Hyperfractionated radiation therapy (72 Gy) for children with brain stem gliomas A childrens cancer group phase I/II trial

Packer, Roger J.; Boyett, James M.; Zimmerman, Robert A.; Rorke, Lucy B.; Kaplan, Allen M.; Albright, A. Leland; Selch, Michael T.; Finlay, Jonathan L.; Hammond, G. Denman; Wara, William M.

doi:10.1002/1097-0142(19930815)72:4<1414::aid-cncr2820720442>3.0.co;2-c

Cited by 127 publications

(48 citation statements)

References 13 publications

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“…Given the paucity of information about the biology of brain stem gliomas, it is often necessary to make inferences about their molecular characteristics based on studies of pediatric highgrade gliomas at non-brain stem sites. Other than radiation therapy, no other therapy has demonstrated efficacy in prolonging the survival of these patients [8].…”

Section: Introductionmentioning

confidence: 99%

Expression of glioma-associated antigens in pediatric brain stem and non-brain stem gliomas

et al. 2008

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We investigated the protein expression of three glioma-associated antigens (GAAs) in pediatric brain stem glioma (BSG) and non-brain stem glioma (NBSG) cases with a view to their possible use in immunotherapy. Expression of EphA2, IL-13Rα2 and Survivin were studied by immunohistochemistry on paraffin-embedded tissues using a series of 15 BSG cases and 12 NBSG cases. Thirteen of 15 BSGs and all 12 NBSGs expressed at least one of GAAs; and 7 BSGs and 9 NBSGs expressed at least two of these GAAs at higher levels than non-neoplastic brain. There was no association between the tumor grade and levels of GAA expression. Although many cases demonstrated diffuse expression of GAAs throughout specimens, partial or patchy expression was noted in a small number of cases, suggesting a need for targeting multiple GAAs in immunotherapy. These results suggest that EphA2, IL-13Ralpha2 and Survivin are suitable targets for developing vaccine strategies for pediatric glioma.

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Section: Introductionmentioning

confidence: 99%

Expression of glioma-associated antigens in pediatric brain stem and non-brain stem gliomas

et al. 2008

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“…Most reports on tumour dissemination of HGG and DIPG after diagnosis, so called secondary dissemination of disease (SDD), are case reports or small series; few reports include large numbers of patients (Packer et al, 1985(Packer et al, , 1990(Packer et al, , 1993Dropcho et al, 1987;Vertosick and Selker, 1990;Grabb et al, 1992;Arita et al, 1994;Heideman et al, 1997;Donahue et al 1998;Allen et al, 1999;Endo et al, 2003;Saito et al, 2003). These series mostly come from the late 1980s and early 1990s, when MRI was not routinely available for follow-up investigations (Awad et al, 1986;Vertosick and Selker, 1990;Arita et al, 1994).…”

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confidence: 99%

Secondary dissemination in children with high-grade malignant gliomas and diffuse intrinsic pontine gliomas

et al. 2006

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In children, treatment regimen for high-grade gliomas (HGG) and diffuse intrinsic pontine gliomas (DIPG) are generally not stratified according to disease stage. The hypothesis was that secondary disseminating disease (SDD) in children with HGG is related to an even worse outcome. Description of SDD pattern was performed. In total, 270 children with newly diagnosed HGG or DIPG were eligible for retrospective analysis of SDD. Medical and computer records of these patients were reviewed for demographic characteristics, sites of dissemination, prognostic variables. Forty-six (17%) of the 270 patients had developed SDD. The median time to SDD was 8.2 months. The median overall survival (OS) after dissemination was 3.2 months. The SDD was located parenchymal in the supratentorial (34.8%), infratentorial (6.5%), supratentorial and infratentorial (19.6%), spinal (10.9%), spinal and cerebral (6.5%) regions of the CNS, or leptomeningeal (21.7%). For HGG patients, the median OS was shorter among patients with SDD than among patients without SDD (1.02 vs 1.41 years, P ¼ 0.0495). In the group of patients with SDD, patients with cerebrospinal fluid dissemination had a worse outcome compared with patients with parenchymal metastases. Summarising, SDD is a negative prognostic factor for patients with HGG outside the pons. Treatment stratification should be considered.

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“…[24,25] CCG-9941 çalışmasında; RT öncesi KT ve ardından hiperfraksiyone RT verilmiş yaşam sü-resi sadece konvansiyonel RT verilen grupla benzer bulunmuştur. [24] Massimino ve ark., [26] 1987-2005 arasında, 62 çocukta yaptıkları 4 pilot protokolün (A-Konvansiyonel KT RT-VP-16/sitosin arabinosid/Ifosfamid/sisplatin/daktinomisi; B-Yüksek Doz KT ve +ABMT+RT+KT; C-sisplatin/etoposid sonrası isotretinoin (preRT+RT+postRT ile eş-zamanlı); D-Vinorelbine (preRT+RT+postRT ile eşzamanlı) sonucunda, hiçbir protokolün yaşam oranları açısından literatürle karşılaştırıldığında bir üstünlük getirmediği görülmüştür (1 yıllık yaşam oranı %45, median yaşam oranı 11 ay).…”

Section: Beyin Sapı Tümörlerinde Tedaviunclassified

Treatment of high-grade glioma in children

Cakir¹

2013

TJ Oncol

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Hyperfractionated radiation therapy (72 Gy) for children with brain stem gliomas A childrens cancer group phase I/II trial

Cited by 127 publications

References 13 publications

Expression of glioma-associated antigens in pediatric brain stem and non-brain stem gliomas

Expression of glioma-associated antigens in pediatric brain stem and non-brain stem gliomas

Secondary dissemination in children with high-grade malignant gliomas and diffuse intrinsic pontine gliomas

Treatment of high-grade glioma in children

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