Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location

Objective: Vertebral bone marrow composition has been extensively studied in the past and shown potential as imaging biomarker for osteoporosis, hematopoietic, and metabolic disorders. However, beyond quantitative assessment of bone marrow fat, little is known about its heterogeneity. Therefore, we...

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Autores principales: Dieckmeyer, Michael, Junker, Daniela, Ruschke, Stefan, Mookiah, Muthu Rama Krishnan, Subburaj, Karupppasamy, Burian, Egon, Sollmann, Nico, Kirschke, Jan S., Karampinos, Dimitrios C., Baum, Thomas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7593641/
https://www.ncbi.nlm.nih.gov/pubmed/33178134
http://dx.doi.org/10.3389/fendo.2020.555931
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author Dieckmeyer, Michael
Junker, Daniela
Ruschke, Stefan
Mookiah, Muthu Rama Krishnan
Subburaj, Karupppasamy
Burian, Egon
Sollmann, Nico
Kirschke, Jan S.
Karampinos, Dimitrios C.
Baum, Thomas
author_facet Dieckmeyer, Michael
Junker, Daniela
Ruschke, Stefan
Mookiah, Muthu Rama Krishnan
Subburaj, Karupppasamy
Burian, Egon
Sollmann, Nico
Kirschke, Jan S.
Karampinos, Dimitrios C.
Baum, Thomas
author_sort Dieckmeyer, Michael
collection PubMed
description Objective: Vertebral bone marrow composition has been extensively studied in the past and shown potential as imaging biomarker for osteoporosis, hematopoietic, and metabolic disorders. However, beyond quantitative assessment of bone marrow fat, little is known about its heterogeneity. Therefore, we investigated bone marrow heterogeneity of the lumbar spine using texture analysis of chemical-shift-encoding (CSE-MRI) based proton density fat fraction (PDFF) maps and its association with age, sex, and anatomical location. Methods: One hundred and fifty-six healthy subjects were scanned (age range: 20–29 years, 12/30 males/females; 30–39, 15/9; 40–49, 5/13; 50–59, 9/27; ≥60: 9/27). A sagittal 8-echo 3D spoiled-gradient-echo sequence at 3T was used for CSE-MRI-based water-fat separation at the lumbar spine. Manual segmentation of vertebral bodies L1-4 was performed. Mean PDFF and texture features (global: variance, skewness, kurtosis; second-order: energy, entropy, contrast, homogeneity, correlation, sum-average, variance, dissimilarity) were extracted at each vertebral level and compared between age groups, sex, and anatomical location. Results: Mean PDFF significantly increased from L1 to L4 (35.89 ± 11.66 to 39.52 ± 11.18%, p = 0.017) and with age (females: 27.19 ± 6.01 to 49.34 ± 7.75%, p < 0.001; males: 31.97 ± 7.96 to 41.83 ± 7.03 %, p = 0.025), but showed no difference between females and males after adjustment for age and BMI (37.13 ± 11.63 vs. 37.17 ± 8.67%; p = 0.199). Bone marrow heterogeneity assessed by texture analysis, in contrast to PDFF, was significantly higher in females compared to males after adjustment for age and BMI (namely contrast and dissimilarity; p < 0.031), demonstrated age-dependent differences, in particular in females (p < 0.05), but showed no statistically significant dependence on vertebral location. Conclusion: Vertebral bone marrow heterogeneity, assessed by texture analysis of PDFF maps, is primarily dependent on sex and age but not on anatomical location. Future studies are needed to investigate bone marrow heterogeneity with regard to aging and disease.
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spelling pubmed-75936412020-11-10 Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location Dieckmeyer, Michael Junker, Daniela Ruschke, Stefan Mookiah, Muthu Rama Krishnan Subburaj, Karupppasamy Burian, Egon Sollmann, Nico Kirschke, Jan S. Karampinos, Dimitrios C. Baum, Thomas Front Endocrinol (Lausanne) Endocrinology Objective: Vertebral bone marrow composition has been extensively studied in the past and shown potential as imaging biomarker for osteoporosis, hematopoietic, and metabolic disorders. However, beyond quantitative assessment of bone marrow fat, little is known about its heterogeneity. Therefore, we investigated bone marrow heterogeneity of the lumbar spine using texture analysis of chemical-shift-encoding (CSE-MRI) based proton density fat fraction (PDFF) maps and its association with age, sex, and anatomical location. Methods: One hundred and fifty-six healthy subjects were scanned (age range: 20–29 years, 12/30 males/females; 30–39, 15/9; 40–49, 5/13; 50–59, 9/27; ≥60: 9/27). A sagittal 8-echo 3D spoiled-gradient-echo sequence at 3T was used for CSE-MRI-based water-fat separation at the lumbar spine. Manual segmentation of vertebral bodies L1-4 was performed. Mean PDFF and texture features (global: variance, skewness, kurtosis; second-order: energy, entropy, contrast, homogeneity, correlation, sum-average, variance, dissimilarity) were extracted at each vertebral level and compared between age groups, sex, and anatomical location. Results: Mean PDFF significantly increased from L1 to L4 (35.89 ± 11.66 to 39.52 ± 11.18%, p = 0.017) and with age (females: 27.19 ± 6.01 to 49.34 ± 7.75%, p < 0.001; males: 31.97 ± 7.96 to 41.83 ± 7.03 %, p = 0.025), but showed no difference between females and males after adjustment for age and BMI (37.13 ± 11.63 vs. 37.17 ± 8.67%; p = 0.199). Bone marrow heterogeneity assessed by texture analysis, in contrast to PDFF, was significantly higher in females compared to males after adjustment for age and BMI (namely contrast and dissimilarity; p < 0.031), demonstrated age-dependent differences, in particular in females (p < 0.05), but showed no statistically significant dependence on vertebral location. Conclusion: Vertebral bone marrow heterogeneity, assessed by texture analysis of PDFF maps, is primarily dependent on sex and age but not on anatomical location. Future studies are needed to investigate bone marrow heterogeneity with regard to aging and disease. Frontiers Media S.A. 2020-10-15 /pmc/articles/PMC7593641/ /pubmed/33178134 http://dx.doi.org/10.3389/fendo.2020.555931 Text en Copyright © 2020 Dieckmeyer, Junker, Ruschke, Mookiah, Subburaj, Burian, Sollmann, Kirschke, Karampinos and Baum. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Dieckmeyer, Michael
Junker, Daniela
Ruschke, Stefan
Mookiah, Muthu Rama Krishnan
Subburaj, Karupppasamy
Burian, Egon
Sollmann, Nico
Kirschke, Jan S.
Karampinos, Dimitrios C.
Baum, Thomas
Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title_full Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title_fullStr Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title_full_unstemmed Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title_short Vertebral Bone Marrow Heterogeneity Using Texture Analysis of Chemical Shift Encoding-Based MRI: Variations in Age, Sex, and Anatomical Location
title_sort vertebral bone marrow heterogeneity using texture analysis of chemical shift encoding-based mri: variations in age, sex, and anatomical location
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7593641/
https://www.ncbi.nlm.nih.gov/pubmed/33178134
http://dx.doi.org/10.3389/fendo.2020.555931
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