Cargando…
Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas
Glioma is recognized to be a highly heterogeneous CNS malignancy, whose diverse cellular composition and cellular interactions have not been well characterized. To gain new clinical- and biological-insights into the genetically-bifurcated IDH1 mutant (mt) vs wildtype (wt) forms of glioma, we integra...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2019
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6934292/ https://www.ncbi.nlm.nih.gov/pubmed/31881020 http://dx.doi.org/10.1371/journal.pone.0219724 |
| _version_ | 1783483359490473984 |
|---|---|
| author | Berens, Michael E. Sood, Anup Barnholtz-Sloan, Jill S. Graf, John F. Cho, Sanghee Kim, Seungchan Kiefer, Jeffrey Byron, Sara A. Halperin, Rebecca F. Nasser, Sara Adkins, Jonathan Cuyugan, Lori Devine, Karen Ostrom, Quinn Couce, Marta Wolansky, Leo McDonough, Elizabeth Schyberg, Shannon Dinn, Sean Sloan, Andrew E. Prados, Michael Phillips, Joanna J. Nelson, Sarah J. Liang, Winnie S. Al-Kofahi, Yousef Rusu, Mirabela Zavodszky, Maria I. Ginty, Fiona |
| author_facet | Berens, Michael E. Sood, Anup Barnholtz-Sloan, Jill S. Graf, John F. Cho, Sanghee Kim, Seungchan Kiefer, Jeffrey Byron, Sara A. Halperin, Rebecca F. Nasser, Sara Adkins, Jonathan Cuyugan, Lori Devine, Karen Ostrom, Quinn Couce, Marta Wolansky, Leo McDonough, Elizabeth Schyberg, Shannon Dinn, Sean Sloan, Andrew E. Prados, Michael Phillips, Joanna J. Nelson, Sarah J. Liang, Winnie S. Al-Kofahi, Yousef Rusu, Mirabela Zavodszky, Maria I. Ginty, Fiona |
| author_sort | Berens, Michael E. |
| collection | PubMed |
| description | Glioma is recognized to be a highly heterogeneous CNS malignancy, whose diverse cellular composition and cellular interactions have not been well characterized. To gain new clinical- and biological-insights into the genetically-bifurcated IDH1 mutant (mt) vs wildtype (wt) forms of glioma, we integrated data from protein, genomic and MR imaging from 20 treatment-naïve glioma cases and 16 recurrent GBM cases. Multiplexed immunofluorescence (MxIF) was used to generate single cell data for 43 protein markers representing all cancer hallmarks, Genomic sequencing (exome and RNA (normal and tumor) and magnetic resonance imaging (MRI) quantitative features (protocols were T1-post, FLAIR and ADC) from whole tumor, peritumoral edema and enhancing core vs equivalent normal region were also collected from patients. Based on MxIF analysis, 85,767 cells (glioma cases) and 56,304 cells (GBM cases) were used to generate cell-level data for 24 biomarkers. K-means clustering was used to generate 7 distinct groups of cells with divergent biomarker profiles and deconvolution was used to assign RNA data into three classes. Spatial and molecular heterogeneity metrics were generated for the cell data. All features were compared between IDH mt and IDHwt patients and were finally combined to provide a holistic/integrated comparison. Protein expression by hallmark was generally lower in the IDHmt vs wt patients. Molecular and spatial heterogeneity scores for angiogenesis and cell invasion also differed between IDHmt and wt gliomas irrespective of prior treatment and tumor grade; these differences also persisted in the MR imaging features of peritumoral edema and contrast enhancement volumes. A coherent picture of enhanced angiogenesis in IDHwt tumors was derived from multiple platforms (genomic, proteomic and imaging) and scales from individual proteins to cell clusters and heterogeneity, as well as bulk tumor RNA and imaging features. Longer overall survival for IDH1mt glioma patients may reflect mutation-driven alterations in cellular, molecular, and spatial heterogeneity which manifest in discernable radiological manifestations. |
| format | Online Article Text |
| id | pubmed-6934292 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2019 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-69342922020-01-07 Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas Berens, Michael E. Sood, Anup Barnholtz-Sloan, Jill S. Graf, John F. Cho, Sanghee Kim, Seungchan Kiefer, Jeffrey Byron, Sara A. Halperin, Rebecca F. Nasser, Sara Adkins, Jonathan Cuyugan, Lori Devine, Karen Ostrom, Quinn Couce, Marta Wolansky, Leo McDonough, Elizabeth Schyberg, Shannon Dinn, Sean Sloan, Andrew E. Prados, Michael Phillips, Joanna J. Nelson, Sarah J. Liang, Winnie S. Al-Kofahi, Yousef Rusu, Mirabela Zavodszky, Maria I. Ginty, Fiona PLoS One Research Article Glioma is recognized to be a highly heterogeneous CNS malignancy, whose diverse cellular composition and cellular interactions have not been well characterized. To gain new clinical- and biological-insights into the genetically-bifurcated IDH1 mutant (mt) vs wildtype (wt) forms of glioma, we integrated data from protein, genomic and MR imaging from 20 treatment-naïve glioma cases and 16 recurrent GBM cases. Multiplexed immunofluorescence (MxIF) was used to generate single cell data for 43 protein markers representing all cancer hallmarks, Genomic