<i>MGMT</i> Promoter Methylation Status Can Predict the Incidence and Outcome of Pseudoprogression After Concomitant Radiochemotherapy in Newly Diagnosed Glioblastoma Patients

Alba A. Brandes , Enrico Franceschi , Alicia Tosoni , Alba A. Brandes , Enrico Franceschi , Alicia Tosoni , V. Blatt , Annalisa Pession , Giovanni Tallini , Roberta Bertorelle , Stefania Bartolini , Fabio Calbucci , Alvaro Andreoli , G. Frezza , Marco Leonardi , F. Spagnolli , Mario Ermani
2008 Journal of Clinical Oncology 814 citations

Abstract

Purpose Standard therapy for glioblastoma (GBM) is temozolomide (TMZ) administration, initially concurrent with radiotherapy (RT), and subsequently as maintenance therapy. The radiologic images obtained in this setting can be difficult to interpret since they may show radiation-induced pseudoprogression (psPD) rather than disease progression. Methods Patients with histologically confirmed GBM underwent radiotherapy plus continuous daily temozolomide (75 mg/m 2 /d), followed by 12 maintenance temozolomide cycles (150 to 200 mg/m 2 for 5 days every 28 days) if magnetic resonance imaging (MRI) showed no enhancement suggesting a tumor; otherwise, chemotherapy was delivered until complete response or unequivocal progression. The first MRI scan was performed 1 month after completing combined chemoradiotherapy. Results In 103 patients (mean age, 52 years [range 20 to 73 years]), total resection, subtotal resection, and biopsy were obtained in 51, 51, and 1 cases, respectively. MGMT promoter was methylated in 36 patients (35%) and unmethylated in 67 patients (65%). Lesion enlargement, evidenced at the first MRI scan in 50 of 103 patients, was subsequently classified as psPD in 32 patients and early disease progression in 18 patients. PsPD was recorded in 21 (91%) of 23 methylated MGMT promoter and 11 (41%) of 27 unmethylated MGMT promoter (P = .0002) patients. MGMT status (P = .001) and psPD detection (P = .045) significantly influenced survival. Conclusion PsPD has a clinical impact on chemotherapy-treated GBM, as it may express the glioma killing effects of treatment and is significantly correlated with MGMT status. Improvement in the early recognition of psPD patterns and knowledge of mechanisms underlying this phenomenon are crucial to eliminating biases in evaluating the results of clinical trials and guaranteeing effective treatment.

Keywords

TemozolomideMedicineChemoradiotherapyRadiation therapyChemotherapyDacarbazineMagnetic resonance imagingConcomitantBiopsyGliomaOncologyStage (stratigraphy)Nuclear medicineInternal medicineRadiologyCancer research

MeSH Terms

AdultAgedAntineoplastic AgentsAlkylatingBrain DiseasesBrain NeoplasmsChemotherapyAdjuvantDNA MethylationDNA Modification MethylasesDNA Repair EnzymesDacarbazineDisease ProgressionFemaleGene Expression RegulationEnzymologicGene Expression RegulationNeoplasticGenetic Predisposition to DiseaseGlioblastomaHumansKaplan-Meier EstimateMagnetic Resonance ImagingMaleMiddle AgedNecrosisPatient SelectionPromoter RegionsGeneticProportional Hazards ModelsRadiation InjuriesRadiotherapyAdjuvantRetrospective StudiesTemozolomideTime FactorsTreatment OutcomeTumor Suppressor Proteins

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Publication Info

Year
2008
Type
article
Volume
26
Issue
13
Pages
2192-2197
Citations
814
Access
Closed

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Alba A. Brandes, Enrico Franceschi, Alicia Tosoni et al. (2008). <i>MGMT</i> Promoter Methylation Status Can Predict the Incidence and Outcome of Pseudoprogression After Concomitant Radiochemotherapy in Newly Diagnosed Glioblastoma Patients. Journal of Clinical Oncology , 26 (13) , 2192-2197. https://doi.org/10.1200/jco.2007.14.8163

Identifiers

DOI
10.1200/jco.2007.14.8163
PMID
18445844

Data Quality

Data completeness: 86%