamed), de Jong, E. (E.), Berge, D.M.H.J.T. (D.M.H.J. ten), Speel, E.J. (Ernst-Jan), Lambin, P. (Philippe), Gietema, H.A. (Hester), Dingemans, A.-M.C. (A-M.C.), Hermans, B.C.M. (B. C.M.), Sanduleanu, S. (S.), Derks, J.L. (Jules L.), Woodruff, H. (H.), Hillen, L.M. (L. M.), Casale, R. (R.), Hoesein, F.A.M. (Firdaus A Mohamed), de Jong, E. (E.), Berge, D.M.H.J.T. (D.M.H.J. ten), Speel, E.J. (Ernst-Jan), Lambin, P. (Philippe), Gietema, H.A. (Hester), and Dingemans, A.-M.C. (A-M.C.)

Abstract

Objectives: Radiological characteristics and radiomics signatures can aid in differentiation between small cell lung carcinoma (SCLC) and non-small cell lung carcinoma (NSCLC). We investigated whether molecular subtypes of large cell neuroendocrine carcinoma (LCNEC), i.e. SCLC-like (with pRb loss) vs. NSCLC-like (with pRb expression), can be distinguished by imaging based on (1) imaging interpretation, (2) semantic features, and/or (3) a radiomics signature, designed to differentiate between SCLC and NSCLC. Materials and Methods: Pulmonary oncologists and chest radiologists assessed chest CT-scans of 44 LCNEC patients for ‘small cell-like’ or ‘non-small cell-like’ appearance. The radiologists also scored semantic features of 50 LCNEC scans. Finally, a radiomics signature was trained on a dataset containing 48 SCLC and 76 NSCLC scans and validated on an external set of 58 SCLC and 40 NSCLC scans. This signature was applied on scans of 28 SCLC-like and 8 NSCLC-like LCNEC patients. Results: Pulmonary oncologists and radiologists were unable to differentiate between molecular subtypes of LCNEC and no significant differences in semantic features were found. The area under the receiver operating characteristics curve of the radiomics signature in the validation set (SCLC vs. NSCLC) was 0.84 (95% confidence interval (CI) 0.77-0.92) and 0.58 (95% CI 0.29-0.86) in the LCNEC dataset (SCLC-like vs. NSCLC-like). Conclusion: LCNEC appears to have radiological characteristics of both SCLC and NSCLC, irrespective of pRb loss, compatible with the SCLC-like subtype. Imaging interpretation, semantic features and our radiomics signature designed to differentiate between SCLC and NSCLC were unable to separate molecular LCNEC subtypes, which underscores that LCNEC is a unique disease.

Published

2020

29. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R.I.Y. (Relinde I Y), Van Limbergen, E.J. (Evert J.), Oberije, C. (Cary), Troost, E.G.C. (Esther G C), Hadrup, S.R. (Sine R.), Dingemans, A.-M.C. (Anne-Marie C), Hendriks, L.E.L. (Lizza E L), Eckert, F. (Franziska), Hiley, C. (Crispin), Dooms, C. (Christophe), Lievens, Y. (Yolande), de Jong, M.C. (Monique C.), Bussink, J. (Johan), Geets, X. (Xavier), Valentini, V. (Vincenzo), Elia, G. (Giuliano), Neri, D. (Dario), Billiet, C. (Charlotte), Abdollahi, A. (Amir), Pasquier, D. (David), Boisselier, P. (Pierre), Yaromina, A. (Ala), Ruysscher, D.K.M. (Dirk) de, Dubois, L., Lambin, P. (Philippe), Lieverse, R.I.Y. (Relinde I Y), Van Limbergen, E.J. (Evert J.), Oberije, C. (Cary), Troost, E.G.C. (Esther G C), Hadrup, S.R. (Sine R.), Dingemans, A.-M.C. (Anne-Marie C), Hendriks, L.E.L. (Lizza E L), Eckert, F. (Franziska), Hiley, C. (Crispin), Dooms, C. (Christophe), Lievens, Y. (Yolande), de Jong, M.C. (Monique C.), Bussink, J. (Johan), Geets, X. (Xavier), Valentini, V. (Vincenzo), Elia, G. (Giuliano), Neri, D. (Dario), Billiet, C. (Charlotte), Abdollahi, A. (Amir), Pasquier, D. (David), Boisselier, P. (Pierre), Yaromina, A. (Ala), Ruysscher, D.K.M. (Dirk) de, Dubois, L., and Lambin, P. (Philippe)

Abstract

BACKGROUND: About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). METHODS: This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised

Published

2020

30. Nitroglycerin as a radiosensitizer in non-small cell lung cancer: Results of a prospective imaging-based phase II trial

Author

Reymen, B. (Bart), van Gisbergen, M.W., Even, A.J.G. (Aniek J.G.), Zegers, C.M.L. (Catharina M.L.), Das, M. (Marco), Vegt, E. (Erik), Wildberger, J.E. (Joachim), Mottaghy, F.M. (Felix M.), Yaromina, A. (Ala), Dubois, L.J. (Ludwig J.), van Elmpt, W. (Wouter), Ruysscher, D.K.M. (Dirk) de, Lambin, P. (Philippe), Reymen, B. (Bart), van Gisbergen, M.W., Even, A.J.G. (Aniek J.G.), Zegers, C.M.L. (Catharina M.L.), Das, M. (Marco), Vegt, E. (Erik), Wildberger, J.E. (Joachim), Mottaghy, F.M. (Felix M.), Yaromina, A. (Ala), Dubois, L.J. (Ludwig J.), van Elmpt, W. (Wouter), Ruysscher, D.K.M. (Dirk) de, and Lambin, P. (Philippe)

