| Literature DB >> 28291423 |
A Charlotte P Sewing1,2,3, Tonny Lagerweij4,2,3, Dannis G van Vuurden1,2,3, Michaël H Meel1,4,3, Susanna J E Veringa1,2,3, Angel M Carcaboso5, Pieter J Gaillard6, W Peter Vandertop4,3, Pieter Wesseling7,2,3,6,8, David Noske4,2,3, Gertjan J L Kaspers2,9, Esther Hulleman1,2,3.
Abstract
OBJECTIVE Pediatric high-grade gliomas (pHGGs) including diffuse intrinsic pontine gliomas (DIPGs) are primary brain tumors with high mortality and morbidity. Because of their poor brain penetrance, systemic chemotherapy regimens have failed to deliver satisfactory results; however, convection-enhanced delivery (CED) may be an alternative mode of drug delivery. Anthracyclines are potent chemotherapeutics that have been successfully delivered via CED in preclinical supratentorial glioma models. This study aims to assess the potency of anthracyclines against DIPG and pHGG cell lines in vitro and to evaluate the efficacy of CED with anthracyclines in orthotopic pontine and thalamic tumor models. METHODS The sensitivity of primary pHGG cell lines to a range of anthracyclines was tested in vitro. Preclinical CED of free doxorubicin and pegylated liposomal doxorubicin (PLD) to the brainstem and thalamus of naïve nude mice was performed. The maximum tolerated dose (MTD) was determined based on the observation of clinical symptoms, and brains were analyzed after H & E staining. Efficacy of the MTD was tested in adult glioma E98-FM-DIPG and E98-FM-thalamus models and in the HSJD-DIPG-007-Fluc primary DIPG model. RESULTS Both pHGG and DIPG cells were sensitive to anthracyclines in vitro. Doxorubicin was selected for further preclinical evaluation. Convection-enhanced delivery of the MTD of free doxorubicin and PLD in the pons was 0.02 mg/ml, and the dose tolerated in the thalamus was 10 times higher (0.2 mg/ml). Free doxorubicin or PLD via CED was ineffective against E98-FM-DIPG or HSJD-DIPG-007-Fluc in the brainstem; however, when applied in the thalamus, 0.2 mg/ml of PLD slowed down tumor growth and increased survival in a subset of animals with small tumors. CONCLUSIONS Local delivery of doxorubicin to the brainstem causes severe toxicity, even at doxorubicin concentrations that are safe in the thalamus. As a consequence, the authors could not establish a therapeutic window for treating orthotopic brainstem tumors in mice. For tumors in the thalamus, therapeutic concentrations to slow down tumor growth could be reached. These data suggest that anatomical location determines the severity of toxicity after local delivery of therapeutic agents and that caution should be used when translating data from supratentorial CED studies to treat infratentorial tumors.Entities:
Keywords: BBB = blood-brain barrier; BLI = bioluminescent imaging; CED; CED = convection-enhanced delivery; DIPG; DIPG = diffuse intrinsic pontine glioma; GBM = glioblastoma multiforme; IC50 = half maximal inhibitory concentration; LG-BSG = low-grade brainstem glioma; MTD = maximum tolerated dose; PBS = phosphate-buffered saline; PLD = pegylated liposomal doxorubicin; TOPIIA = topoisomerase Type IIA; VUMC = VU University Medical Center; anthracyclines; convection-enhanced delivery; diffuse intrinsic pontine glioma; doxorubicin; oncology; pHGG; pHGG = pediatric high-grade glioma; pediatric high-grade glioma; thalamus
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Year: 2017 PMID: 28291423 DOI: 10.3171/2016.9.PEDS16152
Source DB: PubMed Journal: J Neurosurg Pediatr ISSN: 1933-0707 Impact factor: 2.375