The adrenergic receptor antagonists propranolol and carvedilol decrease bone sarcoma cell viability and sustained carvedilol reduces clonogenic survival and increases radiosensitivity in canine osteosarcoma cells

Duckett, Megan M.; Phung, Shee Kwan; Linh-Trung, Nguyen; Khammanivong, Ali; Dickerson, Erin B.; Dusenbery, Kathryn E.; Lawrence, Jessica

doi:10.1111/vco.12560

Cited by 11 publications

(15 citation statements)

References 88 publications

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“…Increased antitumor activity as a result of combining PPN with cytotoxic agents was previously reported in non-OSA preclinical and clinical studies, in which addition of repurposed drug to paclitaxel-, 5-FU-or even CDDP-based chemotherapy increased antiangiogenic and antiproliferative effects of monotherapies, as well as decreased distant metastases in patients [30,37,38]. Moreover, it was recently reported that β-blockade in different bone sarcoma models, increases sensitivity to radiotherapy, especially in canine OSA [24]. In our in vivo protocol sustained treatment with PPN, alone and especially in addition to CDDP, caused a marked decrease in OSA tumor progression, showing that PPN may complement chemotherapy, increasing its effectiveness without overt toxicity.…”

Section: Discussionmentioning

confidence: 81%

“…As recently reported, expression of β-ARs and several catecholamines, including norepinephrine, was signi cantly higher in OSA in comparison to healthy bone [21]. In addition, all subtypes of β-AR were found to be expressed in a wide collection of human and canine OSA or other bone sarcoma models [22][23][24], making the exploration of non-selective β-blocker PPN in OSA an appealing niche for further studies. Considering the unsatis ed clinical needs of OSA and the multiple reported bene ts of PPN as a broad antitumor agent, the aim of the present study was to evaluate the in vitro/in vivo antitumoral activity of PPN in OSA, as a monotherapy or in combination with metronomic chemotherapy.…”

Section: Introductionmentioning

confidence: 66%

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Drug Repurposing of β-blocker Propranolol in Osteosarcoma: Preclinical Antitumor Efficacy Alone or in Combination with Chemotherapy.

Solernó¹,

Sobol²,

Capobianco³

et al. 2020

Preprint

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Background: Osteosarcoma is still associated with poor response to therapy and alarmingly elevated mortality rates, especially in developing countries, highlighting the urgent need of novel therapeutic strategies. Given that β-adrenergic receptor (β-AR) signaling regulates many cellular processes involved in the initiation and progression of cancer, multiple efforts have been made to repurpose non-selective β-blocker propranolol in oncology. Considering the unsatisfied clinical needs of osteosarcoma, we evaluated the in vitro and in vivo antitumoral activity of propranolol as a monotherapy or in combination with metronomic chemotherapy, in β-AR-expressing human osteosarcoma cells. Methods: In vitro anti-osteosarcoma effects of propranolol were assessed on high-density cell growth, chemotaxis, colony-forming ability and three-dimensional spheroids. Cell cycle phase distribution and apoptosis were evaluated using flow cytometry analysis, and quantification of hypodiploid cell population and TUNEL labelling, respectively. Propranolol addition to chemotherapy was evaluated in vitro and in human osteosarcoma xenografts generated in athymic mice.Results: Propranolol significantly impaired MG-63 and U-2 OS cellular growth in a concentration range of 10-100 µM (IC50 ≈ 45µM) and was capable of blocking in vitro protumoral effects triggered by catecholamines. Cytostatic activity of propranolol was associated to reduced mitosis and G0/G1 cell cycle, but not to apoptosis induction. Moreover, β-blocker drastically reduced colony formation, spheroid progression and migration of osteosarcoma cells. Synergistic effects were observed in vitro after combining propranolol with chemotherapeutic agents methotrexate or cisplatin. In vivo, treatment with propranolol (10 mg/kg i.p.), alone and especially in addition to non-interrupted low-dose cisplatin (2 mg/kg i.p.), markedly abrogated xenograft progression, reducing tumor growth rates by 25 or 70%, respectively. After histological analysis, propranolol and cisplatin combined therapy resulted in low tumor mitotic index and increased tumor necrosis. Conclusions: Considering its robust antitumoral effects, β-AR antagonization using β-blocker propranolol seems to be an achievable and cost-effective therapeutic approach to modulate osteosarcoma aggressiveness, in addition to chemotherapy. Propranolol could be proposed as a co-adjuvant agent for the management of osteosarcoma, especially in low- and middle-income countries where access to treatment resources are limited. Further preclinical and clinical studies of propranolol repurposing in osteosarcoma are warranted.