Abstract

Background: Nitroglycerin is proposed as an agent to reduce tumour hypoxia by improving tumour perfusion. We investigated the potenti

Published

2020

31. Exploring imaging features of molecular subtypes of large cell neuroendocrine carcinoma (LCNEC)

Author

Hermans, B. C. M., Hermans, B. C. M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., ten Berge, D. M. H. J., Speel, E. J. M., Lambin, P., Gietema, H. A., Dingemans, A-M C., Hermans, B. C. M., Hermans, B. C. M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., ten Berge, D. M. H. J., Speel, E. J. M., Lambin, P., Gietema, H. A., and Dingemans, A-M C.

Abstract

Objectives: Radiological characteristics and radiomics signatures can aid in differentiation between small cell lung carcinoma (SCLC) and non-small cell lung carcinoma (NSCLC). We investigated whether molecular subtypes of large cell neuroendocrine carcinoma (LCNEC), i.e. SCLC-like (with pRb loss) vs. NSCLC-like (with pRb expres-sion), can be distinguished by imaging based on (1) imaging interpretation, (2) semantic features, and/or (3) a radiomics signature, designed to differentiate between SCLC and NSCLC.Materials and Methods: Pulmonary oncologists and chest radiologists assessed chest CT-scans of 44 LCNEC patients for 'small cell-like' or Mon-small cell-like' appearance. The radiologists also scored semantic features of 50 LCNEC scans. Finally, a radiomics signature was trained on a dataset containing 48 SCLC and 76 NSCLC scans and validated on an external set of 58 SCLC and 40 NSCLC scans. This signature was applied on scans of 28 SCLC-like and 8 NSCLC-like LCNEC patients.Results: Pulmonary oncologists and radiologists were unable to differentiate between molecular subtypes of LCNEC and no significant differences in semantic features were found. The area under the receiver operating characteristics curve of the radiomics signature in the validation set (SCLC vs. NSCLC) was 0.84 (95% confidence interval (CI) 0.77-0.92) and 0.58 (95% CI 0.29-0.86) in the LCNEC dataset (SCLC-like vs. NSCLC-like).Conclusion: LCNEC appears to have radiological characteristics of both SCLC and NSCLC, irrespective of pRb loss, compatible with the SCLC-like subtype. Imaging interpretation, semantic features and our radiomics signature designed to differentiate between SCLC and NSCLC were unable to separate molecular LCNEC subtypes, which underscores that LCNEC is a unique disease.

Published

2020

32. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., Lambin, P., Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., and Lambin, P.

Abstract

Contains fulltext : 220477.pdf (publisher's version ) (Open Access), BACKGROUND: About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). METHODS: This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised to the experimental-arm (E-arm) or the control-arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). The accrual period will be 2.5-years, starting after the first centre is initiated and active. Primary endpoint is PFS at 1.5-years based on blinded radiological review, and secondary endpoints are overall survival, toxicity, quality of life and abscopal response. Associative biomarker studies, immune monitoring, CT-based radiomics, stool collection, iRECIST and tumour growth rate will be performed. DISCUSSION: The combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd li

Published

2020

33. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., Lambin, P., Lieverse, R.I.Y., Limbergen, E.J. Van, Oberije, C.J.G., Troost, E.G.C., Hadrup, S.R., Dingemans, A.C., Hendriks, L.E., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., Jong, M.C. de, Bussink, J., Geets, X., Valentini, V., Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., Ruysscher, D. de, Dubois, L.J., and Lambin, P.

Abstract

Contains fulltext : 220477.pdf (publisher's version ) (Open Access), BACKGROUND: About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). METHODS: This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised to the experimental-arm (E-arm) or the control-arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). The accrual period will be 2.5-years, starting after the first centre is initiated and active. Primary endpoint is PFS at 1.5-years based on blinded radiological review, and secondary endpoints are overall survival, toxicity, quality of life and abscopal response. Associative biomarker studies, immune monitoring, CT-based radiomics, stool collection, iRECIST and tumour growth rate will be performed. DISCUSSION: The combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd li

Published

2020

34. The Image Biomarker Standardization Initiative: standardized quantitative radiomics for highthroughput image-based phenotyping

Author

Zwanenburg, A., Vallières, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, L., Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M.-C., Dinapoli, N., Viet Dinh, C., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, R., Gillies, R. J., Goh, V., Guckenberger, M., Götz, M., Min Ha, S., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, J., Lippert, F., Losnegård, A., Maier-Hein, K. H., Morin, O., Müller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Musib Siddique, M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., (0000-0001-9550-9050) Troost, E. G. C., Upadhaya, T., Valentini, V., V. Van Dijk, L., Griethuysen, J., Velden, F. H. P., Whybra, P., (0000-0003-4261-4214) Richter, C., Löck, S., Zwanenburg, A., Vallières, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, L., Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M.-C., Dinapoli, N., Viet Dinh, C., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, R., Gillies, R. J., Goh, V., Guckenberger, M., Götz, M., Min Ha, S., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, J., Lippert, F., Losnegård, A., Maier-Hein, K. H., Morin, O., Müller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Musib Siddique, M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., (0000-0001-9550-9050) Troost, E. G. C., Upadhaya, T., Valentini, V., V. Van Dijk, L., Griethuysen, J., Velden, F. H. P., Whybra, P., (0000-0003-4261-4214) Richter, C., and Löck, S.

