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DOI: 10.1055/s-0029-1245570
© Georg Thieme Verlag KG Stuttgart · New York
Evaluation des ADC-Mappings als Prädiktor für ein Ansprechen von Glioblastomrezidiven auf eine Therapie mit Avastin
Evaluation of ADC Mapping as an Early Predictor for Tumor Response to Chemotherapy in Recurrent Glioma Treated with Bevacizumab/Irinotecan: Proof of PrinciplePublication History
eingereicht: 21.2.2010
angenommen: 11.6.2010
Publication Date:
25 August 2010 (online)
Zusammenfassung
Ziel: Die Evaluation eines Therapieansprechens von Glioblstomrezidiven beruht bisher auf der Beurteilung nach MacDonald oder nach RECIST 8 – 10 Wochen nach Beginn der Chemotherapie. Diffusionsgewichtete MRT-Sequenzen, insbesondere das ADC-Mapping, können dazu dienen, bereits 3 Wochen nach Chemotherapiebeginn die Wirksamkeit einer antiangiogenetischen Therapie vorauszusagen. Material und Methoden: 12 Patienten mit Glioblastomrezidiven wurden in diese Machbarkeitsstudie eingeschlossen. Prätherapeutisch am Tag 1, intratherapeutisch nach 3 Wochen und posttherapeutisch 3 Monate nach Beginn der Chemotherapie wurden MRT-Untersuchungen durchgeführt. Prognostisch aussagekräftige ADC-Werte (ADCprog) wurden aus den ersten beiden Untersuchungen berechnet (ADCpre – ADCintra = ADCprog) und mit der 3-Monatskontrolle als Goldstandard auf Richtigkeit überprüft. Die ADC-Werte bilden die Brownschen Molekularbewegung im EZR ab, die von der Dichte der umgebenden Zellverbände beeinflusst wird. Abnehmende ADC-Werte aufgrund zunehmender Zelldichte wurden als Zeichen eines Tumorprogresses („progressive disease”) und zunehmende ADC-Werte bei Zellzerfall als Therapieansprechen („partial response”) gewertet. ADCprog-Wertveränderungen von unter 10 × 10–6 mm2 /s wurden als „stable disease” bezeichnet. Die prognostisch relevanten ADC Werte wurden immer vor der 3-Monatskontrolle berechnet, sodass die Reader für die zukünftige Entwicklung des Tumors geblindet waren. Ergebnisse: In 10 von 12 Fällen konnte die zukünftige Entwicklung des Tumors korrekt vorausgesagt werden. ADC-Mapping kann bereits 3 Wochen nach Therapiebeginn das Ansprechen des Glioblastomrezidivs prognostizieren.
Abstract
Purpose: The assessment of the radiological response of recurrent glioma is based on the Macdonald or RECIST criteria 8 to 10 weeks from the start of treatment. Magnetic resonance imaging using an apparent diffusion coefficient map may provide an earlier measure for predicting the response to therapy of recurrent glioma. Materials and Methods: Twelve patients with recurrent high-grade glioma were enrolled in a feasibility study of pretreatment MRI on day 1, intra-treatment MRI in week 3, and post-treatment MRI in week 12. Prognostically relevant ADC values (ADCprog) of each recurrent glioma at 3 weeks were calculated as a function of their pre- and intra-therapy ADC values (ADCpre – ADCintra = ADCprog). Because we hypothesized that smaller ADC values correlate with less Brownian motion of water molecules in the extracellular space and that a higher cell density may restrain this water diffusion, we set smaller ADC values at a second time point as ”progressive disease” (PD) and higher ADC values as ”partial response” (PR). A change in ADCprog of less than 10 × 10–6 mm2 /sec was set as ”stable disease” (SD). The ADCprog values were always calculated before the final scan after 3 months was performed. The readers were blinded to the future development of the tumor. Results: In 10 of the 12 patients we could correctly predict the tumor response to chemotherapy. One patient died before the three-month control, and one recurrent glioma did not develop as predicted. ADC mapping is found to predict patient response at 3 weeks from the start of treatment, revealing that early changes in tumor diffusion values could be used as a prognostic indicator also for chemotherapeutically treated recurrences of high-grade glioma.
Key words
brain - MR diffusion/perfusion - experimental study
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Dr. Adrian Ringelstein
Diagnostische Radiologie, Universitätsklinikum Düsseldorf
Moorenstraße 5
40225 Düsseldorf
Phone: ++ 49/2 11/8 11 77 52
Fax: ++ 49/2 11/81 00
Email: ar75@gmx.de