Central Nervous System Immune Interactome Is a Function of Cancer Lineage, Tumor Microenvironment, and STAT3 Expression

Authors

Hinda Najem
Martina Ott
Cynthia Kassab
Arvind Rao
Ganesh Rao
Anantha Marisetty
Adam M Sonabend
Craig Horbinski
Roel Verhaak
Anand Shankar
Santhoshi N Krishnan
Frederick S Varn
Víctor A Arrieta
Pravesh Gupta
Sherise D Ferguson
Jason T Huse
Gregory N Fuller
James P Long
Daniel E Winkowski
Ben A Freiberg
Charles David James
Leonidas C Platanias
Maciej S Lesniak
Jared K Burks
Amy B Heimberger

Publication Date

5-9-2022

Journal

JCI Insight

Abstract

BACKGROUND

Immune cell profiling of primary and metastatic CNS tumors has been focused on the tumor, not the tumor microenvironment (TME), or has been analyzed via biopsies.

METHODS

En bloc resections of gliomas (n = 10) and lung metastases (n = 10) were analyzed via tissue segmentation and high-dimension Opal 7-color multiplex imaging. Single-cell RNA analyses were used to infer immune cell functionality.

RESULTS

Within gliomas, T cells were localized in the infiltrating edge and perivascular space of tumors, while residing mostly in the stroma of metastatic tumors. CD163⁺ macrophages were evident throughout the TME of metastatic tumors, whereas in gliomas, CD68⁺, CD11c⁺CD68⁺, and CD11c⁺CD68⁺CD163⁺ cell subtypes were commonly observed. In lung metastases, T cells interacted with CD163⁺ macrophages as dyads and clusters at the brain-tumor interface and within the tumor itself and as clusters within the necrotic core. In contrast, gliomas typically lacked dyad and cluster interactions, except for T cell CD68⁺ cell dyads within the tumor. Analysis of transcriptomic data in glioblastomas revealed that innate immune cells expressed both proinflammatory and immunosuppressive gene signatures.

CONCLUSION

Our results show that immunosuppressive macrophages are abundant within the TME and that the immune cell interactome between cancer lineages is distinct. Further, these data provide information for evaluating the role of different immune cell populations in brain tumor growth and therapeutic responses.

FUNDING

This study was supported by the NIH (NS120547), a Developmental research project award (P50CA221747), ReMission Alliance, institutional funding from Northwestern University and the Lurie Comprehensive Cancer Center, and gifts from the Mosky family and Perry McKay. Performed in the Flow Cytometry & Cellular Imaging Core Facility at MD Anderson Cancer Center, this study received support in part from the NIH (CA016672) and the National Cancer Institute (NCI) Research Specialist award 1 (R50 CA243707). Additional support was provided by CCSG Bioinformatics Shared Resource 5 (P30 CA046592), a gift from Agilent Technologies, a Research Scholar Grant from the American Cancer Society (RSG-16-005-01), a Precision Health Investigator Award from University of Michigan (U-M) Precision Health, the NCI (R37-CA214955), startup institutional research funds from U-M, and a Biomedical Informatics & Data Science Training Grant (T32GM141746).

Keywords

Brain Neoplasms, Central Nervous System, Glioblastoma, Humans, Lung Neoplasms, Macrophages, STAT3 Transcription Factor, Tumor Microenvironment, United States, Immunology, Oncology, Brain cancer, Innate immunity, T cells

DOI

10.1172/jci.insight.157612

PMID

35316217

PMCID

PMC9090258

PubMedCentral® Posted Date

5-9-2022

PubMedCentral® Full Text Version

Post-print

Published Open-Access

yes