Abstract

Background: Radiomic features may quantify characteristics present in medical imaging. However, the lack of standardized definitions and validated reference values have hampered clinical usage. Purpose: To standardize a set of 174 radiomic features. Materials and Methods: Radiomic features were assessed in three phases. In phase I, 487 features were derived from the basic set of 174 features. Twenty-five research teams with unique radiomics software implementations computed feature values directly from a digital phantom, without any additional image processing. In phase II, fifteen teams computed values for 1347 derived features using a CT image of a patient with lung cancer and predefined image processing configurations. In both phases, consensus among the teams on the validity of tentative reference values was measured through the frequency of the modal value: <3 matches: weak; 3-5: moderate; 6-9: strong; ≥10 very strong. In the final phase (III), a public dataset of multi-modality imaging (CT, 18F-FDG-PET and T1-weighted MR) from 51 patients with soft-tissue sarcoma was used to prospectively assess reproducibility of standardized features.. Results: Consensus on reference values was initially weak for 232/302 (76.8%; phase I) and 703/1075 (65.4%; phase II) features. At the final iteration, weak consensus remained for only 2/487 (0.4%; phase I) and 19/1347 (1.4%; phase II) features, and strong or better consensus was achieved for 463/487 (95.1%; phase I) and 1220/1347 (90.6%; phase II). Overall, 169/174 features were standardized in the first two phases. In the final validation phase (III), almost all standardized features could be excellently reproduced: CT:166/169 features; PET:164/169 and MRI: 164/169. Conclusion: A set of 169 radiomics features was standardized, which enables verification and calibration of different radiomics software.

Published

2020

35. Stereotactic ablative body radiotherapy (SABR) combined with Immunotherapy (L19-IL2) in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R., Van, L. E., Oberije, C., (0000-0001-9550-9050) Troost, E. G. C., Hadrup, S., Dingemans, A., Hendriks, L., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., De, J. M., Bussink, J., Geets, X., Valentini, V., Elia, G., Nerio, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., De, R. D., Dubois, L., Lambin, P., Lieverse, R., Van, L. E., Oberije, C., (0000-0001-9550-9050) Troost, E. G. C., Hadrup, S., Dingemans, A., Hendriks, L., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., De, J. M., Bussink, J., Geets, X., Valentini, V., Elia, G., Nerio, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., De, R. D., Dubois, L., and Lambin, P.

Abstract

About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit, and new treatment strategies are therefore still needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-EDB scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). Within this phase II ImmunoSABR trial, the combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd line treatment in stage IV NSCLC patients. This bi-modal and triple treatment approach is based on the direct cytotoxic effect of radiotherapy, the tumour selective immunocytokine L19-IL2, the abscopal effect observed distant from the irradiated metastatic site(s), and the memory effect. This investigator initiated, multicentric, randomised controlled open-label phase II clinical trial (NCT03705403) will test the hypothesis that the combination of SABR and L19-IL2 increases the progression free survival (PFS) in patients with limited metastatic NSCLC. Patients will be stratified according to their metastatic load (oligo-metastatic: up to 5, or poly-metastatic: 6 to 10 metastases). Patients will be randomised by minimisation to the experimental (E-arm) or the control arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of at least one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). ImmunoSABR consists of 14 participating centres located i

Published

2020

36. The Image Biomarker Standardization Initiative: standardized quantitative radiomics for highthroughput image-based phenotyping

Author

Zwanenburg, A., Vallières, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, L., Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M.-C., Dinapoli, N., Viet Dinh, C., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, R., Gillies, R. J., Goh, V., Guckenberger, M., Götz, M., Min Ha, S., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, J., Lippert, F., Losnegård, A., Maier-Hein, K. H., Morin, O., Müller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Musib Siddique, M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., (0000-0001-9550-9050) Troost, E. G. C., Upadhaya, T., Valentini, V., V. Van Dijk, L., Griethuysen, J., Velden, F. H. P., Whybra, P., (0000-0003-4261-4214) Richter, C., Löck, S., Zwanenburg, A., Vallières, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, L., Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M.-C., Dinapoli, N., Viet Dinh, C., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, R., Gillies, R. J., Goh, V., Guckenberger, M., Götz, M., Min Ha, S., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, J., Lippert, F., Losnegård, A., Maier-Hein, K. H., Morin, O., Müller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Musib Siddique, M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., (0000-0001-9550-9050) Troost, E. G. C., Upadhaya, T., Valentini, V., V. Van Dijk, L., Griethuysen, J., Velden, F. H. P., Whybra, P., (0000-0003-4261-4214) Richter, C., and Löck, S.

