[18F]-fluoromisonidazole (FMISO) PET/MRI hypoxic fraction distinguishes neuroinflammatory pseudoprogression from recurrent glioblastoma in patients treated with pembrolizumab

Author:

Barajas Ramon F12ORCID,Ambady Prakash3,Link Jeanne4,Krohn Kenneth A4,Raslan Ahmed5ORCID,Mallak Nadine6,Woltjer Randy7,Muldoon Leslie3,Neuwelt Edward A358

Affiliation:

1. Department of Radiology, Neuroradiology Section, Oregon Health & Science University , Portland Oregon , USA

2. Knight Cancer Institute Translational Oncology Program, Oregon Health & Science University , Portland, Oregon , USA

3. Neuro-Oncology and Blood-Brain Barrier Program , Department of Neurology, Oregon Health & Science University, Portland, Oregon , USA

4. Center for Radiochemistry Research, Oregon Health & Science University , Portland, Oregon , USA

5. Department of Neurological Surgery, Oregon Health & Science University , Portland, Oregon , USA

6. Advanced Imaging Research Center, Oregon Health & Science University , Portland Oregon , USA

7. Department of Pathology, Oregon Health & Science University , Portland, Oregon , USA

8. Office of Research and Development, Portland Veterans Affairs Medical Center , Portland, Oregon , USA

Abstract

Abstract Response assessment after immunotherapy remains a major challenge in glioblastoma due to an expected increased incidence of pseudoprogression. Gadolinium-enhanced magnetic resonance imaging (MRI) is the standard for monitoring therapeutic response, however, is markedly limited in characterizing pseudoprogression. Given that hypoxia is an important defining feature of glioblastoma regrowth, we hypothesized that [18F]-fluoromisonidazole (FMISO) positron emission tomography (PET) could provide an additional physiological measure for the diagnosis of immunotherapeutic failure. Six patients with newly diagnosed glioblastoma who had previously received maximal safe resection followed by Stupp protocol CRT concurrent with pembrolizumab immunotherapy were recruited for FMISO PET and Gd-MRI at the time of presumed progression. The hypoxic fraction was defined as the ratio of hypoxic volume to T1-weighted gadolinium-enhancing volume. Four patients diagnosed with pseudoprogression demonstrated a mean hypoxic fraction of 9.8 ± 10%. Two with recurrent tumor demonstrated a mean hypoxic fraction of 131 ± 66%. Our results, supported by histopathology, suggest that the noninvasive assessment of hypoxic fraction by FMISO PET/MRI is clinically feasible and may serve as a biologically specific metric of therapeutic failure.

Funder

National Institutes of Health

National Cancer Institute

Publisher

Oxford University Press (OUP)

Subject

Medicine (miscellaneous)

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