The Extracellular ATP Receptor P2RX7 Imprints a Promemory Transcriptional Signature in Effector CD8+ T Cells

Author:

Vardam-Kaur Trupti1ORCID,van Dijk Sarah1ORCID,Peng Changwei2ORCID,Wanhainen Kelsey M.2,Jameson Stephen C.2ORCID,Borges da Silva Henrique1ORCID

Affiliation:

1. *Department of Immunology, Mayo Clinic Arizona, Scottsdale, AZ; and

2. †Center for Immunology, Department of Laboratory Medicine and Pathology, University of Minnesota, Minneapolis, MN

Abstract

Abstract Development of CD8+ central memory T (Tcm) and resident memory T (Trm) cells, which promote immunity in the circulation and in barrier tissues, respectively, is not completely understood. Tcm and Trm cells may arise from common precursors; however, their fate-inducing signals are elusive. We found that virus-specific effector CD8+ T cells display heterogeneous expression of the extracellular ATP sensor P2RX7. P2RX7-high expression is confined, at peak effector phase, to CD62L+ memory precursors, which preferentially form Tcm cells. Among early effector CD8+ T cells, asymmetrical P2RX7 distribution correlated with distinct transcriptional signatures, with P2RX7-high cells enriched for memory and tissue residency sets. P2RX7-high early effectors preferentially form both Tcm and Trm cells. Defective Tcm and Trm cell formation in P2RX7 deficiency is significantly reverted when the transcriptional repressor Zeb2 is ablated. Mechanistically, P2RX7 negatively regulates Zeb2 expression, at least partially through TGF-β sensing in early effector CD8+ T cells. Our study indicates that unequal P2RX7 upregulation in effector CD8+ T cells is a foundational element of the early Tcm/Trm fate.

Funder

HHS | NIH | National Institute of Allergy and Infectious Diseases

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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