Abstract

Background: Radiomic features may quantify characteristics present in medical imaging. However, the lack of standardized definitions and validated reference values have hampered clinical usage. Purpose: To standardize a set of 174 radiomic features. Materials and Methods: Radiomic features were assessed in three phases. In phase I, 487 features were derived from the basic set of 174 features. Twenty-five research teams with unique radiomics software implementations computed feature values directly from a digital phantom, without any additional image processing. In phase II, fifteen teams computed values for 1347 derived features using a CT image of a patient with lung cancer and predefined image processing configurations. In both phases, consensus among the teams on the validity of tentative reference values was measured through the frequency of the modal value: <3 matches: weak; 3-5: moderate; 6-9: strong; ≥10 very strong. In the final phase (III), a public dataset of multi-modality imaging (CT, 18F-FDG-PET and T1-weighted MR) from 51 patients with soft-tissue sarcoma was used to prospectively assess reproducibility of standardized features.. Results: Consensus on reference values was initially weak for 232/302 (76.8%; phase I) and 703/1075 (65.4%; phase II) features. At the final iteration, weak consensus remained for only 2/487 (0.4%; phase I) and 19/1347 (1.4%; phase II) features, and strong or better consensus was achieved for 463/487 (95.1%; phase I) and 1220/1347 (90.6%; phase II). Overall, 169/174 features were standardized in the first two phases. In the final validation phase (III), almost all standardized features could be excellently reproduced: CT:166/169 features; PET:164/169 and MRI: 164/169. Conclusion: A set of 169 radiomics features was standardized, which enables verification and calibration of different radiomics software.

Published

2020

37. Exploring imaging features of molecular subtypes of large cell neuroendocrine carcinoma (LCNEC)

Author

Hermans, B. C. M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., ten Berge, D. M. H. J., Speel, E. J. M., Lambin, P., Gietema, H. A., Dingemans, A-M C., Hermans, B. C. M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., ten Berge, D. M. H. J., Speel, E. J. M., Lambin, P., Gietema, H. A., and Dingemans, A-M C.

Abstract

Objectives: Radiological characteristics and radiomics signatures can aid in differentiation between small cell lung carcinoma (SCLC) and non-small cell lung carcinoma (NSCLC). We investigated whether molecular subtypes of large cell neuroendocrine carcinoma (LCNEC), i.e. SCLC-like (with pRb loss) vs. NSCLC-like (with pRb expres-sion), can be distinguished by imaging based on (1) imaging interpretation, (2) semantic features, and/or (3) a radiomics signature, designed to differentiate between SCLC and NSCLC.Materials and Methods: Pulmonary oncologists and chest radiologists assessed chest CT-scans of 44 LCNEC patients for 'small cell-like' or Mon-small cell-like' appearance. The radiologists also scored semantic features of 50 LCNEC scans. Finally, a radiomics signature was trained on a dataset containing 48 SCLC and 76 NSCLC scans and validated on an external set of 58 SCLC and 40 NSCLC scans. This signature was applied on scans of 28 SCLC-like and 8 NSCLC-like LCNEC patients.Results: Pulmonary oncologists and radiologists were unable to differentiate between molecular subtypes of LCNEC and no significant differences in semantic features were found. The area under the receiver operating characteristics curve of the radiomics signature in the validation set (SCLC vs. NSCLC) was 0.84 (95% confidence interval (CI) 0.77-0.92) and 0.58 (95% CI 0.29-0.86) in the LCNEC dataset (SCLC-like vs. NSCLC-like).Conclusion: LCNEC appears to have radiological characteristics of both SCLC and NSCLC, irrespective of pRb loss, compatible with the SCLC-like subtype. Imaging interpretation, semantic features and our radiomics signature designed to differentiate between SCLC and NSCLC were unable to separate molecular LCNEC subtypes, which underscores that LCNEC is a unique disease.

Published

2020

38. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: A multicentre, randomised controlled open-label phase II trial

Author

Lieverse, R. I. Y., Van Limbergen, E. J., Oberije, C. J. G., Troost, E. G. C., Hadrup, S. R., Dingemans, A. -M. C., Hendriks, L. E. L., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., De Jong, M. C., Bussink, J., Geets, X., Valentini, Vincenzo, Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., De Ruysscher, D., Dubois, L. J., Lambin, P., Valentini V. (ORCID:0000-0003-4637-6487), Lieverse, R. I. Y., Van Limbergen, E. J., Oberije, C. J. G., Troost, E. G. C., Hadrup, S. R., Dingemans, A. -M. C., Hendriks, L. E. L., Eckert, F., Hiley, C., Dooms, C., Lievens, Y., De Jong, M. C., Bussink, J., Geets, X., Valentini, Vincenzo, Elia, G., Neri, D., Billiet, C., Abdollahi, A., Pasquier, D., Boisselier, P., Yaromina, A., De Ruysscher, D., Dubois, L. J., Lambin, P., and Valentini V. (ORCID:0000-0003-4637-6487)

Abstract

Background: About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). Methods: This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised to the experimental-arm (E-arm) or the control-arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). The accrual period will be 2.5-years, starting after the first centre is initiated and active. Primary endpoint is PFS at 1.5-years based on blinded radiological review, and secondary endpoints are overall survival, toxicity, quality of life and abscopal response. Associative biomarker studies, immune monitoring, CT-based radiomics, stool collection, iRECIST and tumour growth rate will be performed. Discussion: The combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd li

Published

2020

39. The image biomarker standardization initiative: Standardized quantitative radiomics for high-throughput image-based phenotyping

