A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models

Pascal O. Zinn; Sanjay K. Singh; Aikaterini Kotrotsou; Islam Hassan; Ginu Thomas; Markus M. Luedi; Ahmed Elakkad; Nabil Elshafeey; Tagwa Idris; Jennifer Mosley; Joy Gumin; Gregory N. Fuller; John F. De Groot; Veera Baladandayuthapani; Erik P. Sulman; Ashok J. Kumar; Raymond Sawaya; Frederick F. Lang; David Piwnica-Worms; Rivka R. Colen

doi:10.1158/1078-0432.CCR-17-3420

A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models

Pascal O. Zinn, Sanjay K. Singh, Aikaterini Kotrotsou, Islam Hassan, Ginu Thomas, Markus M. Luedi, Ahmed Elakkad, Nabil Elshafeey, Tagwa Idris, Jennifer Mosley, Joy Gumin, Gregory N. Fuller, John F. De Groot, Veera Baladandayuthapani, Erik P. Sulman, Ashok J. Kumar, Raymond Sawaya, Frederick F. Lang, David Piwnica-Worms, Rivka R. Colen

Research output: Contribution to journal › Article › peer-review

73 Scopus citations

Abstract

Purpose: Radiomics is the extraction of multidimensional imaging features, which when correlated with genomics, is termed radiogenomics. However, radiogenomic biological validation is not sufficiently described in the literature. We seek to establish causality between differential gene expression status and MRI-extracted radiomic-features in glioblastoma. Experimental Design: Radiogenomic predictions and validation were done using the Cancer Genome Atlas and Repository of Molecular Brain Neoplasia Data glioblastoma patients (n ¼ 93) and orthotopic xenografts (OX; n ¼ 40). Tumor phenotypes were segmented, and radiomic-features extracted using the developed radiome-sequencing pipeline. Patients and animals were dichotomized on the basis of Periostin (POSTN) expression levels. RNA and protein levels confirmed RNAi-mediated POSTN knockdown in OX. Total RNA of tumor cells isolated from mouse brains (knockdown and control) was used for microarray-based expression profiling. Radiomic-features were utilized to predict POSTN expression status in patient, mouse, and interspecies. Results: Our robust pipeline consists of segmentation, radiomic-feature extraction, feature normalization/selection, and predictive modeling. The combination of skull stripping, brain-tissue focused normalization, and patient-specific normalization are unique to this study, providing comparable cross-platform, cross-institution radiomic features. POSTN expression status was not associated with qualitative or volumetric MRI parameters. Radiomic features significantly predicted POSTN expression status in patients (AUC: 76.56%; sensitivity/specificity: 73.91/78.26%) and OX (AUC: 92.26%; sensitivity/specificity: 92.86%/91.67%). Furthermore, radiomic features in OX were significantly associated with patients with similar POSTN expression levels (AUC: 93.36%; sensitivity/specificity: 82.61%/95.74%; P ¼ 02.021E15). Conclusions: We determined causality between radiomic texture features and POSTN expression levels in a preclinical model with clinical validation. Our biologically validated radiomic pipeline also showed the potential application for human–mouse matched coclinical trials.

Original language	English (US)
Pages (from-to)	6288-6299
Number of pages	12
Journal	Clinical Cancer Research
Volume	24
Issue number	24
DOIs	https://doi.org/10.1158/1078-0432.CCR-17-3420
State	Published - Dec 15 2018

ASJC Scopus subject areas

Oncology
Cancer Research

MD Anderson CCSG core facilities

Biostatistics Resource Group

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10.1158/1078-0432.CCR-17-3420

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Zinn, P. O., Singh, S. K., Kotrotsou, A., Hassan, I., Thomas, G., Luedi, M. M., Elakkad, A., Elshafeey, N., Idris, T., Mosley, J., Gumin, J., Fuller, G. N., De Groot, J. F., Baladandayuthapani, V., Sulman, E. P., Kumar, A. J., Sawaya, R., Lang, F. F., Piwnica-Worms, D., & Colen, R. R. (2018). A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models. Clinical Cancer Research, 24(24), 6288-6299. https://doi.org/10.1158/1078-0432.CCR-17-3420

A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models. / Zinn, Pascal O.; Singh, Sanjay K.; Kotrotsou, Aikaterini et al.
In: Clinical Cancer Research, Vol. 24, No. 24, 15.12.2018, p. 6288-6299.

