Retrospective examination of pseudoprogression in IDH mutant gliomas

Author:

Wetzel Ethan A1,Farrell Matthew J2,Eldred Blaine S C1,Liu Vicki1,Saha Ishan1,Zapanta Rinonos Serendipity1,Prins Terry1,Li Tie1,Cao Minsong2,Hegde John2,Kaprealian Tania2,Khanlou Negar3,Liau Linda M4,Nghiemphu Phioanh Leia1,Cloughesy Timothy Francis1,Chong Robert A1,Ellingson Benjamin M45,Lai Albert1

Affiliation:

1. Department of Neurology, University of California, Los Angeles , Los Angeles, CA , USA

2. Department of Radiation Oncology, University of California, Los Angeles , Los Angeles, CA , USA

3. Department of Pathology and Laboratory Medicine, University of California, Los Angeles , Los Angeles, CA , USA

4. Department of Neurosurgery, University of California, Los Angeles , Los Angeles, CA , USA

5. Department of Radiological Sciences, University of California, Los Angeles , Los Angeles, CA , USA

Abstract

Abstract Background Tumor surveillance of isocitrate dehydrogenase (IDH) mutant gliomas is accomplished via serial contrast MRI. When new contrast enhancement (CEnew) is detected during postsurgical surveillance, clinicians must assess whether CEnew indicates pseudoprogression (PsP) or tumor progression (TP). PsP has been better studied in IDH wild-type glioblastoma but has not been well characterized in IDH mutant gliomas. We conducted a retrospective study evaluating the incidence, predictors, natural history, and survival of PsP patients in a large cohort of IDH mutant glioma patients treated at a single institution. Methods We identified 587 IDH mutant glioma patients treated at UCLA. We directly inspected MRI images and radiology reports to identify CEnew and categorized CEnew into TP or PsP using MRI or histopathology. Results Fifty-six percent of patients developed CEnew (326/587); of these, 92/326 patients (28% of CEnew; 16% of all) developed PsP and 179/326 (55%) developed TP. All PsP patients had prior radiation, chemotherapy, or chemoradiotherapy. PsP was associated with longer overall survival (OS) versus TP patients and similar OS versus no CEnew. PsP differs from TP based on earlier time of onset (median 5.8 vs 17.4 months from treatment, P < .0001) and MRI features that include punctate enhancement and enhancement location. Conclusion PsP patients represented 28% of CEnew patients and 16% of all patients; PsP patients demonstrated superior outcomes to TP patients, and equivalent survival to patients without CEnew. PsP persists for <1 year, occurs after treatment, and differs from TP based on time of onset and radiographic features. Poor outcomes after CEnew are driven by TP.

Funder

Heart of the Brain, Bradley Zankel Foundation

National Institutes of Health

National Cancer Institute

American Cancer Society

DoD

Publisher

Oxford University Press (OUP)

Subject

Surgery,Oncology,Neurology (clinical)

Reference26 articles.

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3. Contrast enhancement predicting survival in integrated molecular subtypes of diffuse glioma: an observational cohort study;Hempel;J Neurooncol.,2018

4. Pseudoprogression after glioma therapy: a comprehensive review;Kruser;Expert Rev Neurother.,2013

5. Pseudoprogression after glioma therapy: an update;Galldiks;Expert Rev Neurother.,2017

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