Author

Zwanenburg, A., Vallieres, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, Luca, Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M. -C., Dinapoli, Nicola, Dinh, C. V., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, Roberto, Gillies, R. J., Goh, V., Gotz, M., Guckenberger, M., Ha, S. M., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, Jacopo, Lippert, F., Losnegard, A., Maier-Hein, K. H., Morin, O., Muller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Siddique, M. M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., Troost, E. G. C., Upadhaya, T., Valentini, Vincenzo, van Dijk, L. V., van Griethuysen, J., van Velden, F. H. P., Whybra, P., Richter, C., Lock, S., Boldrini L., Dinapoli N., Gatta R., Lenkowicz J., Valentini V. (ORCID:0000-0003-4637-6487), Zwanenburg, A., Vallieres, M., Abdalah, M. A., Aerts, H. J. W. L., Andrearczyk, V., Apte, A., Ashrafinia, S., Bakas, S., Beukinga, R. J., Boellaard, R., Bogowicz, M., Boldrini, Luca, Buvat, I., Cook, G. J. R., Davatzikos, C., Depeursinge, A., Desseroit, M. -C., Dinapoli, Nicola, Dinh, C. V., Echegaray, S., El Naqa, I., Fedorov, A. Y., Gatta, Roberto, Gillies, R. J., Goh, V., Gotz, M., Guckenberger, M., Ha, S. M., Hatt, M., Isensee, F., Lambin, P., Leger, S., Leijenaar, R. T. H., Lenkowicz, Jacopo, Lippert, F., Losnegard, A., Maier-Hein, K. H., Morin, O., Muller, H., Napel, S., Nioche, C., Orlhac, F., Pati, S., Pfaehler, E. A. G., Rahmim, A., Rao, A. U. K., Scherer, J., Siddique, M. M., Sijtsema, N. M., Socarras Fernandez, J., Spezi, E., Steenbakkers, R. J. H. M., Tanadini-Lang, S., Thorwarth, D., Troost, E. G. C., Upadhaya, T., Valentini, Vincenzo, van Dijk, L. V., van Griethuysen, J., van Velden, F. H. P., Whybra, P., Richter, C., Lock, S., Boldrini L., Dinapoli N., Gatta R., Lenkowicz J., and Valentini V. (ORCID:0000-0003-4637-6487)

Abstract

Background: Radiomic features may quantify characteristics present in medical imaging. However, the lack of standardized definitions and validated reference values have hampered clinical use. Purpose: To standardize a set of 174 radiomic features. Materials and Methods: Radiomic features were assessed in three phases. In phase I, 487 features were derived from the basic set of 174 features. Twenty-five research teams with unique radiomics software implementations computed feature values directly from a digital phantom, without any additional image processing. In phase II, 15 teams computed values for 1347 derived features using a CT image of a patient with lung cancer and predefined image processing configurations. In both phases, consensus among the teams on the validity of tentative reference values was measured through the frequency of the modal value and classified as follows: less than three matches, weak; three to five matches, moderate; six to nine matches, strong; 10 or more matches, very strong. In the final phase (phase III), a public data set of multimodality images (CT, fluorine 18 fluorodeoxyglucose PET, and T1-weighted MRI) from 51 patients with soft-tissue sarcoma was used to prospectively assess reproducibility of standardized features. Results: Consensus on reference values was initially weak for 232 of 302 features (76.8%) at phase I and 703 of 1075 features (65.4%) at phase II. At the final iteration, weak consensus remained for only two of 487 features (0.4%) at phase I and 19 of 1347 features (1.4%) at phase II. Strong or better consensus was achieved for 463 of 487 features (95.1%) at phase I and 1220 of 1347 features (90.6%) at phase II. Overall, 169 of 174 features were standardized in the first two phases. In the final validation phase (phase III), most of the 169 standardized features could be excellently reproduced (166 with CT; 164 with PET; and 164 with MRI). Conclusion: A set of 169 radiomics features was standardized, which enabled ver

Published

2020

40. Exploring imaging features of molecular subtypes of large cell neuroendocrine carcinoma (LCNEC)

Author

Hermans, B. C.M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., Berge, D. M.H.J.ten, Speel, E. J.M., Lambin, P., Gietema, H. A., Dingemans, A. M.C., Hermans, B. C.M., Sanduleanu, S., Derks, J. L., Woodruff, H., Hillen, L. M., Casale, R., Hoesein, F. Mohamed, de Jong, E., Berge, D. M.H.J.ten, Speel, E. J.M., Lambin, P., Gietema, H. A., and Dingemans, A. M.C.

Abstract

Objectives: Radiological characteristics and radiomics signatures can aid in differentiation between small cell lung carcinoma (SCLC) and non-small cell lung carcinoma (NSCLC). We investigated whether molecular subtypes of large cell neuroendocrine carcinoma (LCNEC), i.e. SCLC-like (with pRb loss) vs. NSCLC-like (with pRb expression), can be distinguished by imaging based on (1) imaging interpretation, (2) semantic features, and/or (3) a radiomics signature, designed to differentiate between SCLC and NSCLC. Materials and Methods: Pulmonary oncologists and chest radiologists assessed chest CT-scans of 44 LCNEC patients for ‘small cell-like’ or ‘non-small cell-like’ appearance. The radiologists also scored semantic features of 50 LCNEC scans. Finally, a radiomics signature was trained on a dataset containing 48 SCLC and 76 NSCLC scans and validated on an external set of 58 SCLC and 40 NSCLC scans. This signature was applied on scans of 28 SCLC-like and 8 NSCLC-like LCNEC patients. Results: Pulmonary oncologists and radiologists were unable to differentiate between molecular subtypes of LCNEC and no significant differences in semantic features were found. The area under the receiver operating characteristics curve of the radiomics signature in the validation set (SCLC vs. NSCLC) was 0.84 (95% confidence interval (CI) 0.77-0.92) and 0.58 (95% CI 0.29-0.86) in the LCNEC dataset (SCLC-like vs. NSCLC-like). Conclusion: LCNEC appears to have radiological characteristics of both SCLC and NSCLC, irrespective of pRb loss, compatible with the SCLC-like subtype. Imaging interpretation, semantic features and our radiomics signature designed to differentiate between SCLC and NSCLC were unable to separate molecular LCNEC subtypes, which underscores that LCNEC is a unique disease.

