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Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility

OBJECTIVES: To investigate sources of variation in a multicenter rectal cancer MRI dataset focusing on hardware and image acquisition, segmentation methodology, and radiomics feature extraction software. METHODS: T2W and DWI/ADC MRIs from 649 rectal cancer patients were retrospectively acquired in 9...

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Autores principales: Schurink, Niels W., van Kranen, Simon R., Roberti, Sander, van Griethuysen, Joost J. M., Bogveradze, Nino, Castagnoli, Francesca, el Khababi, Najim, Bakers, Frans C. H., de Bie, Shira H., Bosma, Gerlof P. T., Cappendijk, Vincent C., Geenen, Remy W. F., Neijenhuis, Peter A., Peterson, Gerald M., Veeken, Cornelis J., Vliegen, Roy F. A., Beets-Tan, Regina G. H., Lambregts, Doenja M. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Berlin Heidelberg 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8831294/
https://www.ncbi.nlm.nih.gov/pubmed/34655313
http://dx.doi.org/10.1007/s00330-021-08251-8
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author Schurink, Niels W.
van Kranen, Simon R.
Roberti, Sander
van Griethuysen, Joost J. M.
Bogveradze, Nino
Castagnoli, Francesca
el Khababi, Najim
Bakers, Frans C. H.
de Bie, Shira H.
Bosma, Gerlof P. T.
Cappendijk, Vincent C.
Geenen, Remy W. F.
Neijenhuis, Peter A.
Peterson, Gerald M.
Veeken, Cornelis J.
Vliegen, Roy F. A.
Beets-Tan, Regina G. H.
Lambregts, Doenja M. J.
author_facet Schurink, Niels W.
van Kranen, Simon R.
Roberti, Sander
van Griethuysen, Joost J. M.
Bogveradze, Nino
Castagnoli, Francesca
el Khababi, Najim
Bakers, Frans C. H.
de Bie, Shira H.
Bosma, Gerlof P. T.
Cappendijk, Vincent C.
Geenen, Remy W. F.
Neijenhuis, Peter A.
Peterson, Gerald M.
Veeken, Cornelis J.
Vliegen, Roy F. A.
Beets-Tan, Regina G. H.
Lambregts, Doenja M. J.
author_sort Schurink, Niels W.
collection PubMed
description OBJECTIVES: To investigate sources of variation in a multicenter rectal cancer MRI dataset focusing on hardware and image acquisition, segmentation methodology, and radiomics feature extraction software. METHODS: T2W and DWI/ADC MRIs from 649 rectal cancer patients were retrospectively acquired in 9 centers. Fifty-two imaging features (14 first-order/6 shape/32 higher-order) were extracted from each scan using whole-volume (expert/non-expert) and single-slice segmentations using two different software packages (PyRadiomics/CapTk). Influence of hardware, acquisition, and patient-intrinsic factors (age/gender/cTN-stage) on ADC was assessed using linear regression. Feature reproducibility was assessed between segmentation methods and software packages using the intraclass correlation coefficient. RESULTS: Image features differed significantly (p < 0.001) between centers with more substantial variations in ADC compared to T2W-MRI. In total, 64.3% of the variation in mean ADC was explained by differences in hardware and acquisition, compared to 0.4% by patient-intrinsic factors. Feature reproducibility between expert and non-expert segmentations was good to excellent (median ICC 0.89–0.90). Reproducibility for single-slice versus whole-volume segmentations was substantially poorer (median ICC 0.40–0.58). Between software packages, reproducibility was good to excellent (median ICC 0.99) for most features (first-order/shape/GLCM/GLRLM) but poor for higher-order (GLSZM/NGTDM) features (median ICC 0.00–0.41). CONCLUSIONS: Significant variations are present in multicenter MRI data, particularly related to differences in hardware and acquisition, which will likely negatively influence subsequent analysis if not corrected for. Segmentation variations had a minor impact when using whole volume segmentations. Between software packages, higher-order features were less reproducible and caution is warranted when implementing these in prediction models. KEY POINTS: • Features derived from T2W-MRI and in particular ADC differ significantly between centers when performing multicenter data analysis. • Variations in ADC are mainly (> 60%) caused by hardware and image acquisition differences and less so (< 1%) by patient- or tumor-intrinsic variations. • Features derived using different image segmentations (expert/non-expert) were reproducible, provided that whole-volume segmentations were used. When using different feature extraction software packages with similar settings, higher-order features were less reproducible. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s00330-021-08251-8.