Research output: Contribution to journal › Article › peer-review

Zinn, PO, Singh, SK, Kotrotsou, A, Hassan, I, Thomas, G, Luedi, MM, Elakkad, A, Elshafeey, N, Idris, T, Mosley, J, Gumin, J, Fuller, GN, De Groot, JF, Baladandayuthapani, V, Sulman, EP, Kumar, AJ, Sawaya, R, Lang, FF , Piwnica-Worms, D & Colen, RR 2018, 'A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models', Clinical Cancer Research, vol. 24, no. 24, pp. 6288-6299. https://doi.org/10.1158/1078-0432.CCR-17-3420

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title = "A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models",

abstract = "Purpose: Radiomics is the extraction of multidimensional imaging features, which when correlated with genomics, is termed radiogenomics. However, radiogenomic biological validation is not sufficiently described in the literature. We seek to establish causality between differential gene expression status and MRI-extracted radiomic-features in glioblastoma. Experimental Design: Radiogenomic predictions and validation were done using the Cancer Genome Atlas and Repository of Molecular Brain Neoplasia Data glioblastoma patients (n ¼ 93) and orthotopic xenografts (OX; n ¼ 40). Tumor phenotypes were segmented, and radiomic-features extracted using the developed radiome-sequencing pipeline. Patients and animals were dichotomized on the basis of Periostin (POSTN) expression levels. RNA and protein levels confirmed RNAi-mediated POSTN knockdown in OX. Total RNA of tumor cells isolated from mouse brains (knockdown and control) was used for microarray-based expression profiling. Radiomic-features were utilized to predict POSTN expression status in patient, mouse, and interspecies. Results: Our robust pipeline consists of segmentation, radiomic-feature extraction, feature normalization/selection, and predictive modeling. The combination of skull stripping, brain-tissue focused normalization, and patient-specific normalization are unique to this study, providing comparable cross-platform, cross-institution radiomic features. POSTN expression status was not associated with qualitative or volumetric MRI parameters. Radiomic features significantly predicted POSTN expression status in patients (AUC: 76.56%; sensitivity/specificity: 73.91/78.26%) and OX (AUC: 92.26%; sensitivity/specificity: 92.86%/91.67%). Furthermore, radiomic features in OX were significantly associated with patients with similar POSTN expression levels (AUC: 93.36%; sensitivity/specificity: 82.61%/95.74%; P ¼ 02.021E15). Conclusions: We determined causality between radiomic texture features and POSTN expression levels in a preclinical model with clinical validation. Our biologically validated radiomic pipeline also showed the potential application for human–mouse matched coclinical trials.",

author = "Zinn, {Pascal O.} and Singh, {Sanjay K.} and Aikaterini Kotrotsou and Islam Hassan and Ginu Thomas and Luedi, {Markus M.} and Ahmed Elakkad and Nabil Elshafeey and Tagwa Idris and Jennifer Mosley and Joy Gumin and Fuller, {Gregory N.} and {De Groot}, {John F.} and Veera Baladandayuthapani and Sulman, {Erik P.} and Kumar, {Ashok J.} and Raymond Sawaya and Lang, {Frederick F.} and David Piwnica-Worms and Colen, {Rivka R.}",

note = "Publisher Copyright: {\textcopyright} 2018 American Association for Cancer Research.",

year = "2018",

month = dec,

day = "15",

doi = "10.1158/1078-0432.CCR-17-3420",

language = "English (US)",

volume = "24",

pages = "6288--6299",

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TY - JOUR

T1 - A coclinical radiogenomic validation study

T2 - Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models

AU - Zinn, Pascal O.

AU - Singh, Sanjay K.

AU - Kotrotsou, Aikaterini

AU - Hassan, Islam

AU - Thomas, Ginu

AU - Luedi, Markus M.

AU - Elakkad, Ahmed

AU - Elshafeey, Nabil

AU - Idris, Tagwa

AU - Mosley, Jennifer

AU - Gumin, Joy

AU - Fuller, Gregory N.

AU - De Groot, John F.

AU - Baladandayuthapani, Veera

AU - Sulman, Erik P.

AU - Kumar, Ashok J.