Published

2020

41. Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

Author

Lieverse, RIY, Van Limbergen, EJ, Oberije, CJG, Troost, EGC, Hadrup, SR, Dingemans, AMA, Hendriks, LEL, Eckert, F, Hiley, C, Dooms, C, Lievens, Y, de Jong, M, Bussink, J, Geets, X, Valentini, V, Elia, G, Neri, D, Billiet, C, Abdollahi, A, Du Pasquier, D, Boisselier, P, Yaromina, A, De Ruysscher, D, Dubois, LJ, Lambin, P, Lieverse, RIY, Van Limbergen, EJ, Oberije, CJG, Troost, EGC, Hadrup, SR, Dingemans, AMA, Hendriks, LEL, Eckert, F, Hiley, C, Dooms, C, Lievens, Y, de Jong, M, Bussink, J, Geets, X, Valentini, V, Elia, G, Neri, D, Billiet, C, Abdollahi, A, Du Pasquier, D, Boisselier, P, Yaromina, A, De Ruysscher, D, Dubois, LJ, and Lambin, P

Published

2020

42. Nitroglycerin as a radiosensitizer in non-small cell lung cancer: Results of a prospective imaging-based phase II trial

Author

Reymen, BJT, van Gisbergen, MW, Even, AJG, Zegers, CML, Das, M, Vegt, Erik, Wildberger, JE, Mottaghy, FM, Yaromina, A, Dubois, LJ, van Elmpt, W, De Ruysscher, D, Lambin, P, Reymen, BJT, van Gisbergen, MW, Even, AJG, Zegers, CML, Das, M, Vegt, Erik, Wildberger, JE, Mottaghy, FM, Yaromina, A, Dubois, LJ, van Elmpt, W, De Ruysscher, D, and Lambin, P

Published

2020

43. Distributed learning on 20 000+ lung cancer patients – The Personal Health Train

Author

Deist, T. M., Dankers, F. J. W. M., Ojha, P., Scott Marshall, M., Janssen, T., Faivre-Finn, C., Masciocchi, Carlotta, Valentini, Vincenzo, Wang, J., Chen, J., Zhang, Z., Spezi, E., Button, M., Jan Nuyttens, J., Vernhout, R., van Soest, J., Jochems, A., Monshouwer, R., Bussink, J., Price, G., Lambin, P., Dekker, A., Masciocchi C., Valentini V. (ORCID:0000-0003-4637-6487), Deist, T. M., Dankers, F. J. W. M., Ojha, P., Scott Marshall, M., Janssen, T., Faivre-Finn, C., Masciocchi, Carlotta, Valentini, Vincenzo, Wang, J., Chen, J., Zhang, Z., Spezi, E., Button, M., Jan Nuyttens, J., Vernhout, R., van Soest, J., Jochems, A., Monshouwer, R., Bussink, J., Price, G., Lambin, P., Dekker, A., Masciocchi C., and Valentini V. (ORCID:0000-0003-4637-6487)

Abstract

Background and purpose: Access to healthcare data is indispensable for scientific progress and innovation. Sharing healthcare data is time-consuming and notoriously difficult due to privacy and regulatory concerns. The Personal Health Train (PHT) provides a privacy-by-design infrastructure connecting FAIR (Findable, Accessible, Interoperable, Reusable) data sources and allows distributed data analysis and machine learning. Patient data never leaves a healthcare institute. Materials and methods: Lung cancer patient-specific databases (tumor staging and post-treatment survival information) of oncology departments were translated according to a FAIR data model and stored locally in a graph database. Software was installed locally to enable deployment of distributed machine learning algorithms via a central server. Algorithms (MATLAB, code and documentation publicly available) are patient privacy-preserving as only summary statistics and regression coefficients are exchanged with the central server. A logistic regression model to predict post-treatment two-year survival was trained and evaluated by receiver operating characteristic curves (ROC), root mean square prediction error (RMSE) and calibration plots. Results: In 4 months, we connected databases with 23 203 patient cases across 8 healthcare institutes in 5 countries (Amsterdam, Cardiff, Maastricht, Manchester, Nijmegen, Rome, Rotterdam, Shanghai) using the PHT. Summary statistics were computed across databases. A distributed logistic regression model predicting post-treatment two-year survival was trained on 14 810 patients treated between 1978 and 2011 and validated on 8 393 patients treated between 2012 and 2015. Conclusion: The PHT infrastructure demonstrably overcomes patient privacy barriers to healthcare data sharing and enables fast data analyses across multiple institutes from different countries with different regulatory regimens. This infrastructure promotes global evidence-based medicine while prioriti

Published

2020

44. Addressing the dichotomy between individual and societal approaches to personalised medicine in oncology

Author

Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., Massard, C., Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., and Massard, C.

Abstract

Item does not contain fulltext, Academic, industry, regulatory leaders and patient advocates in cancer clinical research met in November 2018 at the Innovation and Biomarkers in Cancer Drug Development meeting in Brussels to address the existing dichotomy between increasing calls for personalised oncology approaches based on individual molecular profiles and the need to make resource and regulatory decisions at the societal level in differing health-care delivery systems around the globe. Novel clinical trial designs, the utility and limitations of real-world evidence (RWE) and emerging technologies for profiling patient tumours and tumour-derived DNA in plasma were discussed. While randomised clinical trials remain the gold standard approach to defining clinical utility of local and systemic therapeutic interventions, the broader adoption of comprehensive tumour profiling and novel trial designs coupled with RWE may allow patient and physician autonomy to be appropriately balanced with broader assessments of safety and overall societal benefit.

