Oligodendroglioma patient survival is associated with circulating B-cells and age

Author:

Taylor Jennie W123ORCID,Warrier Gayathri3ORCID,Hansen Helen M3,McCoy Lucie3ORCID,Rice Terri3,Guerra Geno3ORCID,Francis Stephen S413,Clarke Jennifer L123ORCID,Bracci Paige M4ORCID,Hadad Sara3,Kelsey Karl T5ORCID,Wrensch Margaret3,Molinaro Annette M413,Wiencke John K43

Affiliation:

1. Weill Institute for Neurosciences, University of California San Francisco , San Francisco, California, USA

2. Department of Neurology, University of California San Francisco , San Francisco, California, USA

3. Department of Neurological Surgery, University of California San Francisco , San Francisco, California, USA

4. Department of Epidemiology and Biostatistics, University of California San Francisco , San Francisco, California, USA

5. Departments of Epidemiology; Pathology and Laboratory Medicine, Brown University , Providence, Rhode Island, USA

Abstract

Abstract Background Variations in survival among patients with oligodendroglioma are unexplained by known prognostic factors. To assess the impact of peripheral immune profiles on prognosis, we applied immunomethylomics analyses—DNA methylation of archived whole blood samples, to characterize immune cells. Methods We compared the proportions of immune cells from patients with oligodendroglioma to other glioma subtypes and controls. We used recursive partitioning analysis (RPA) within the oligodendrogliomas to correlate with survival. Results Patients with oligodendrogliomas (141) were median age at diagnosis of 44 years; 57% male; 75% White; 60% prior chemotherapy; and 25% on dexamethasone at sample collection. Patients with oligodendrogliomas had immune profiles more similar to controls than other glioma subtypes, though with notably lower B-cells. RPA of patients with oligodendrogliomas delineated 2 survival groups based on an interaction between age and B-naïve cells. Patients with longer survival (median 24.2 years) were ≤42 years of age with higher B-naïve cells versus worse survival (median 16.9 years) who were ≤42 years of age with lower B-naïve cells or >42 years of age (P = .00032). Patients with worse survival also had lower CD4- and CD8-naïve T-cells. Similar immune profiles were observed in an independent cohort of oligodendroglioma patients prior to surgery. Conclusions Peripheral blood immune profiles in oligodendroglioma suggested that younger patients with lower B-naïve cells experienced shorter survival. Though our findings lack of validation cohort and use a heterogenous patient population, they suggest peripheral blood immune profiles may be prognostic for patients with glioma and warrant further investigation.

Funder

Work at University of California, San Francisco

National Institutes of Health

National Brain Tumor Foundation

Stanley D. Lewis and Virginia S. Lewis Endowed Chair in Brain Tumor Research

Robert Magnin Newman Endowed Chair in Neuro-oncology

National Center for Research Resources

National Center for Advancing Translational Sciences

UCSF-CTSI

Publisher

Oxford University Press (OUP)

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