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spelling pubmed-88312942022-02-23 Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility Schurink, Niels W. van Kranen, Simon R. Roberti, Sander van Griethuysen, Joost J. M. Bogveradze, Nino Castagnoli, Francesca el Khababi, Najim Bakers, Frans C. H. de Bie, Shira H. Bosma, Gerlof P. T. Cappendijk, Vincent C. Geenen, Remy W. F. Neijenhuis, Peter A. Peterson, Gerald M. Veeken, Cornelis J. Vliegen, Roy F. A. Beets-Tan, Regina G. H. Lambregts, Doenja M. J. Eur Radiol Imaging Informatics and Artificial Intelligence OBJECTIVES: To investigate sources of variation in a multicenter rectal cancer MRI dataset focusing on hardware and image acquisition, segmentation methodology, and radiomics feature extraction software. METHODS: T2W and DWI/ADC MRIs from 649 rectal cancer patients were retrospectively acquired in 9 centers. Fifty-two imaging features (14 first-order/6 shape/32 higher-order) were extracted from each scan using whole-volume (expert/non-expert) and single-slice segmentations using two different software packages (PyRadiomics/CapTk). Influence of hardware, acquisition, and patient-intrinsic factors (age/gender/cTN-stage) on ADC was assessed using linear regression. Feature reproducibility was assessed between segmentation methods and software packages using the intraclass correlation coefficient. RESULTS: Image features differed significantly (p < 0.001) between centers with more substantial variations in ADC compared to T2W-MRI. In total, 64.3% of the variation in mean ADC was explained by differences in hardware and acquisition, compared to 0.4% by patient-intrinsic factors. Feature reproducibility between expert and non-expert segmentations was good to excellent (median ICC 0.89–0.90). Reproducibility for single-slice versus whole-volume segmentations was substantially poorer (median ICC 0.40–0.58). Between software packages, reproducibility was good to excellent (median ICC 0.99) for most features (first-order/shape/GLCM/GLRLM) but poor for higher-order (GLSZM/NGTDM) features (median ICC 0.00–0.41). CONCLUSIONS: Significant variations are present in multicenter MRI data, particularly related to differences in hardware and acquisition, which will likely negatively influence subsequent analysis if not corrected for. Segmentation variations had a minor impact when using whole volume segmentations. Between software packages, higher-order features were less reproducible and caution is warranted when implementing these in prediction models. KEY POINTS: • Features derived from T2W-MRI and in particular ADC differ significantly between centers when performing multicenter data analysis. • Variations in ADC are mainly (> 60%) caused by hardware and image acquisition differences and less so (< 1%) by patient- or tumor-intrinsic variations. • Features derived using different image segmentations (expert/non-expert) were reproducible, provided that whole-volume segmentations were used. When using different feature extraction software packages with similar settings, higher-order features were less reproducible. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s00330-021-08251-8. Springer Berlin Heidelberg 2021-10-16 2022 /pmc/articles/PMC8831294/ /pubmed/34655313 http://dx.doi.org/10.1007/s00330-021-08251-8 Text en © The Author(s) 2021, corrected publication 2022 https://creativecommons.org/licenses/by/4.0/Open AccessThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Imaging Informatics and Artificial Intelligence
Schurink, Niels W.
van Kranen, Simon R.
Roberti, Sander
van Griethuysen, Joost J. M.
Bogveradze, Nino
Castagnoli, Francesca
el Khababi, Najim
Bakers, Frans C. H.
de Bie, Shira H.
Bosma, Gerlof P. T.
Cappendijk, Vincent C.
Geenen, Remy W. F.
Neijenhuis, Peter A.
Peterson, Gerald M.
Veeken, Cornelis J.
Vliegen, Roy F. A.
Beets-Tan, Regina G. H.
Lambregts, Doenja M. J.
Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title_full Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title_fullStr Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title_full_unstemmed Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title_short Sources of variation in multicenter rectal MRI data and their effect on radiomics feature reproducibility
title_sort sources of variation in multicenter rectal mri data and their effect on radiomics feature reproducibility
topic Imaging Informatics and Artificial Intelligence
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8831294/
https://www.ncbi.nlm.nih.gov/pubmed/34655313
http://dx.doi.org/10.1007/s00330-021-08251-8
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