AU - Sawaya, Raymond

AU - Lang, Frederick F.

AU - Piwnica-Worms, David

AU - Colen, Rivka R.

PY - 2018/12/15

Y1 - 2018/12/15

N2 - Purpose: Radiomics is the extraction of multidimensional imaging features, which when correlated with genomics, is termed radiogenomics. However, radiogenomic biological validation is not sufficiently described in the literature. We seek to establish causality between differential gene expression status and MRI-extracted radiomic-features in glioblastoma. Experimental Design: Radiogenomic predictions and validation were done using the Cancer Genome Atlas and Repository of Molecular Brain Neoplasia Data glioblastoma patients (n ¼ 93) and orthotopic xenografts (OX; n ¼ 40). Tumor phenotypes were segmented, and radiomic-features extracted using the developed radiome-sequencing pipeline. Patients and animals were dichotomized on the basis of Periostin (POSTN) expression levels. RNA and protein levels confirmed RNAi-mediated POSTN knockdown in OX. Total RNA of tumor cells isolated from mouse brains (knockdown and control) was used for microarray-based expression profiling. Radiomic-features were utilized to predict POSTN expression status in patient, mouse, and interspecies. Results: Our robust pipeline consists of segmentation, radiomic-feature extraction, feature normalization/selection, and predictive modeling. The combination of skull stripping, brain-tissue focused normalization, and patient-specific normalization are unique to this study, providing comparable cross-platform, cross-institution radiomic features. POSTN expression status was not associated with qualitative or volumetric MRI parameters. Radiomic features significantly predicted POSTN expression status in patients (AUC: 76.56%; sensitivity/specificity: 73.91/78.26%) and OX (AUC: 92.26%; sensitivity/specificity: 92.86%/91.67%). Furthermore, radiomic features in OX were significantly associated with patients with similar POSTN expression levels (AUC: 93.36%; sensitivity/specificity: 82.61%/95.74%; P ¼ 02.021E15). Conclusions: We determined causality between radiomic texture features and POSTN expression levels in a preclinical model with clinical validation. Our biologically validated radiomic pipeline also showed the potential application for human–mouse matched coclinical trials.

AB - Purpose: Radiomics is the extraction of multidimensional imaging features, which when correlated with genomics, is termed radiogenomics. However, radiogenomic biological validation is not sufficiently described in the literature. We seek to establish causality between differential gene expression status and MRI-extracted radiomic-features in glioblastoma. Experimental Design: Radiogenomic predictions and validation were done using the Cancer Genome Atlas and Repository of Molecular Brain Neoplasia Data glioblastoma patients (n ¼ 93) and orthotopic xenografts (OX; n ¼ 40). Tumor phenotypes were segmented, and radiomic-features extracted using the developed radiome-sequencing pipeline. Patients and animals were dichotomized on the basis of Periostin (POSTN) expression levels. RNA and protein levels confirmed RNAi-mediated POSTN knockdown in OX. Total RNA of tumor cells isolated from mouse brains (knockdown and control) was used for microarray-based expression profiling. Radiomic-features were utilized to predict POSTN expression status in patient, mouse, and interspecies. Results: Our robust pipeline consists of segmentation, radiomic-feature extraction, feature normalization/selection, and predictive modeling. The combination of skull stripping, brain-tissue focused normalization, and patient-specific normalization are unique to this study, providing comparable cross-platform, cross-institution radiomic features. POSTN expression status was not associated with qualitative or volumetric MRI parameters. Radiomic features significantly predicted POSTN expression status in patients (AUC: 76.56%; sensitivity/specificity: 73.91/78.26%) and OX (AUC: 92.26%; sensitivity/specificity: 92.86%/91.67%). Furthermore, radiomic features in OX were significantly associated with patients with similar POSTN expression levels (AUC: 93.36%; sensitivity/specificity: 82.61%/95.74%; P ¼ 02.021E15). Conclusions: We determined causality between radiomic texture features and POSTN expression levels in a preclinical model with clinical validation. Our biologically validated radiomic pipeline also showed the potential application for human–mouse matched coclinical trials.

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A coclinical radiogenomic validation study: Conserved magnetic resonance radiomic appearance of periostin-expressing glioblastoma in patients and xenograft models

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ASJC Scopus subject areas

MD Anderson CCSG core facilities

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