PHD3 Acts as Tumor Suppressor in Mouse Osteosarcoma and Influences Tumor Vascularization via PDGF-C Signaling

Egners, Antje; Rezaei, Maryam; Kuzmanov, Aleksandar; Poitz, David M.; Streichert, D.; Müller‐Reichert, Thomas; Wielockx, Ben; Breier, Georg

doi:10.3390/cancers10120496

Cited by 7 publications

(5 citation statements)

References 65 publications

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“…Possible targets for anti‐angiogenesis therapies include transcription factors or signal pathways that directly or indirectly affect VEGF, PDGF, fibroblast growth factor (FGF), hepatocyte growth factor, integrin, cyclooxygenase (COX‐2), metalloproteinases (MMP‐2, MMP‐9) and HIF‐1. 19 , 20 , 21 VEGF and its receptors (VEGFRs) are key mediators of angiogenesis in cancer.…”

Section: Tumour Angiogenesis In Osmentioning

confidence: 99%

Current research progress in targeted anti‐angiogenesis therapy for osteosarcoma

et al. 2021

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Osteosarcoma (OS) is the most common primary malignant bone tumour with a peak in incidence during adolescence. Delayed patient presentation and diagnosis is common with approximately 15% of OS patients presenting with metastatic disease at initial diagnosis. With the introduction of neoadjuvant chemotherapy in the 1970s, disease prognosis improved from 17% to 60%‐70% 5‐year survival, but outcomes have not significantly improved since then. Novel and innovative therapeutic strategies are urgently needed as an adjunct to conventional treatment modalities to improve outcomes for OS patients. Angiogenesis is crucial for tumour growth, metastasis and invasion, and its prevention will ultimately inhibit tumour growth and metastasis. Dysregulation of angiogenesis in bone microenvironment involving osteoblasts and osteoclasts might contribute to OS development. This review summarizes existing knowledge regarding pre‐clinical and developmental research of targeted anti‐angiogenic therapy for OS with the aim of highlighting the limitations associated with this application. Targeted anti‐angiogenic therapies include monoclonal antibody to VEGF (bevacizumab), tyrosine kinase inhibitors (Sorafenib, Apatinib, Pazopanib and Regorafenib) and human recombinant endostatin (Endostar). However, considering the safety and efficacy of these targeted anti‐angiogenesis therapies in clinical trials cannot be guaranteed at this point, further research is needed to completely understand and characterize targeted anti‐angiogenesis therapy in OS.

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Section: Tumour Angiogenesis In Osmentioning

confidence: 99%

Current research progress in targeted anti‐angiogenesis therapy for osteosarcoma

et al. 2021

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“…The details of all signaling pathway networks identified were also shown in Figures 6A-C (A: numbers of ligand receptors among all cell types; B: weights of ligand receptors among all cell types; C: chordal graph of ligand-receptor interactions among all cell types). Among the total of 57 signaling pathways, the following signaling pathways were related to osteosarcoma: COLLAGEN ( Baumann and Hennet, 2016 ; Elenjord et al, 2009 ; Levinson et al, 2002 ; Yamaguchi et al, 2005 ), CD99 ( Manara et al, 2006 ; Sciandra et al, 2014 ; Zucchini et al, 2014 ), PTN ( He et al, 2019 ; Qin et al, 2022 ; Sun et al, 2020 ), MIF( Liu et al, 2014 ), SPP1( Dalla-Torre et al, 2006 ; Li et al, 2017 ), FN1( Saba et al, 2019 ; Zhou et al, 2019 ), LAMININ( Heino and Massague, 1989 ), FGF ( Kurogi et al, 1996 ; Laulederkind et al, 2000 ; Li et al, 2019 ; Xu et al, 2010 ), VEGF ( Ji et al, 2020 ; Lei et al, 2018 ; Oda et al, 2006 ; Tsai et al, 2017 ; Zhang et al, 2019 ), GALECTIN( Gomez-Brouchet et al, 2010 ; Miao et al, 2014 ; Park et al, 2015 ; Zhou et al, 2014 ), PERIOSTIN( Ma et al, 2020 ; Xu et al, 2022 ), VISFATIN( Cheng et al, 2015 ; Wang et al, 2019 , 2016 ), ITGB2 ( Dai et al, 2018 ), NOTCH( Jin et al, 2017 ; Mu et al, 2013 ; Ongaro et al, 2016 ; Tanaka et al, 2009 ; Zhang et al, 2010 ), IGF ( Armakolas et al, 2016 ; Giatagana et al, 2022 ; Gvozdenovic et al, 2017 ; Molina et al, 2019 ; Tan et al, 2015 ), VWF( Wang et al, 2020 ), and PDGF ( Chen et al, 2009 ; Egners et al, 2018 ; Heldin et al, 1986 ). The ligand-receptor interact...…”

Section: Resultsmentioning

confidence: 99%

Comprehensive analysis of potential cellular communication networks in advanced osteosarcoma using single-cell RNA sequencing data

Wang

et al. 2022

Front. Genet.