sequencing (exome and RNA (normal and tumor) and magnetic resonance imaging (MRI) quantitative features (protocols were T1-post, FLAIR and ADC) from whole tumor, peritumoral edema and enhancing core vs equivalent normal region were also collected from patients. Based on MxIF analysis, 85,767 cells (glioma cases) and 56,304 cells (GBM cases) were used to generate cell-level data for 24 biomarkers. K-means clustering was used to generate 7 distinct groups of cells with divergent biomarker profiles and deconvolution was used to assign RNA data into three classes. Spatial and molecular heterogeneity metrics were generated for the cell data. All features were compared between IDH mt and IDHwt patients and were finally combined to provide a holistic/integrated comparison. Protein expression by hallmark was generally lower in the IDHmt vs wt patients. Molecular and spatial heterogeneity scores for angiogenesis and cell invasion also differed between IDHmt and wt gliomas irrespective of prior treatment and tumor grade; these differences also persisted in the MR imaging features of peritumoral edema and contrast enhancement volumes. A coherent picture of enhanced angiogenesis in IDHwt tumors was derived from multiple platforms (genomic, proteomic and imaging) and scales from individual proteins to cell clusters and heterogeneity, as well as bulk tumor RNA and imaging features. Longer overall survival for IDH1mt glioma patients may reflect mutation-driven alterations in cellular, molecular, and spatial heterogeneity which manifest in discernable radiological manifestations. Public Library of Science 2019-12-27 /pmc/articles/PMC6934292/ /pubmed/31881020 http://dx.doi.org/10.1371/journal.pone.0219724 Text en © 2019 Berens et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Article Berens, Michael E. Sood, Anup Barnholtz-Sloan, Jill S. Graf, John F. Cho, Sanghee Kim, Seungchan Kiefer, Jeffrey Byron, Sara A. Halperin, Rebecca F. Nasser, Sara Adkins, Jonathan Cuyugan, Lori Devine, Karen Ostrom, Quinn Couce, Marta Wolansky, Leo McDonough, Elizabeth Schyberg, Shannon Dinn, Sean Sloan, Andrew E. Prados, Michael Phillips, Joanna J. Nelson, Sarah J. Liang, Winnie S. Al-Kofahi, Yousef Rusu, Mirabela Zavodszky, Maria I. Ginty, Fiona Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title | Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title_full | Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title_fullStr | Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title_full_unstemmed | Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title_short | Multiscale, multimodal analysis of tumor heterogeneity in IDH1 mutant vs wild-type diffuse gliomas |
| title_sort | multiscale, multimodal analysis of tumor heterogeneity in idh1 mutant vs wild-type diffuse gliomas |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6934292/ https://www.ncbi.nlm.nih.gov/pubmed/31881020 http://dx.doi.org/10.1371/journal.pone.0219724 |
| work_keys_str_mv | AT berensmichaele multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT soodanup multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT barnholtzsloanjills multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT grafjohnf multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT chosanghee multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT kimseungchan multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT kieferjeffrey multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT byronsaraa multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT halperinrebeccaf multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT nassersara multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT adkinsjonathan multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT cuyuganlori multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT devinekaren multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT ostromquinn multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT coucemarta multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT wolanskyleo multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT mcdonoughelizabeth multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT schybergshannon multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT dinnsean multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT sloanandrewe multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT pradosmichael multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT phillipsjoannaj multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT nelsonsarahj multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT liangwinnies multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT alkofahiyousef multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT rusumirabela multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT zavodszkymariai multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas AT gintyfiona multiscalemultimodalanalysisoftumorheterogeneityinidh1mutantvswildtypediffusegliomas |