Association of mutations in DNA polymerase epsilon with increased CD8+ cell infiltration and prolonged progression-free survival in patients with meningiomas

John W Rutland; Jonathan T Dullea; Corey M Gill; Danielle Chaluts; Daniel Ranti; Ethan Ellis; Annie Arrighi-Allisan; Yayoi Kinoshita; Russell B McBride; Joshua Bederson; Michael Donovan; Robert Sebra; Mary Fowkes; Melissa Umphlett; Raj K Shrivastava

doi:10.3171/2021.11.FOCUS21592

Association of mutations in DNA polymerase epsilon with increased CD8+ cell infiltration and prolonged progression-free survival in patients with meningiomas

Neurosurg Focus. 2022 Feb;52(2):E7. doi: 10.3171/2021.11.FOCUS21592.

Authors

John W Rutland¹, Jonathan T Dullea¹, Corey M Gill¹, Danielle Chaluts¹, Daniel Ranti¹, Ethan Ellis², Annie Arrighi-Allisan¹, Yayoi Kinoshita³, Russell B McBride^{3

4}, Joshua Bederson¹, Michael Donovan³, Robert Sebra^{2

5}, Mary Fowkes³, Melissa Umphlett³, Raj K Shrivastava¹

Affiliations

¹ 1Department of Neurosurgery, Icahn School of Medicine at Mount Sinai.
² 2Department of Genetics and Genomic Sciences, Icahn School of Medicine at Mount Sinai.
³ 3Department of Pathology, Icahn School of Medicine at Mount Sinai.
⁴ 4The Institute for Translational Epidemiology, Icahn School of Medicine at Mount Sinai, New York, New York; and.
⁵ 5Sema4, A Mount Sinai venture, Stamford, Connecticut.

PMID: 35104796
DOI: 10.3171/2021.11.FOCUS21592

Abstract

Objective: Prior studies have demonstrated a relationship between underlying tumor genetics and lymphocyte infiltration in meningiomas. In this study, the authors aimed to further characterize the relationship between meningioma genomics, CD4+ and CD8+ T-cell infiltration, and oncological outcomes of meningiomas. Understanding specific characteristics of the inflammatory infiltration could have implications for treatment and prognostication.

Methods: Immunohistochemically stained meningioma slides were reviewed to assess the CD4+ and CD8+ cell infiltration burden. The relationship between immune cell infiltration and tumor genomics was then assessed using an adjusted ANOVA model. For a specific gene identified by the ANOVA, the relationship between that mutation and tumor recurrence was assessed using Cox regression.

Results: In immunohistochemically stained samples from a subcohort of 25 patients, the mean number of CD4+ cells was 42.2/400× field and the mean number of CD8+ cells was 69.8/400× field. Elevated CD8+ cell infiltration was found to be associated with the presence of a mutation in the gene encoding for DNA polymerase epsilon, POLE (51.6 cells/hpf in wild-type tumors vs 95.9 cells/hpf in mutant tumors; p = 0.0199). In a retrospective cohort of 173 patients, the presence of any mutation in POLE was found to be associated with a 46% reduction in hazard of progression (HR 0.54, 95% CI 0.311-0.952; p = 0.033). The most frequent mutation was a near-C-terminal nonsense mutation.

Conclusions: A potential association was found between mutant POLE and both an increase in CD8+ cell infiltration and progression-free survival. The predominant mutation was found outside of the known exonuclease hot spot; however, it was still associated with a slight increase in mutational burden, CD8+ cell infiltration, and progression-free survival. Alterations in gene expression, resulting from alterations in POLE, may yield an increased presentation of neoantigens, and, thus, greater CD8+ cell-mediated apoptosis of neoplastic cells. These findings have suggested the utility of checkpoint inhibitors in the treatment of POLE-mutant meningiomas.

Keywords: DNA sequencing; POLE; immune response; immunotherapy; meningioma; molecular genetics.

MeSH terms

CD8-Positive T-Lymphocytes
DNA Polymerase II / genetics
Humans
Meningeal Neoplasms* / genetics
Meningioma* / genetics
Mutation / genetics
Neoplasm Recurrence, Local
Progression-Free Survival
Retrospective Studies

Substances

DNA Polymerase II