High dose methotrexate for pediatric high grade glioma: results of the HIT-GBM-D Pilot study

Wolff, Johannes; Kortmann, Rolf Dieter; Wolff, Birte; Pietsch, Torsten; Peters, Ove A.; Schmid, Hans; Rutkowski, Stefan; Warmuth‐Metz, Monika; Kramm, Christoph

doi:10.1007/s11060-010-0334-2

Cited by 44 publications

(24 citation statements)

References 32 publications

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“…19 HIT-GBM-B -treated participants with RT and concurrent chemotherapy (cisplatin/etoposide in the first cycle and cisplatin/ etoposide/ifosfamide in the second cycle) followed by interferon-g and/or low-dose cyclophosphamide maintenance therapy 20 ; HIT-GBM-C involved administration of intensive chemotherapy (vincristine, cisplatin, ifosfamide, and etoposide) both during and after RT followed by oral valproic acid as maintenance therapy (a histone deacetylase/HDAC inhibitor) 1 ; and HIT-GBM-D, a pilot phase II study, evaluated the efficacy of single-agent methotrexate (MTX) prior to RT and chemotherapy. 22 In this pilot study, 2 doses of MTX (5 gm/m 2 ) were given prior to RT followed by simultaneous chemotherapy-RT and subsequent maintenance chemotherapy as per the HIT-GBM-C protocol. The toxicity profile was acceptable, with no deaths related to drug toxicity.…”

Section: Chemotherapymentioning

confidence: 99%

“…Data from this study suggested that the HIT-GBM-D protocol is favorable for treating pHGG patients with a GTR. 22 The approach of giving 2 cycles of high-dose MTX prior to radiochemotherapy will be assessed in a phase III RCT, and results from the randomized study are pending. The German Society for Pediatric Oncology Vanan and Eisenstat: "Management of pediatric high-grade gliomas" conducted a randomized clinical trial to evaluate the efficacy of pre-RT intensive chemotherapy in pHGGs in 1991.…”

Section: Chemotherapymentioning

confidence: 99%

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Management of high-grade gliomas in the pediatric patient: Past, present, and future

Vanan

Eisenstat

2014

Neuro-Oncology Practice

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High-grade gliomas (HGGs) constitute 15% of all primary brain tumors in children and adolescents. Routine histopathological diagnosis is based on tissue obtained from biopsy or, preferably, from the resected tumor itself. The majority of pediatric HGGs are clinically and biologically distinct from histologically similar adult malignant gliomas; these differences may explain the disparate responses to therapy and clinical outcomes when comparing children and adults with HGG. The recently proposed integrated genomic classification identifies 6 distinct biological subgroups of glioblastoma (GBM) throughout the age spectrum. Driver mutations in genes affecting histone H3.3 (K27M and G34R/V) coupled with mutations involving specific proteins (TP53, ATRX, DAXX, SETD2, ACVR1, FGFR1, NTRK) induce defects in chromatin remodeling and may play a central role in the genesis of many pediatric HGGs. Current clinical practice in pediatric HGGs includes surgical resection followed by radiation therapy (in children aged . 3 years) with concurrent and adjuvant chemotherapy with temozolomide. However, these multimodality treatment strategies have had a minimal impact on improving survival. Ongoing clinical trials are investigating new molecular targets, chemoradiation sensitization strategies, and immunotherapy. Future clinical trials of pediatric HGG will incorporate the distinction between GBM molecular subgroups and stratify patients using group-specific biomarkers.

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Section: Chemotherapymentioning

confidence: 99%

Section: Chemotherapymentioning

confidence: 99%

Management of high-grade gliomas in the pediatric patient: Past, present, and future

Vanan

Eisenstat

2014

Neuro-Oncology Practice

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“…MTX is a folate antagonist with limited uptake in the brain, which likely contributes to the need for high-dose therapy (Nierenberg et al, 1991;Wolff et al, 2011). Studies in rodents (Devineni et al, 1996) and patients (Blakeley et al, 2009) that used brain microdialysis to measure the brain interstitial fluid MTX concentrations attest to its limited distribution in the normal brain, with a brain-to-plasma ratio 0.051 6 0.032 and 0.032 6 0.094 in rodents and humans, respectively.…”

Section: Introductionmentioning

confidence: 99%

The Effect of ABCG2 and ABCC4 on the Pharmacokinetics of Methotrexate in the Brain

Sane¹,

Wu²,

Zhang³

et al. 2014

Drug Metab Dispos

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Methotrexate (MTX) is the cornerstone of chemotherapy for primary central nervous system lymphoma, yet how the bloodbrain barrier (BBB) efflux transporters ABCG2 and ABCC4 influence the required high-dose therapy is unknown. To evaluate their role, we used four mouse strains, C57BL/6 (wild-type; WT), Abcg2 2/2 , Abcc4 2/2 , and Abcg2 2/2 ;Abcc4 2/2 (double knockout; DKO) to conduct brain microdialysis studies after single intravenous MTX doses of 50 mg/kg. When the area under the concentrationtime curve for plasma (AUC plasma ) was used to assess systemic exposure to MTX, the rank order was Abcc4 2/2 < WT < Abcg2 2/2 < Abcg2 2/2 Abcc4 2/2 . Only the DKO exposure was significantly higher than that of the WT group (P < 0.01), a reflection of the role of Abcg2 in biliary excretion and Abcc4 in renal excretion. MTX brain interstitial fluid concentrations obtained by microdialysis were used to calculate the area under the concentration-time curve for the brain (AUC brain ), which found the rank order of exposure to be WT < Abcc4 2/2 < Abcg2 2/2 < Abcg2Abcc4 2/2 with the largest difference being 4-fold: 286.13 6 130 mg*min/ml (DKO) versus 66.85 6 26 (WT). Because the transporters affected the systemic disposition of MTX, particularly in the DKO group, the ratio of the AUC brain /AUC plasma or the brain/plasma partition coefficient Kp was calculated, revealing that the DKO strain had a significantly higher value (0.23 6 0.09) than the WT strain (0.11 6 0.05). Both Abcg2 and Abcc4 limited BBB penetration of MTX; however, only when both drug efflux pumps were negated did the brain accumulation of MTX significantly increase. These findings indicate a contributory role of both ABCG2 and ABCC4 to limiting MTX distribution in patients.

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“…Hiçbiri YDG olgularına anlamlı bir yarar getirmemiştir. [14][15][16] Fransa Pediatrik Onkoloji Grubu da, 1990-1996 arasında RT öncesi verilen karmustin (BCNU), sisplatin ve etoposid (VP-16) (BCV) tedavisinin etkinliğini araştırmış ancak pulmoner toksisitesi çok fazla görülen bu KT seçeneği önerilmemiştir. [17] Erişkin GBM'li hastalarda Temozolomide'nin (TMZ) etkinliği gösterildikten sonra, birçok pediatrik çalışma bu tedavi protokolünü denemiş ancak benzer yaşam sürelerini gösterememiştir.…”

Section: Yüksek Dereceli Gliom Tedavisiunclassified

Treatment of high-grade glioma in children

Cakir¹

2013

TJ Oncol

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High dose methotrexate for pediatric high grade glioma: results of the HIT-GBM-D Pilot study

Cited by 44 publications

References 32 publications

Management of high-grade gliomas in the pediatric patient: Past, present, and future

Management of high-grade gliomas in the pediatric patient: Past, present, and future

The Effect of ABCG2 and ABCC4 on the Pharmacokinetics of Methotrexate in the Brain

Treatment of high-grade glioma in children

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