Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior
Osteosarcoma (OS) is a heterogeneous and rare disease with a disproportionate impact because it mainly affects children and adolescents. Lamentably, more than half of patients with OS succumb to metastatic disease. Clarification of the etiology of the disease, development of better strategies to man...
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2016-12-01
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doaj-08fa8389824b4a929503584dbe5960032020-11-24T21:46:25ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112016-12-019121435144410.1242/dmm.026849026849Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behaviorMilcah C. Scott0Hirotaka Tomiyasu1John R. Garbe2Ingrid Cornax3Clarissa Amaya4M. Gerard O'Sullivan5Subbaya Subramanian6Brad A. Bryan7Jaime F. Modiano8 Animal Cancer Care and Research Program, University of Minnesota, St Paul, MN 55108, USA Animal Cancer Care and Research Program, University of Minnesota, St Paul, MN 55108, USA Minnesota Supercomputing Institute, University of Minnesota, Minneapolis, MN 55455, USA Masonic Cancer Center, University of Minnesota, Minneapolis, MN 55455, USA Department of Biomedical Sciences, Center of Emphasis in Cancer Research at the Paul Foster School of Medicine, Texas Tech University Health Sciences Center, El Paso, TX 79905, USA Animal Cancer Care and Research Program, University of Minnesota, St Paul, MN 55108, USA Animal Cancer Care and Research Program, University of Minnesota, St Paul, MN 55108, USA Department of Biomedical Sciences, Center of Emphasis in Cancer Research at the Paul Foster School of Medicine, Texas Tech University Health Sciences Center, El Paso, TX 79905, USA Animal Cancer Care and Research Program, University of Minnesota, St Paul, MN 55108, USA Osteosarcoma (OS) is a heterogeneous and rare disease with a disproportionate impact because it mainly affects children and adolescents. Lamentably, more than half of patients with OS succumb to metastatic disease. Clarification of the etiology of the disease, development of better strategies to manage progression, and methods to guide personalized treatments are among the unmet health needs for OS patients. Progress in managing the disease has been hindered by the extreme heterogeneity of OS; thus, better models that accurately recapitulate the natural heterogeneity of the disease are needed. For this study, we used cell lines derived from two spontaneous canine OS tumors with distinctly different biological behavior (OS-1 and OS-2) for heterotypic in vivo modeling that recapitulates the heterogeneous biology and behavior of this disease. Both cell lines demonstrated stability of the transcriptome when grown as orthotopic xenografts in athymic nude mice. Consistent with the behavior of the original tumors, OS-2 xenografts grew more rapidly at the primary site and had greater propensity to disseminate to lung and establish microscopic metastasis. Moreover, OS-2 promoted formation of a different tumor-associated stromal environment than OS-1 xenografts. OS-2-derived tumors comprised a larger percentage of the xenograft tumors than OS-1-derived tumors. In addition, a robust pro-inflammatory population dominated the stromal cell infiltrates in OS-2 xenografts, whereas a mesenchymal population with a gene signature reflecting myogenic signaling dominated those in the OS-1 xenografts. Our studies show that canine OS cell lines maintain intrinsic features of the tumors from which they were derived and recapitulate the heterogeneous biology and behavior of bone cancer in mouse models. This system provides a resource to understand essential interactions between tumor cells and the stromal environment that drive the progression and metastatic propensity of OS.http://dmm.biologists.org/content/9/12/1435OsteosarcomaMetastasisHeterotypic modelsXenograftComparative studiesTumor–stromal interactions |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Milcah C. Scott Hirotaka Tomiyasu John R. Garbe Ingrid Cornax Clarissa Amaya M. Gerard O'Sullivan Subbaya Subramanian Brad A. Bryan Jaime F. Modiano |
spellingShingle |
Milcah C. Scott Hirotaka Tomiyasu John R. Garbe Ingrid Cornax Clarissa Amaya M. Gerard O'Sullivan Subbaya Subramanian Brad A. Bryan Jaime F. Modiano Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior Disease Models & Mechanisms Osteosarcoma Metastasis Heterotypic models Xenograft Comparative studies Tumor–stromal interactions |
author_facet |
Milcah C. Scott Hirotaka Tomiyasu John R. Garbe Ingrid Cornax Clarissa Amaya M. Gerard O'Sullivan Subbaya Subramanian Brad A. Bryan Jaime F. Modiano |
author_sort |
Milcah C. Scott |
title |
Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
title_short |
Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
title_full |
Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
title_fullStr |
Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
title_full_unstemmed |
Heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
title_sort |
heterotypic mouse models of canine osteosarcoma recapitulate tumor heterogeneity and biological behavior |
publisher |
The Company of Biologists |
series |
Disease Models & Mechanisms |
issn |
1754-8403 1754-8411 |
publishDate |
2016-12-01 |
description |
Osteosarcoma (OS) is a heterogeneous and rare disease with a disproportionate impact because it mainly affects children and adolescents. Lamentably, more than half of patients with OS succumb to metastatic disease. Clarification of the etiology of the disease, development of better strategies to manage progression, and methods to guide personalized treatments are among the unmet health needs for OS patients. Progress in managing the disease has been hindered by the extreme heterogeneity of OS; thus, better models that accurately recapitulate the natural heterogeneity of the disease are needed. For this study, we used cell lines derived from two spontaneous canine OS tumors with distinctly different biological behavior (OS-1 and OS-2) for heterotypic in vivo modeling that recapitulates the heterogeneous biology and behavior of this disease. Both cell lines demonstrated stability of the transcriptome when grown as orthotopic xenografts in athymic nude mice. Consistent with the behavior of the original tumors, OS-2 xenografts grew more rapidly at the primary site and had greater propensity to disseminate to lung and establish microscopic metastasis. Moreover, OS-2 promoted formation of a different tumor-associated stromal environment than OS-1 xenografts. OS-2-derived tumors comprised a larger percentage of the xenograft tumors than OS-1-derived tumors. In addition, a robust pro-inflammatory population dominated the stromal cell infiltrates in OS-2 xenografts, whereas a mesenchymal population with a gene signature reflecting myogenic signaling dominated those in the OS-1 xenografts. Our studies show that canine OS cell lines maintain intrinsic features of the tumors from which they were derived and recapitulate the heterogeneous biology and behavior of bone cancer in mouse models. This system provides a resource to understand essential interactions between tumor cells and the stromal environment that drive the progression and metastatic propensity of OS. |
topic |
Osteosarcoma Metastasis Heterotypic models Xenograft Comparative studies Tumor–stromal interactions |
url |
http://dmm.biologists.org/content/9/12/1435 |
work_keys_str_mv |
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