FANCD2 Is a Potential Therapeutic Target and Biomarker in Alveolar Rhabdomyosarcoma Harboring the PAX3–FOXO1 Fusion Gene

Singh, Manorama; Leasure, Justin M.; Chronowski, Christopher; Geier, Brian; Bondra, Kathryn; Duan, Wenrui; Hensley, Lauren A.; Villalona‐Calero, Miguel A.; Li, Ning; Vergis, Anthony M.; Kurmasheva, Raushan T.; Shen, Changxian; Woods, Gary M.; Sebastian, Nikhil; Fabian, Denise; Kaplon, Rita; Hammond, Sue; Palanichamy, Kamalakannan; Chakravarti, Arnab; Houghton, Peter J.

doi:10.1158/1078-0432.ccr-13-0556

Cited by 11 publications

(15 citation statements)

References 26 publications

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“…4D). Using an index of skin toxicity previously reported, [40] there was a slight decrease in the cumulative toxicity in the combination treatment arm of this study compared to 10 Gy XRT alone (Fig. 4E).…”

Section: Resultssupporting

confidence: 59%

“…Inhibition of TORC1 has been associated with increased sensitivity to XRT, and it was considered that rapamycin‐induced G1 arrest could contribute to the sensitizing effects. We also showed that AZD8055 could enhance the effect of XRT, and that FANCD2 was regulated downstream of TORC1 in part by S6K1/2 activity . It was therefore of interest to determine whether selumetinib could enhance daily fractionated XRT.…”

Section: Resultsmentioning

confidence: 97%

“…We also showed that AZD8055 could enhance the effect of XRT, and that FANCD2 was regulated downstream of TORC1 in part by S6K1/2 activity. [27,40] It was therefore of interest to determine whether selumetinib could enhance daily fractionated XRT. In a pilot study to define the radiosensitivity of BT-40 xenografts, tumor-bearing mice were irradiated (2 Gy fractions) daily to a total dose of 10, 20, or 30 Gy, as previously described.…”

Section: Resultsmentioning

confidence: 99%

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Inhibition of MEK confers hypersensitivity to X-radiation in the context of BRAF mutation in a model of childhood astrocytoma

Studebaker

Bondra

Seum

et al. 2015

Pediatr Blood Cancer

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Purpose Curative therapy for childhood glioma presents challenges when complete resection is not possible. Patients with recurrent low-grade tumors or anaplastic astrocytoma may receive radiation treatment, however, the long-term sequellae from radiation treatment can be severe. As many childhood gliomas are associated with activation of BRAF, we have explored the combination of ionizing radiation with MEK inhibition in a model of BRAF-mutant anaplastic astrocytoma. Experimental Design The regulation of TORC1 signaling by BRAF was examined in BT-40 (BRAF mutant) and BT-35 (BRAF wild type) xenografts, in a cell line derived from the BT-40 xenograft and two adult BRAF mutant glioblastoma cell lines. The effect of MEK inhibition (selumetinib), XRT (total dose10 Gy as 2 Gy daily fractions), or the combination of selumetinib and XRT was evaluated in subcutaneous BT-40 xenografts. Results Inhibition of MEK signaling by selumetinib, suppressed TORC1 signaling only in the context of the BRAF-mutant both in vitro and in vivo. Inhibition of MEK signaling in BT-40 cells or in xenografts lead to a complete suppression of FANCD2 and conferred hypersensitivity to XRT in BT-40 xenografts without increasing local skin toxicity. Conclusions Selumetinib suppressed TORC1 signaling in the context of BRAF mutation. Selumetinib caused a rapid downregulation of FANCD2 and markedly potentiated the effect of XRT. These data suggest the possibility of potentiating the effect of XRT selectively in tumor cells by MEK inhibition in the context of mutant BRAF or maintaining tumor control at lower doses of XRT that would decrease long-term sequelae.

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Section: Resultssupporting

confidence: 59%

Section: Resultsmentioning

confidence: 97%

Section: Resultsmentioning

confidence: 99%

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Inhibition of MEK confers hypersensitivity to X-radiation in the context of BRAF mutation in a model of childhood astrocytoma

Studebaker

Bondra

Seum

et al. 2015

Pediatr Blood Cancer

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“…Recent preclinical data have shown that FANCD2 is a potential therapeutic target in fusion-positive alveolar rhabdomyosarcoma. In mouse models, FANCD2 may have a significant role in the radiation resistance of alveolar rhabdomyosarcoma, and offers a possibility for targeting this DNA repair protein through mTOR inhibition [ 7 ]. Targeting of the fusion protein is an area of active research from multiple directions; Jothi et al .…”

Section: Advances In Biologymentioning

confidence: 99%

Recent advances in understanding and managing rhabdomyosarcoma

Hiniker

Donaldson

2015

F1000Prime Rep

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Rhabdomyosarcoma is the most common childhood soft tissue sarcoma and the fourth most common pediatric solid tumor. For most patients, treatment consists of a multimodality approach, including chemotherapy, surgery, and/or radiotherapy. To guide treatment, patients with rhabdomyosarcoma are risk stratified based on a number of factors. These factors include clinical group, which depends largely on the extent of resection and nodal involvement, and stage, which takes into account tumor size, invasion, nodal involvement, and disease site. Histology of the tumor and age at diagnosis are also factored into risk stratification. Recent advances in understanding the biology of the disease have allowed for the further sub-classification of rhabdomyosarcoma. In addition, elucidation of additional clinical features associated with poor prognosis has allowed for better understanding of risk and provides more clarity regarding those patients who require more intensive therapy. Many areas of active investigation are ongoing, including the following: further delineation of the biological underpinnings of the various disease subtypes with the possibility of molecularly targeted therapy; a better understanding of clinical risk factors, including the evaluation and management of potentially involved lymph nodes; determination of the appropriate role of post-treatment imaging and assessment of response to therapy; and incorporation of advanced radiotherapeutic techniques, including conformal intensity-modulated photon and proton therapy.

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“…For instance, it may happen from lung cancer (3). Many biomarkers are assigned for rhabdomyosarcomas (4,5). The identification of the tumor major proteins can be helpful to better understand the muscle cancer mechanisms.…”

Section: Introductionmentioning

confidence: 99%

Towards understanding topological features of protein interactome map of muscle cancer

Okhovatian¹

2017

Arvand Journal of Health and Medical Sciences

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Muscle cancer despite being rare but it is important for more examination due to its high mortality risk. Here, applying protein-protein interaction PPI network, we analyzed proteins that are related to this neoplasm in more details. The String Database (db) as the source for network was used through Cytoscape 3.4. The centrality examination by Network Analyzer, Cytoscape plug-in is done. The findings indicate that there are some proteins with higher linkage to the disease and with central topological features. These hub-bottlenecks are TP53, AKT1, MYC, and KIT. The prioritized proteins in this analysis indicate that these molecules may have prominent role in interactome of muscle cancer; however, more investigation is required to establish this claim.

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FANCD2 Is a Potential Therapeutic Target and Biomarker in Alveolar Rhabdomyosarcoma Harboring the PAX3–FOXO1 Fusion Gene

Cited by 11 publications

References 26 publications

Inhibition of MEK confers hypersensitivity to X-radiation in the context of BRAF mutation in a model of childhood astrocytoma

Inhibition of MEK confers hypersensitivity to X-radiation in the context of BRAF mutation in a model of childhood astrocytoma

Recent advances in understanding and managing rhabdomyosarcoma

Towards understanding topological features of protein interactome map of muscle cancer

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