Interferon-α2a and 13-cis-retinoic acid with radiation
treatment for high-grade glioma

Dillman, Robert O.; Shea, William M.; Tai, D. F.; Mahdavi, Khosrow; Barth, Neil M.; Kharkar, Bharati R.; Poor, Marshall M.; Church, Curtis K.; DePriest, Carol

doi:10.1093/neuonc/3.1.35

Cited by 24 publications

(7 citation statements)

References 15 publications

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“…However, partial responses and prolonged disease stability have occurred with several agents. They are often combined with cytotoxic agents for the treatment of glioblastoma (14)(15)(16)(17).…”

Section: Introductionmentioning

confidence: 99%

Combination celecoxib and temozolomide in C6 rat glioma orthotopic model

et al. 2006

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Abstract. The purpose of this study was to determine whether a combination treatment of temozolomide with celecoxib is effective in the rat orthotopic glioma model. After stereotactic injection of C6/LacZ rat glioma cells into the Sprague Dawley rat brain, the rats were randomly assigned to four treatment groups [group 1, control treatment; group 2, celecoxib (25 mg/kg p.o. everyday) alone; group 3, temozolomide (7.5 mg/kg i.p. for 5 days at 2nd week) alone; group 4, a combination of celecoxib and temozolomide]. Rats were sacrificed 18 days after treatment, and the body weight, tumor volume, tumor cell proliferation, microvessel densities, and apoptosis were evaluated. There was a significant reduction of tumor volume in combination group compared to control or single-agent therapy. The median tumor volume was estimated to be 111.5 mm 3 (control), 65.0 mm 3 (celecoxib), 71.8 mm 3 (temozolomide) and 18.7 mm 3 (combination). In the combination group, there was increased tumor cell apoptosis as well as decreased microvessel density and tumor cell proliferation relative to the control and singleagent therapy (P<0.05). Collectively, the data suggest that the combination celecoxib and temozolomide may provide a novel and effective approach to the treatment of glioblastoma.

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Section: Introductionmentioning

confidence: 99%

Combination celecoxib and temozolomide in C6 rat glioma orthotopic model

et al. 2006

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“…Pre-RT chemotherapy with carmustine, oral etoposide and cisplatin was insufficiently active, while substantial grade III and IV toxicity was observed in 48% of patients in one study 46 . Antiangiogenic substances such as interferonalpha did not confer any benefit 47,48 .…”

Section: Discussionmentioning

confidence: 88%

Long-Term Outcome of Postoperative Irradiation in Patients with Newly Diagnosed WHO Grade III Anaplastic Gliomas

Nagy

Schulz-Ertner

Bischof

et al. 2009

Tumori

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“…Addition of IFN-α to IR plus carmustine chemotherapy did not improve the survival of newly-diagnosed high-grade glioma patients [ 46 ]. Moreover, the combination of IFN-α and 13-cis-retinoic acid enhanced glioma susceptibility to IR in vitro but did not result in a better outcome in patients treated with IR plus IFN-α as compared to IR alone [ 47 ].…”

Section: Discussionmentioning

confidence: 99%

No role of IFITM3 in brain tumor formationin vivo

et al. 2016

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Glioblastoma multiforme (GBM) is one of the most lethal solid tumors in adults. Despite aggressive treatment approaches for patients, GBM recurrence is inevitable, in part due to the existence of stem-like brain tumor-propagating cells (BTPCs), which produce factors rendering them resistant to radio- and chemotherapy. Comparative transcriptome analysis of irradiated, patient-derived BTPCs revealed a significant upregulation of the interferon-inducible transmembrane protein 3 (IFITM3), suggesting the protein as a factor mediating radio resistance. Previously, IFITM3 has been described to affect glioma cells; therefore, the role of IFITM3 in the formation and progression of brain tumors has been investigated in vivo. Intracranial implantation studies using radio-selected BTPCs alongside non-irradiated parental BTPCs in immunodeficient mice displayed no influence of irradiation on animal survival. Furthermore, gain and loss of function studies using BTPCs ectopically expressing IFITM3 or having IFITM3 down-modulated by a shRNA approach, did affect neither tumor growth nor animal survival. Additionally, a syngeneic model based on the mouse glioma cell line GL261 was applied in order to consider the possibility that IFITM3 relies on an intact immune system to unfold its tumorigenic potential. GL261 cells ectopically expressing IFITM3 were implanted into the striatum of immunocompetent mice without influencing the survival of glioma-bearing animals. Lastly, the vasculature and the extent of microglia/macrophage invasion into the tumor were studied in BTPC and GL261 tumors but neither parameter was altered by IFITM3. This report presents for the first time that IFITM3 is upregulated in patient-derived BTPCs upon irradiation but does not affect brain tumor formation or progression in vivo.

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Interferon-α2a and 13-cis-retinoic acid with radiation treatment for high-grade glioma

Cited by 24 publications

References 15 publications

Combination celecoxib and temozolomide in C6 rat glioma orthotopic model

Combination celecoxib and temozolomide in C6 rat glioma orthotopic model

Long-Term Outcome of Postoperative Irradiation in Patients with Newly Diagnosed WHO Grade III Anaplastic Gliomas

No role of IFITM3 in brain tumor formationin vivo

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