Circulation of gut-preactivated naïve CD8+T cells enhances antitumor immunity in B cell-defective mice

Author:

Akrami MaryamORCID,Menzies Rosemary,Chamoto Kenji,Miyajima Michio,Suzuki Ryuji,Sato HiroyukiORCID,Nishii Akiko,Tomura Michio,Fagarasan Sidonia,Honjo TasukuORCID

Abstract

The gut microbiome has garnered attention as an effective target to boost immunity and improve cancer immunotherapy. We found that B cell-defective (BCD) mice, such as µ-membrane targeted deletion (µMT) and activation-induced cytidine deaminase (AID) knockouts (KOs), have elevated antitumor immunity under specific pathogen-free but not germ-free conditions. Microbial dysbiosis in these BCD mice enriched the type I IFN (IFN) signature in mucosal CD8+T cells, resulting in up-regulation of the type I IFN-inducible protein stem cell antigen-1 (Sca-1). Among CD8+T cells, naïve cells predominantly circulate from the gut to the periphery, and those that had migrated from the mesenteric lymph nodes (mLNs) to the periphery had significantly higher expression of Sca-1. The gut-educated Sca-1+naïve subset is endowed with enhanced mitochondrial activity and antitumor effector potential. The heterogeneity and functional versatility of the systemic naïve CD8+T cell compartment was revealed by single-cell analysis and functional assays of CD8+T cell subpopulations. These results indicate one of the potential mechanisms through which microbial dysbiosis regulates antitumor immunity.

Funder

Japan Agency for Medical Research and Development

Tang Prize Foundation

Bristol-Myers Squibb Research Grants

JSPS KAKENHI

Honjo International Scholarship Foundation

MEXT Scholarship

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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