Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma

BACKGROUND: The prognostic roles of clinical and laboratory markers have been exploited to model risk in patients with primary CNS lymphoma, but these approaches do not fully explain the observed variation in outcome. To date, neuroimaging or molecular information is not used. The aim of this study...

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Autores principales: Nenning, Karl-Heinz, Gesperger, Johanna, Furtner, Julia, Nemc, Amelie, Roetzer-Pejrimovsky, Thomas, Choi, Seung-Won, Mitter, Christian, Leber, Stefan L, Hofmanninger, Johannes, Klughammer, Johanna, Ergüner, Bekir, Bauer, Marlies, Brada, Martina, Chong, Kyuha, Brandner-Kokalj, Tanisa, Freyschlag, Christian F, Grams, Astrid, Haybaeck, Johannes, Hoenigschnabl, Selma, Hoffermann, Markus, Iglseder, Sarah, Kiesel, Barbara, Kitzwoegerer, Melitta, Kleindienst, Waltraud, Marhold, Franz, Moser, Patrizia, Oberndorfer, Stefan, Pinggera, Daniel, Scheichel, Florian, Sherif, Camillo, Stockhammer, Guenther, Stultschnig, Martin, Thomé, Claudius, Trenkler, Johannes, Urbanic-Purkart, Tadeja, Weis, Serge, Widhalm, Georg, Wuertz, Franz, Preusser, Matthias, Baumann, Bernhard, Simonitsch-Klupp, Ingrid, Nam, Do-Hyun, Bock, Christoph, Langs, Georg, Woehrer, Adelheid
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Basic and Translational Investigations
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10676053/
https://www.ncbi.nlm.nih.gov/pubmed/38024240
http://dx.doi.org/10.1093/noajnl/vdad136
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author Nenning, Karl-Heinz
Gesperger, Johanna
Furtner, Julia
Nemc, Amelie
Roetzer-Pejrimovsky, Thomas
Choi, Seung-Won
Mitter, Christian
Leber, Stefan L
Hofmanninger, Johannes
Klughammer, Johanna
Ergüner, Bekir
Bauer, Marlies
Brada, Martina
Chong, Kyuha
Brandner-Kokalj, Tanisa
Freyschlag, Christian F
Grams, Astrid
Haybaeck, Johannes
Hoenigschnabl, Selma
Hoffermann, Markus
Iglseder, Sarah
Kiesel, Barbara
Kitzwoegerer, Melitta
Kleindienst, Waltraud
Marhold, Franz
Moser, Patrizia
Oberndorfer, Stefan
Pinggera, Daniel
Scheichel, Florian
Sherif, Camillo
Stockhammer, Guenther
Stultschnig, Martin
Thomé, Claudius
Trenkler, Johannes
Urbanic-Purkart, Tadeja
Weis, Serge
Widhalm, Georg
Wuertz, Franz
Preusser, Matthias
Baumann, Bernhard
Simonitsch-Klupp, Ingrid
Nam, Do-Hyun
Bock, Christoph
Langs, Georg
Woehrer, Adelheid
author_facet Nenning, Karl-Heinz
Gesperger, Johanna
Furtner, Julia
Nemc, Amelie
Roetzer-Pejrimovsky, Thomas
Choi, Seung-Won
Mitter, Christian
Leber, Stefan L
Hofmanninger, Johannes
Klughammer, Johanna
Ergüner, Bekir
Bauer, Marlies
Brada, Martina
Chong, Kyuha
Brandner-Kokalj, Tanisa
Freyschlag, Christian F
Grams, Astrid
Haybaeck, Johannes
Hoenigschnabl, Selma
Hoffermann, Markus
Iglseder, Sarah
Kiesel, Barbara
Kitzwoegerer, Melitta
Kleindienst, Waltraud
Marhold, Franz
Moser, Patrizia
Oberndorfer, Stefan
Pinggera, Daniel
Scheichel, Florian
Sherif, Camillo
Stockhammer, Guenther
Stultschnig, Martin
Thomé, Claudius
Trenkler, Johannes
Urbanic-Purkart, Tadeja
Weis, Serge
Widhalm, Georg
Wuertz, Franz
Preusser, Matthias
Baumann, Bernhard
Simonitsch-Klupp, Ingrid
Nam, Do-Hyun
Bock, Christoph
Langs, Georg
Woehrer, Adelheid
author_sort Nenning, Karl-Heinz
collection PubMed
description BACKGROUND: The prognostic roles of clinical and laboratory markers have been exploited to model risk in patients with primary CNS lymphoma, but these approaches do not fully explain the observed variation in outcome. To date, neuroimaging or molecular information is not used. The aim of this study was to determine the utility of radiomic features to capture clinically relevant phenotypes, and to link those to molecular profiles for enhanced risk stratification. METHODS: In this retrospective study, we investigated 133 patients across 9 sites in Austria (2005–2018) and an external validation site in South Korea (44 patients, 2013–2016). We used T1-weighted contrast-enhanced MRI and an L1-norm regularized Cox proportional hazard model to derive a radiomic risk score. We integrated radiomic features with DNA methylation profiles using machine learning-based prediction, and validated the most relevant biological associations in tissues and cell lines. RESULTS: The radiomic risk score, consisting of 20 mostly textural features, was a strong and independent predictor of survival (multivariate hazard ratio = 6.56 [3.64–11.81]) that remained valid in the external validation cohort. Radiomic features captured gene regulatory differences such as in BCL6 binding activity, which was put forth as testable treatment target for a subset of patients. CONCLUSIONS: The radiomic risk score was a robust and complementary predictor of survival and reflected characteristics in underlying DNA methylation patterns. Leveraging imaging phenotypes to assess risk and inform epigenetic treatment targets provides a concept on which to advance prognostic modeling and precision therapy for this aggressive cancer.
