In vitro and in vivo effects of toceranib phosphate on canine osteosarcoma cell lines and xenograft orthotopic models

Sánchez-Céspedes, R.; Accornero, Paolo; Miretti, Silvia; Martignani, Eugenio; Gattino, Francesca; Maniscalco, Lorella; Gola, Cecilia; Iussich, Selina; Martano, Marina; Morello, Emanuela; Buracco, Paolo; Aresu, Luca; Maria, Raffaella De

doi:10.1111/vco.12562

Cited by 17 publications

(18 citation statements)

References 35 publications

(74 reference statements)

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“…Specifically, two commercial and six primary cOSA cell lines established and validated in our laboratory were analyzed. The assorted cell lines were previously used in several studies to investigate cOSA pathogenetic mechanisms and response to therapies (11,12,14,(36)(37)(38). So far, only the D17 cell line has been characterized at the genomic level by Das et al in 2019 (13).…”

Section: Discussionmentioning

confidence: 99%

Genomic and Transcriptomic Characterization of Canine Osteosarcoma Cell Lines: A Valuable Resource in Translational Medicine

et al. 2021

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Osteosarcoma (OSA) represents the most common primary bone tumor in dogs and is characterized by a highly aggressive behavior. Cell lines represent one of the most suitable and reproducible pre-clinical models, and therefore the knowledge of their molecular landscape is mandatory to investigate oncogenic mechanisms and drug response. The present study aims at determining variants, putative driver genes, and gene expression aberrations by integrating whole-exome and RNA sequencing. For this purpose, eight canine OSA cell lines and one matched pair of primary tumor and normal tissue were analyzed. Overall, cell lines revealed a mean tumor mutational burden of 9.6 mutations/Mb (range 3.9–16.8). Several known oncogenes and tumor suppressor genes, such as ALK, MYC, and MET, were prioritized as having a likely role in canine OSA. Mutations in eight genes, previously described as human OSA drivers and including TP53, PTCH1, MED12, and PI3KCA, were retrieved in our cell lines. When variants were cross-referenced with human OSA driver mutations, the E273K mutation of TP53 was identified in the Wall cell line and tumor sample. The transcriptome profiling detected two possible p53 inactivation mechanisms in the Wall cell line on the one hand, and in D17 and D22 on the other. Moreover, MET overexpression, potentially leading to MAPK/ERK pathway activation, was observed in D17 and D22 cell lines. In conclusion, our data provide the molecular characterization of a large number of canine OSA cell lines, allowing future investigations on potential therapeutic targets and associated biomarkers. Notably, the Wall cell line represents a valuable model to empower prospective in vitro studies both in human and in dogs, since the TP53 driver mutation was maintained during cell line establishment and was widely reported as a mutation hotspot in several human cancers.

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Section: Discussionmentioning

confidence: 99%

Genomic and Transcriptomic Characterization of Canine Osteosarcoma Cell Lines: A Valuable Resource in Translational Medicine

et al. 2021

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“…Furthermore, no significant correlation was observed between the expression of these molecules and survival or histological grading in canine OSA ( 105 ). Despite this, the significant relation of this axis with malignant features of canine OSA has been observed both in vivo and in vitro ( 111 ). In fact, treating OSA cells with Toracenib, a potent inhibitor of PDGFRs, has been shown to induce a decrease in cell growth, migration, motility, and colony formation, as well as a significant blunting of tumor growth and proliferation index in an orthotopic xenograft model ( 111 ).…”

Section: Endothelial Mediatorsmentioning

confidence: 99%

“…Despite this, the significant relation of this axis with malignant features of canine OSA has been observed both in vivo and in vitro ( 111 ). In fact, treating OSA cells with Toracenib, a potent inhibitor of PDGFRs, has been shown to induce a decrease in cell growth, migration, motility, and colony formation, as well as a significant blunting of tumor growth and proliferation index in an orthotopic xenograft model ( 111 ). These findings suggest that PDGF/PDGFR axis can represent a target therapy more than a diagnostic tool.…”

Section: Endothelial Mediatorsmentioning

confidence: 99%

An Update on Molecular Pathways Regulating Vasculogenic Mimicry in Human Osteosarcoma and Their Role in Canine Oncology

et al. 2021

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Canine tumors are valuable comparative models for human counterparts, especially to explore novel biomarkers and to understand pathways and processes involved in metastasis. Vasculogenic mimicry (VM) is a unique property of malignant cancer cells which promote metastasis. Thus, it represents an opportunity to investigate both the molecular mechanisms and the therapeutic targets of a crucial phenotypic malignant switch. Although this biological process has been largely investigated in different human cancer types, including osteosarcoma, it is still largely unknown in veterinary pathology, where it has been mainly explored in canine mammary tumors. The presence of VM in human osteosarcoma is associated with poor clinical outcome, reduced patient survival, and increased risk of metastasis and it shares the main pathways involved in other type of human tumors. This review illustrates the main findings concerning the VM process in human osteosarcoma, search for the related current knowledge in canine pathology and oncology, and potential involvement of multiple pathways in VM formation, in order to provide a basis for future investigations on VM in canine tumors.

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“…Included in this issue are reviews aimed at understanding the clinical and pathological course of sarcomas by refining histologic classification and improving or standardizing histologic margin assessment of sarcomas . Original research manuscripts investigating the basic biology of sarcoma cells include studies evaluating the effects of toceranib phosphate in vitro and in vivo and a potential role for adrenergic receptor antagonists in moderating radiosensitivity . Yet another manuscript builds on previous data and identifies the interaction between RUNX2 and core‐binding factor beta as a potential target in osteosarcoma cells .…”

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Vet Comparative Oncology

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The first issue of Veterinary and Comparative Oncology was published in March 2003. This inaugural issue outlined simple objectives that included "to provide a forum for the exchange of information among veterinary oncologists, laboratory scientists and clinical investigators concerned with the aetiology, basic biology, and clinical and pathological course of cancer in domestic animals and its diagnosis, treatment and prevention. We believe it is important that the Journal not be restricted to veterinary oncology, but rather to reflect the value of comparative studies. The shared benefits between man and the veterinary species in terms of fundamental and clinical studies are well recognized in other disciplines of medicine, and it is the aim of this journal to promote that same philosophy in comparative oncology." 1 It is with these original objectives in mind, 17 years later, that we set out to publish a special issue on "Sarcoma." Sarcomas represent a

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In vitro and in vivo effects of toceranib phosphate on canine osteosarcoma cell lines and xenograft orthotopic models

Cited by 17 publications

References 35 publications

Genomic and Transcriptomic Characterization of Canine Osteosarcoma Cell Lines: A Valuable Resource in Translational Medicine

Genomic and Transcriptomic Characterization of Canine Osteosarcoma Cell Lines: A Valuable Resource in Translational Medicine

An Update on Molecular Pathways Regulating Vasculogenic Mimicry in Human Osteosarcoma and Their Role in Canine Oncology

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