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Osteosarcoma (OS) is a common bone cancer in children and adolescents, and metastasis and recurrence are the major causes of poor treatment outcomes. A better understanding of the tumor microenvironment is required to develop an effective treatment for OS. In this paper, a single-cell RNA sequencing dataset was taken to a systematic genetic analysis, and potential signaling pathways linked with osteosarcoma development were explored. Our findings revealed 25 clusters across 11 osteosarcoma tissues, with 11 cell types including “Chondroblastic cells”, “Osteoblastic cells”, “Myeloid cells”, “Pericytes”, “Fibroblasts”, “Proliferating osteoblastic cells”, “Osteoclasts”, “TILs”, “Endothelial cells”, “Mesenchymal stem cells”, and “Myoblasts”. The results of Cell communication analysis showed 17 potential cellular communication networks including “COLLAGEN signaling pathway network”, “CD99 signaling pathway network”, “PTN signaling pathway network”, “MIF signaling pathway network”, “SPP1 signaling pathway network”, “FN1 signaling pathway network”, “LAMININ signaling pathway network”, “FGF signaling pathway network”, “VEGF signaling pathway network”, “GALECTIN signaling pathway network”, “PERIOSTIN signaling pathway network”, “VISFATIN signaling pathway network”, “ITGB2 signaling pathway network”, “NOTCH signaling pathway network”, “IGF signaling pathway network”, “VWF signaling pathway network”, “PDGF signaling pathway network”. This research may provide novel insights into the pathophysiology of OS’s molecular processes.

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“…In gastric cancer, cell migration and invasion were significantly higher in PHD3-silenced tumor cells than controls, and both HIF1 and VEGF showed greater expression [141]. In mouse LM8 osteosarcoma, we showed that PHD3 is a tumor suppressor as silencing of this oxygen sensor led to enhanced tumor growth and dramatically changed vessel morphology that was directly related to significantly activated platelet-derived growth factor (PDGF)-C signaling in the vasculature of PHD3 knockdown tumors [142]. Thus, the impact of the PHDs in tumor progression is diverse and cell-dependent, i.e., tumor cell vs. TME.…”

Section: The Phd-hif Axis As a Central Regulator Of Tumor Developmentmentioning

confidence: 87%

Hif-Prolyl Hydroxylase Domain Proteins (Phds) in Cancer – Potential Targets for Anti-Tumor Therapy?

Gaete¹,

Rodríguez²,

Watts³

et al. 2020

Preprint

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Solid tumors are typically associated with unbridled proliferation of malignant cells, accompanied by an immature and dysfunctional tumor-associated vascular network. Consequent impairment in transport of nutrients and oxygen eventually leads to a hypoxic environment wherein cells must adapt to survive and overcome these stresses. Hypoxia inducible factors (HIFs) are central transcription factors in the hypoxia response and drive the expression of a vast number of survival genes in cancer cells and in cells in the tumor microenvironment. HIFs are tightly controlled by a class of oxygen sensors, the HIF-prolyl hydroxylase domain proteins (PHDs), which hydroxylate HIFs, thereby marking them for proteasomal degradation. Remarkable and intense research during the past decade has revealed that, contrary to expectations, PHDs are often overexpressed in many tumor types and that inhibition of PHDs can lead to decreased tumor growth, impaired metastasis and diminished tumor-associated immune-tolerance. Therefore, PHDs represent an attractive therapeutic target in cancer research. Multiple PHD inhibitors have been developed that have either been recently accepted in China as erythropoiesis stimulating agents (ESA) or are currently in phase III trials. We review here the function of HIFs and PHDs in cancer and related therapeutic opportunities.

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PHD3 Acts as Tumor Suppressor in Mouse Osteosarcoma and Influences Tumor Vascularization via PDGF-C Signaling

Cited by 7 publications

References 65 publications

Current research progress in targeted anti‐angiogenesis therapy for osteosarcoma

Current research progress in targeted anti‐angiogenesis therapy for osteosarcoma

Comprehensive analysis of potential cellular communication networks in advanced osteosarcoma using single-cell RNA sequencing data

Hif-Prolyl Hydroxylase Domain Proteins (Phds) in Cancer – Potential Targets for Anti-Tumor Therapy?

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