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spelling pubmed-106760532023-10-18 Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma Nenning, Karl-Heinz Gesperger, Johanna Furtner, Julia Nemc, Amelie Roetzer-Pejrimovsky, Thomas Choi, Seung-Won Mitter, Christian Leber, Stefan L Hofmanninger, Johannes Klughammer, Johanna Ergüner, Bekir Bauer, Marlies Brada, Martina Chong, Kyuha Brandner-Kokalj, Tanisa Freyschlag, Christian F Grams, Astrid Haybaeck, Johannes Hoenigschnabl, Selma Hoffermann, Markus Iglseder, Sarah Kiesel, Barbara Kitzwoegerer, Melitta Kleindienst, Waltraud Marhold, Franz Moser, Patrizia Oberndorfer, Stefan Pinggera, Daniel Scheichel, Florian Sherif, Camillo Stockhammer, Guenther Stultschnig, Martin Thomé, Claudius Trenkler, Johannes Urbanic-Purkart, Tadeja Weis, Serge Widhalm, Georg Wuertz, Franz Preusser, Matthias Baumann, Bernhard Simonitsch-Klupp, Ingrid Nam, Do-Hyun Bock, Christoph Langs, Georg Woehrer, Adelheid Neurooncol Adv Basic and Translational Investigations BACKGROUND: The prognostic roles of clinical and laboratory markers have been exploited to model risk in patients with primary CNS lymphoma, but these approaches do not fully explain the observed variation in outcome. To date, neuroimaging or molecular information is not used. The aim of this study was to determine the utility of radiomic features to capture clinically relevant phenotypes, and to link those to molecular profiles for enhanced risk stratification. METHODS: In this retrospective study, we investigated 133 patients across 9 sites in Austria (2005–2018) and an external validation site in South Korea (44 patients, 2013–2016). We used T1-weighted contrast-enhanced MRI and an L1-norm regularized Cox proportional hazard model to derive a radiomic risk score. We integrated radiomic features with DNA methylation profiles using machine learning-based prediction, and validated the most relevant biological associations in tissues and cell lines. RESULTS: The radiomic risk score, consisting of 20 mostly textural features, was a strong and independent predictor of survival (multivariate hazard ratio = 6.56 [3.64–11.81]) that remained valid in the external validation cohort. Radiomic features captured gene regulatory differences such as in BCL6 binding activity, which was put forth as testable treatment target for a subset of patients. CONCLUSIONS: The radiomic risk score was a robust and complementary predictor of survival and reflected characteristics in underlying DNA methylation patterns. Leveraging imaging phenotypes to assess risk and inform epigenetic treatment targets provides a concept on which to advance prognostic modeling and precision therapy for this aggressive cancer. Oxford University Press 2023-10-18 /pmc/articles/PMC10676053/ /pubmed/38024240 http://dx.doi.org/10.1093/noajnl/vdad136 Text en © The Author(s) 2023. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Basic and Translational Investigations
Nenning, Karl-Heinz
Gesperger, Johanna
Furtner, Julia
Nemc, Amelie
Roetzer-Pejrimovsky, Thomas
Choi, Seung-Won
Mitter, Christian
Leber, Stefan L
Hofmanninger, Johannes
Klughammer, Johanna
Ergüner, Bekir
Bauer, Marlies
Brada, Martina
Chong, Kyuha
Brandner-Kokalj, Tanisa
Freyschlag, Christian F
Grams, Astrid
Haybaeck, Johannes
Hoenigschnabl, Selma
Hoffermann, Markus
Iglseder, Sarah
Kiesel, Barbara
Kitzwoegerer, Melitta
Kleindienst, Waltraud
Marhold, Franz
Moser, Patrizia
Oberndorfer, Stefan
Pinggera, Daniel
Scheichel, Florian
Sherif, Camillo
Stockhammer, Guenther
Stultschnig, Martin
Thomé, Claudius
Trenkler, Johannes
Urbanic-Purkart, Tadeja
Weis, Serge
Widhalm, Georg
Wuertz, Franz
Preusser, Matthias
Baumann, Bernhard
Simonitsch-Klupp, Ingrid
Nam, Do-Hyun
Bock, Christoph
Langs, Georg
Woehrer, Adelheid
Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title_full Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title_fullStr Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title_full_unstemmed Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title_short Radiomic features define risk and are linked to DNA methylation attributes in primary CNS lymphoma
title_sort radiomic features define risk and are linked to dna methylation attributes in primary cns lymphoma
topic Basic and Translational Investigations
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10676053/
https://www.ncbi.nlm.nih.gov/pubmed/38024240
http://dx.doi.org/10.1093/noajnl/vdad136
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