Published

2019

45. Intensity-modulated proton therapy decreases dose to organs at risk in low-grade glioma patients: results of a multicentric in silico ROCOCO trial

Author

Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., Troost, E.G., Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., and Troost, E.G.

Abstract

Contains fulltext : 203174.pdf (publisher's version ) (Open Access), BACKGROUND AND PURPOSE: Patients with low-grade glioma (LGG) have a prolonged survival expectancy due to better discriminative tumor classification and multimodal treatment. Consequently, long-term treatment toxicity gains importance. Contemporary radiotherapy techniques such as intensity-modulated radiotherapy (IMRT), volumetric modulated arc therapy (VMAT), tomotherapy (TOMO) and intensity-modulated proton therapy (IMPT) enable high-dose irradiation of the target but they differ regarding delivered dose to organs at risk (OARs). The aim of this comparative in silico study was to determine these dosimetric differences in delivered doses. MATERIAL AND METHODS: Imaging datasets of 25 LGG patients having undergone postoperative radiotherapy were included. For each of these patients, in silico treatment plans to a total dose of 50.4 Gy to the target volume were generated for the four treatment modalities investigated (i.e., IMRT, VMAT, TOMO, IMPT). Resulting treatment plans were analyzed regarding dose to target and surrounding OARs comparing IMRT, TOMO and IMPT to VMAT. RESULTS: In total, 100 treatment plans (four per patient) were analyzed. Compared to VMAT, the IMPT mean dose (Dmean) for nine out of 10 (90%) OARs was statistically significantly (p < .02) reduced, for TOMO this was true in 3/10 (30%) patients and for 1/10 (10%) patients for IMRT. IMPT was the prime modality reducing dose to the OARs followed by TOMO. DISCUSSION: The low dose volume to the majority of OARs was significantly reduced when using IMPT compared to VMAT. Whether this will lead to a significant reduction in neurocognitive decline and improved quality of life is to be determined in carefully designed future clinical trials.

Published

2019

46. Addressing the dichotomy between individual and societal approaches to personalised medicine in oncology

Author

Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., Massard, C., Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., and Massard, C.

Abstract

Item does not contain fulltext, Academic, industry, regulatory leaders and patient advocates in cancer clinical research met in November 2018 at the Innovation and Biomarkers in Cancer Drug Development meeting in Brussels to address the existing dichotomy between increasing calls for personalised oncology approaches based on individual molecular profiles and the need to make resource and regulatory decisions at the societal level in differing health-care delivery systems around the globe. Novel clinical trial designs, the utility and limitations of real-world evidence (RWE) and emerging technologies for profiling patient tumours and tumour-derived DNA in plasma were discussed. While randomised clinical trials remain the gold standard approach to defining clinical utility of local and systemic therapeutic interventions, the broader adoption of comprehensive tumour profiling and novel trial designs coupled with RWE may allow patient and physician autonomy to be appropriately balanced with broader assessments of safety and overall societal benefit.

Published

2019

47. Intensity-modulated proton therapy decreases dose to organs at risk in low-grade glioma patients: results of a multicentric in silico ROCOCO trial

Author

Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., Troost, E.G., Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., and Troost, E.G.

Abstract

Contains fulltext : 203174.pdf (publisher's version ) (Open Access), BACKGROUND AND PURPOSE: Patients with low-grade glioma (LGG) have a prolonged survival expectancy due to better discriminative tumor classification and multimodal treatment. Consequently, long-term treatment toxicity gains importance. Contemporary radiotherapy techniques such as intensity-modulated radiotherapy (IMRT), volumetric modulated arc therapy (VMAT), tomotherapy (TOMO) and intensity-modulated proton therapy (IMPT) enable high-dose irradiation of the target but they differ regarding delivered dose to organs at risk (OARs). The aim of this comparative in silico study was to determine these dosimetric differences in delivered doses. MATERIAL AND METHODS: Imaging datasets of 25 LGG patients having undergone postoperative radiotherapy were included. For each of these patients, in silico treatment plans to a total dose of 50.4 Gy to the target volume were generated for the four treatment modalities investigated (i.e., IMRT, VMAT, TOMO, IMPT). Resulting treatment plans were analyzed regarding dose to target and surrounding OARs comparing IMRT, TOMO and IMPT to VMAT. RESULTS: In total, 100 treatment plans (four per patient) were analyzed. Compared to VMAT, the IMPT mean dose (Dmean) for nine out of 10 (90%) OARs was statistically significantly (p < .02) reduced, for TOMO this was true in 3/10 (30%) patients and for 1/10 (10%) patients for IMRT. IMPT was the prime modality reducing dose to the OARs followed by TOMO. DISCUSSION: The low dose volume to the majority of OARs was significantly reduced when using IMPT compared to VMAT. Whether this will lead to a significant reduction in neurocognitive decline and improved quality of life is to be determined in carefully designed future clinical trials.

Published

2019

48. Intensity-modulated proton therapy decreases dose to organs at risk in low-grade glioma patients: results of a multicentric in silico ROCOCO trial

Author

Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., Troost, E.G., Eekers, D.B., Roelofs, E., Cubillos-Mesias, M., Niel, C., Smeenk, R.J., Hoeben, A., Minken, A.W.H., Granzier, M., Janssens, G.O., Kaanders, J.H., Lambin, P., and Troost, E.G.