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Section: Discussionmentioning

confidence: 81%

Section: Introductionmentioning

confidence: 66%

Drug Repurposing of β-blocker Propranolol in Osteosarcoma: Preclinical Antitumor Efficacy Alone or in Combination with Chemotherapy.

Solernó¹,

Sobol²,

Capobianco³

et al. 2020

Preprint

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“…Enhancement of antineoplastic activity as a result of combining PPN with cytotoxic agents was previously reported for other tumor types, in which addition of repurposed drug to chemotherapy increased antiangiogenic and antiproliferative effects of monotherapies, as well as decreased distant metastases in patients [57][58][59] . Moreover, it was recently reported that β-blockade increases sensitivity to radiotherapy in different bone sarcoma models, especially in canine OSA 17 . In our in vivo protocol, sustained treatment with PPN using validated human equivalent doses (10 mg/kg/day i.p.…”

Section: Discussionmentioning

confidence: 98%

“…Although sympathetic nervous system (SNS) activation and catecholamine-triggered signaling pathways are deeply involved in cancer initiation and growth 15 , little is known about the specific role of β-adrenergic signaling in OSA progression. Interestingly, expression of catecholamines and their receptors was previously reported in multiple human and canine OSA models 16,17 . Moreover, norepinephrine and β-adrenergic receptors were also detected in OSA clinical samples, showing increased expression levels in comparison to matched non-oncological healthy bone 18 , making the exploration of β-blocker PPN in OSA an appealing niche for further studies.…”

mentioning

confidence: 90%

Propranolol blocks osteosarcoma cell cycle progression, inhibits angiogenesis and slows xenograft growth in combination with cisplatin-based chemotherapy

Solernó

Sobol

Gottardo

et al. 2022

Sci Rep

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Osteosarcoma is still associated with limited response to standard-of-care therapy and alarmingly elevated mortality rates, especially in low- and middle-income countries. Despite multiple efforts to repurpose β-blocker propranolol in oncology, its potential application in osteosarcoma management remains largely unexplored. Considering the unsatisfied clinical needs of this aggressive disease, we evaluated the antitumoral activity of propranolol using different in vitro and in vivo osteosarcoma preclinical models, alone or in addition to chemotherapy. Propranolol significantly impaired cellular growth in β2-adrenergic receptor-expressing MG-63 and U-2OS cells, and was capable of blocking growth-stimulating effects triggered by catecholamines. siRNA-mediated ADRB2 knockdown in MG-63 cells was associated with decreased cell survival and a significant attenuation of PPN anti-osteosarcoma activity. Direct cytostatic effects of propranolol were independent of apoptosis induction and were associated with reduced mitosis, G0/G1 cell cycle arrest and a significant down-regulation of cell cycle regulator Cyclin D1. Moreover, colony formation, 3D spheroid growth, cell chemotaxis and capillary-like tube formation were drastically impaired after propranolol treatment. Interestingly, anti-migratory activity of β-blocker was associated with altered actin cytoskeleton dynamics. In vivo, propranolol treatment (10 mg/kg/day i.p.) reduced the early angiogenic response triggered by MG-63 cells in nude mice. Synergistic effects were observed in vitro after combining propranolol with chemotherapeutic agent cisplatin. Sustained administration of propranolol (10 mg/kg/day i.p., five days a week), alone and especially in addition to low-dose metronomic cisplatin (2 mg/kg/day i.p., three times a week), markedly reduced xenograft progression. After histological analysis, propranolol and cisplatin combination resulted in low tumor mitotic index and increased tumor necrosis. β-blockade using propranolol seems to be an achievable and cost-effective therapeutic approach to modulate osteosarcoma aggressiveness. Further translational studies of propranolol repurposing in osteosarcoma are warranted.

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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 .…”

mentioning

confidence: 99%

Editorial

Buracco

Rebhun

2020

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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The adrenergic receptor antagonists propranolol and carvedilol decrease bone sarcoma cell viability and sustained carvedilol reduces clonogenic survival and increases radiosensitivity in canine osteosarcoma cells

Cited by 11 publications

References 88 publications

Drug Repurposing of β-blocker Propranolol in Osteosarcoma: Preclinical Antitumor Efficacy Alone or in Combination with Chemotherapy.

Drug Repurposing of β-blocker Propranolol in Osteosarcoma: Preclinical Antitumor Efficacy Alone or in Combination with Chemotherapy.

Propranolol blocks osteosarcoma cell cycle progression, inhibits angiogenesis and slows xenograft growth in combination with cisplatin-based chemotherapy

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