MS-275 (Entinostat) Promotes Radio-Sensitivity in PAX3-FOXO1 Rhabdomyosarcoma Cells

Cassandri, Matteo; Pomella, Silvia; Rossetti, Alessandra; Petragnano, Francesco; Milazzo, Luisa; Vulcano, Francesca; Camero, Simona; Codenotti, Silvia; Cicchetti, Francesca; Maggio, Roberto; Festuccia, Claudio; Gravina, Giovanni Luca; Fanzani, Alessandro; Megiorni, Francesca; Catanoso, Marialuigia; Marchese, Cinzia; Tombolini, Vincenzo; Locatelli, Franco; Rota, Rossella; Marampon, Francesco

doi:10.3390/ijms221910671

Cited by 16 publications

(23 citation statements)

References 84 publications

(130 reference statements)

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“…No preclinical and/or clinical data related to the use of directly targeting redox proteins drugs have been collected on RMS. However, several pieces of evidence suggest the use of drugs able to increase ROS beyond targeting redox proteins (137)(138)(139). On this regard, ROS generation has been identified as a mediator of histone deacetylase (HDAC) inhibitor (HDACi)-induced cell death (161), and the combination of HDACi with RT brings to RMS radiosensitization through increased ROS accumulation (137)(138)(139).…”

Section: Rt and Antioxidant Responsementioning

confidence: 99%

“…Ferroptosis, induced by excessive lipid peroxidation that leads to Fe 3+ accumulation-induced oxidative stress, is mediated by SLC11A2 and negatively regulated by GSH/GPx4 cascade (172). RMS is resistant to apoptosis (173) and necrosis (174), including from RT, as we have shown in preclinical in vitro and in vivo models (130, [137][138][139]175). The tumor suppressor p53, a master promoter of apoptosis (176) and programmed necrosis (177), is frequently mutated in ERMS (178) and downregulated in ARMS (179).…”

Section: Rt and Cell Death Autophagy And Senescencementioning

confidence: 99%

“…Thus, it seems unlikely that DNA-PKcs targeting will not lead to an RMS radiosensitization. Notably, several molecules have been identified as upstream regulators of DDR in RMS including ERKs ( 126 , 129 ), DNA methyltransferases 3A (DNMT3A) and DNMT3B ( 130 ), BET proteins ( 131 ), ephrin-A2 ( 132 ), caveolin-1 (CAV-1) ( 128 ), nuclear factor erythroid 2–related factor 2 (NRF-2) ( 133 ), c-Myc ( 116 ), SNAI2 ( 134 ), FAK ( 135 ), androgen receptor ( 136 ), and HDAC ( 137 – 139 ). Thus, another strategy to target DDR could be inhibiting these upstream molecules.…”

Section: Mechanisms Of Radioresistance In Rmsmentioning

confidence: 99%

“…Increasing oxidative stress has been shown to efficiently kill RMS ( 154 ). RMS antioxidant response is finely regulated by molecular epigenetic mechanisms ( 137 – 139 ), known to be critical regulator of adaptive responses to stress ( 155 , 156 ), including RT ( 157 ). Interestingly, the ability of RMS to detoxify from ROS increases in parallel with the acquisition of a more radioresistant phenotype ( 109 ), suggesting that, for these cells, ROS detoxification is critical to survive to radiation.…”

Section: Mechanisms Of Radioresistance In Rmsmentioning

confidence: 99%

“…Therefore, identifying the molecules and epigenetic reprogramming pathways used by cancer cells could lead to the development of promising targeted therapies able of weakening the different mechanisms of radioresistance, also in the context of RMS. Indeed, targeting specific DNMTs or HDACs has been demonstrated to reverse RMS phenotype, counteracting stemness and inducing radiosensitization ( 137 – 139 ). Specifically, our group has recently demonstrated the overexpression of DNMT3A and DNMT3B in ERMS primary tumor biopsies ( 251 ) and highlighted the synergic impact of DNMT3A or DNMT3B silencing and irradiation on viability and aggressiveness of RMS cells, suggesting that DNMT inhibitors could have a clinical application in combination with standard RT in the clinical management of patients with RMS.…”

Section: Mechanisms Of Radioresistance In Rmsmentioning

confidence: 99%

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Radioresistance in rhabdomyosarcomas: Much more than a question of dose

Camero

Cassandri²,

Pomella³

et al. 2022

Front. Oncol.

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Management of rhabdomyosarcoma (RMS), the most common soft tissue sarcoma in children, frequently accounting the genitourinary tract is complex and requires a multimodal therapy. In particular, as a consequence of the advancement in dose conformity technology, radiation therapy (RT) has now become the standard therapeutic option for patients with RMS. In the clinical practice, dose and timing of RT are adjusted on the basis of patients’ risk stratification to reduce late toxicity and side effects on normal tissues. However, despite the substantial improvement in cure rates, local failure and recurrence frequently occur. In this review, we summarize the general principles of the treatment of RMS, focusing on RT, and the main molecular pathways and specific proteins involved into radioresistance in RMS tumors. Specifically, we focused on DNA damage/repair, reactive oxygen species, cancer stem cells, and epigenetic modifications that have been reported in the context of RMS neoplasia in both in vitro and in vivo studies. The precise elucidation of the radioresistance-related molecular mechanisms is of pivotal importance to set up new more effective and tolerable combined therapeutic approaches that can radiosensitize cancer cells to finally ameliorate the overall survival of patients with RMS, especially for the most aggressive subtypes.

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