Literature DB >> 30777922

ARTC2.2/P2RX7 Signaling during Cell Isolation Distorts Function and Quantification of Tissue-Resident CD8+ T Cell and Invariant NKT Subsets.

Henrique Borges da Silva1, Haiguang Wang1, Lily J Qian1, Kristin A Hogquist2, Stephen C Jameson2.   

Abstract

Peripheral invariant NKT cells (iNKT) and CD8+ tissue-resident memory T cells (TRM) express high levels of the extracellular ATP receptor P2RX7 in mice. High extracellular ATP concentrations or NAD-mediated P2RX7 ribosylation by the enzyme ARTC2.2 can induce P2RX7 pore formation and cell death. Because both ATP and NAD are released during tissue preparation for analysis, cell death through these pathways may compromise the analysis of iNKT and CD8+ TRM Indeed, ARTC2.2 blockade enhanced recovery of viable liver iNKT and TRM The expression of ARTC2.2 and P2RX7 on distinct iNKT subsets and TRM is unclear, however, as is the impact of recovery from other nonlymphoid sites. In this study, we performed a comprehensive analysis of ARTC2.2 and P2RX7 expression in iNKT and CD8+ T cells in diverse tissues, at steady-state and after viral infection. NKT1 cells and CD8+ TRM express high levels of both ARTC2.2 and P2RX7 compared with NKT2, NKT17, and CD8+ circulating memory subsets. Using nanobody-mediated ARTC2.2 antagonism, we showed that ARTC2.2 blockade enhanced NKT1 and TRM recovery from nonlymphoid tissues during cell preparation. Moreover, blockade of this pathway was essential to preserve functionality, viability, and proliferation of both populations. We also showed that short-term direct P2RX7 blockade enhanced recovery of TRM, although to a lesser degree. In summary, our data show that short-term in vivo blockade of the ARTC2.2/P2RX7 axis permits much improved flow cytometry-based phenotyping and enumeration of murine iNKT and TRM from nonlymphoid tissues, and it represents a crucial step for functional studies of these populations.
Copyright © 2019 by The American Association of Immunologists, Inc.

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Year:  2019        PMID: 30777922      PMCID: PMC6424602          DOI: 10.4049/jimmunol.1801613

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  48 in total

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Authors:  Rachael Bartlett; Leanne Stokes; Ronald Sluyter
Journal:  Pharmacol Rev       Date:  2014-07       Impact factor: 25.468

Review 4.  The P2X7 Receptor in Infection and Inflammation.

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Journal:  Immunity       Date:  2017-07-18       Impact factor: 31.745

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6.  Purinergic control of T cell activation by ATP released through pannexin-1 hemichannels.

Authors:  Ursula Schenk; Astrid M Westendorf; Enrico Radaelli; Anna Casati; Micol Ferro; Marta Fumagalli; Claudia Verderio; Jan Buer; Eugenio Scanziani; Fabio Grassi
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Authors:  S Hashimoto-Hill; L Friesen; M Kim; C H Kim
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Review 10.  How Lipid-Specific T Cells Become Effectors: The Differentiation of iNKT Subsets.

Authors:  Haiguang Wang; Kristin A Hogquist
Journal:  Front Immunol       Date:  2018-06-26       Impact factor: 7.561

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  20 in total

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Journal:  Int Immunol       Date:  2020-09-08       Impact factor: 4.823

3.  Sensing of ATP via the Purinergic Receptor P2RX7 Promotes CD8+ Trm Cell Generation by Enhancing Their Sensitivity to the Cytokine TGF-β.

Authors:  Henrique Borges da Silva; Changwei Peng; Haiguang Wang; Kelsey M Wanhainen; Chaoyu Ma; Sharon Lopez; Alexander Khoruts; Nu Zhang; Stephen C Jameson
Journal:  Immunity       Date:  2020-07-07       Impact factor: 31.745

4.  Control of Tissue-Resident Invariant NKT Cells by Vitamin A Metabolites and P2X7-Mediated Cell Death.

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5.  P2RX7 Enhances Tumor Control by CD8+ T Cells in Adoptive Cell Therapy.

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Review 6.  Metabolic regulation of tissue-resident memory CD8+ T cells.

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7.  TGFβ restricts expansion, survival, and function of T cells within the tuberculous granuloma.

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Journal:  Cell Host Microbe       Date:  2021-03-11       Impact factor: 21.023

8.  Innate cell microenvironments in lymph nodes shape the generation of T cell responses during type I inflammation.

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Review 9.  Divergence of Tissue-Memory T Cells: Distribution and Function-Based Classification.

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10.  Hypoxia acts as an environmental cue for the human tissue-resident memory T cell differentiation program.

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