Abstract

Contains fulltext : 203174.pdf (publisher's version ) (Open Access), BACKGROUND AND PURPOSE: Patients with low-grade glioma (LGG) have a prolonged survival expectancy due to better discriminative tumor classification and multimodal treatment. Consequently, long-term treatment toxicity gains importance. Contemporary radiotherapy techniques such as intensity-modulated radiotherapy (IMRT), volumetric modulated arc therapy (VMAT), tomotherapy (TOMO) and intensity-modulated proton therapy (IMPT) enable high-dose irradiation of the target but they differ regarding delivered dose to organs at risk (OARs). The aim of this comparative in silico study was to determine these dosimetric differences in delivered doses. MATERIAL AND METHODS: Imaging datasets of 25 LGG patients having undergone postoperative radiotherapy were included. For each of these patients, in silico treatment plans to a total dose of 50.4 Gy to the target volume were generated for the four treatment modalities investigated (i.e., IMRT, VMAT, TOMO, IMPT). Resulting treatment plans were analyzed regarding dose to target and surrounding OARs comparing IMRT, TOMO and IMPT to VMAT. RESULTS: In total, 100 treatment plans (four per patient) were analyzed. Compared to VMAT, the IMPT mean dose (Dmean) for nine out of 10 (90%) OARs was statistically significantly (p < .02) reduced, for TOMO this was true in 3/10 (30%) patients and for 1/10 (10%) patients for IMRT. IMPT was the prime modality reducing dose to the OARs followed by TOMO. DISCUSSION: The low dose volume to the majority of OARs was significantly reduced when using IMPT compared to VMAT. Whether this will lead to a significant reduction in neurocognitive decline and improved quality of life is to be determined in carefully designed future clinical trials.

Published

2019

49. Addressing the dichotomy between individual and societal approaches to personalised medicine in oncology

Author

Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., Massard, C., Salgado, R., Solit, D.B., Rimm, D.L., Bogaerts, J., Canetta, R., Lively, T., Lyerly, K., Span, P.N., Bateman-House, A., Makady, A., Bergmann, L., Nagai, S., Smith, C., Robson, M., Savage, M., Voest, E., Sweeney, C., Lambin, P., Thomas, M., Harris, L., Lacombe, D., and Massard, C.

Abstract

Item does not contain fulltext, Academic, industry, regulatory leaders and patient advocates in cancer clinical research met in November 2018 at the Innovation and Biomarkers in Cancer Drug Development meeting in Brussels to address the existing dichotomy between increasing calls for personalised oncology approaches based on individual molecular profiles and the need to make resource and regulatory decisions at the societal level in differing health-care delivery systems around the globe. Novel clinical trial designs, the utility and limitations of real-world evidence (RWE) and emerging technologies for profiling patient tumours and tumour-derived DNA in plasma were discussed. While randomised clinical trials remain the gold standard approach to defining clinical utility of local and systemic therapeutic interventions, the broader adoption of comprehensive tumour profiling and novel trial designs coupled with RWE may allow patient and physician autonomy to be appropriately balanced with broader assessments of safety and overall societal benefit.

Published

2019

50. Challenges and caveats of a multi-center retrospective radiomics study: An example of early treatment response assessment for NSCLC patients using FDG-PET/CT radiomics

Author

Timmeren, J.-E., Carvalho, S., Leijenaar, R. T. H., Troost, E. G. C., Elmpt, W., Ruysscher, D., Muratet, J. P., Denis, F., Schimek-Jasch, T., Nestle, U., Jochems, A., Woodruff, H. C., Oberije, C., Lambin, P., Timmeren, J.-E., Carvalho, S., Leijenaar, R. T. H., Troost, E. G. C., Elmpt, W., Ruysscher, D., Muratet, J. P., Denis, F., Schimek-Jasch, T., Nestle, U., Jochems, A., Woodruff, H. C., Oberije, C., and Lambin, P.

Abstract

Background Prognostic models based on individual patient characteristics can improve treatment decisions and outcome in the future. In many (radiomic) studies, small size and heterogeneity of datasets is a challenge that often limits performance and potential clinical applicability of these models. The current study is example of a retrospective multi-centric study with challenges and caveats. To highlight common issues and emphasize potential pitfalls, we aimed for an extensive analysis of these multi-center pre-treatment datasets, with an additional 18F-fluorodeoxyglucose (FDG) positron emission tomography/computed tomography (PET/ CT) scan acquired during treatment. Methods The dataset consisted of 138 stage II-IV non-small cell lung cancer (NSCLC) patients from four different cohorts acquired from three different institutes. The differences between the cohorts were compared in terms of clinical characteristics and using the so-called ‘cohort differences model’ approach. Moreover, the potential prognostic performances for overall survival of radiomic features extracted from CT or FDG-PET, or relative or absolute differences between the scans at the two time points, were assessed using the LASSO regression method. Furthermore, the performances of five different classifiers were evaluated for all image sets. Results The individual cohorts substantially differed in terms of patient characteristics. Moreover, the cohort differences model indicated statistically significant differences between the cohorts. Neither LASSO nor any of the tested classifiers resulted in a clinical relevant prognostic model that could be validated on the available datasets. Conclusion The results imply that the study might have been influenced by a limited sample size, heterogeneous patient characteristics, and inconsistent imaging parameters. No prognostic performance of FDG-PET or CT based radiomics models can be reported. This study highlights the necessity of extensive evaluations of co

Published

2019