P2X7 is expressed on human innate‐like T lymphocytes and mediates susceptibility to ATP‐induced cell death

Winzer, Riekje; Prat, Arnau Serracant; Brock, Valerie J.; Pinto-Espinoza, Carolina; Rissiek, Björn; Amadi, Miriam; Eich, Niklas; Rissiek, Anne; Schneider, Enja; Magnus, Tim; Guse, Andreas H.; Diercks, Björn‐Philipp; Koch-Nolte, Friedrich

doi:10.1002/eji.202249932

Cited by 9 publications

(7 citation statements)

References 76 publications

(104 reference statements)

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“…Native-like T cells effectively respond to innate stimuli by secreting a multitude of pro-inflammatory cytokines, and human T cell compartments exhibit the highest expression of the P2X7R. Within the innate lymphoid population, Tγδ cells demonstrate heightened sensitivity to P2X7R activation compared to conventional T cells, influencing fundamental cellular mechanisms such as calcium signaling and AICD[ 36 ]. Neuroinflammation is positively linked to P2X7R activation through risk-associated molecular patterns, with eATP being the most prominent among them.…”

Section: Aicd Mechanismsmentioning

confidence: 99%

Adenosine triphosphate induced cell death: Mechanisms and implications in cancer biology and therapy

Zhang,

Sandai,

Zhang

et al. 2023

World J Clin Oncol

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Adenosine triphosphate ( ATP) induced cell death (AICD) is a critical cellular process that has garnered substantial scientific interest for its profound relevance to cancer biology and to therapeutic interventions. This comprehensive review unveils the intricate web of AICD mechanisms and their intricate connections with cancer biology. This review offers a comprehensive framework for comprehending the multifaceted role of AICD in the context of cancer. This is achieved by elucidating the dynamic interplay between systemic and cellular ATP homeostasis, deciphering the intricate mechanisms governing AICD, elucidating its intricate involvement in cancer signaling pathways, and scrutinizing validated key genes. Moreover, the exploration of AICD as a potential avenue for cancer treatment underscores its essential role in shaping the future landscape of cancer therapeutics.

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Section: Aicd Mechanismsmentioning

confidence: 99%

Adenosine triphosphate induced cell death: Mechanisms and implications in cancer biology and therapy

Zhang,

Sandai,

Zhang

et al. 2023

World J Clin Oncol

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“…Nonetheless, several overarching mechanisms have been revealed. First, the activation of purinergic receptors, particularly the P2X purinoceptor 7 receptor (P2X7R), has emerged as a pivotal mechanism, triggering a cascade of events culminating in cell death[ 8 , 24 ]. Second, a significant mechanism of AICD involves the elevation of intracellular calcium ion concentration[ 25 , 26 ].…”

Section: Introductionmentioning

confidence: 99%

“…Second, a significant mechanism of AICD involves the elevation of intracellular calcium ion concentration[ 25 , 26 ]. Moreover, AICD may also be linked to the activation of inflammatory responses[ 8 ]. Finally, the disruption of mitochondrial function is crucial in AICD, with cytochrome c release intimately connected with the activation of apoptosis signaling pathways[ 27 - 29 ].…”

Section: Introductionmentioning

confidence: 99%

Elucidating the molecular basis of ATP-induced cell death in breast cancer: Construction of a robust prognostic model

Zhang,

Doblin,

Zhang

et al. 2024

World J Clin Oncol

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BACKGROUND Breast cancer is a multifaceted and formidable disease with profound public health implications. Cell demise mechanisms play a pivotal role in breast cancer pathogenesis, with ATP-triggered cell death attracting mounting interest for its unique specificity and potential therapeutic pertinence. AIM To investigate the impact of ATP-induced cell death (AICD) on breast cancer, enhancing our understanding of its mechanism. METHODS The foundational genes orchestrating AICD mechanisms were extracted from the literature, underpinning the establishment of a prognostic model. Simultaneously, a microRNA (miRNA) prognostic model was constructed that mirrored the gene-based prognostic model. Distinctions between high- and low-risk cohorts within mRNA and miRNA characteristic models were scrutinized, with the aim of delineating common influence mechanisms, substantiated through enrichment analysis and immune infiltration assessment. RESULTS The mRNA prognostic model in this study encompassed four specific mRNAs: P2X purinoceptor 4, pannexin 1, caspase 7, and cyclin 2. The miRNA prognostic model integrated four pivotal miRNAs: hsa-miR-615-3p, hsa-miR-519b-3p, hsa-miR-342-3p, and hsa-miR-324-3p. B cells, CD4+ T cells, CD8+ T cells, endothelial cells, and macrophages exhibited inverse correlations with risk scores across all breast cancer subtypes. Furthermore, Kyoto Encyclopedia of Genes and Genomes analysis revealed that genes differentially expressed in response to mRNA risk scores significantly enriched 25 signaling pathways, while miRNA risk scores significantly enriched 29 signaling pathways, with 16 pathways being jointly enriched. CONCLUSION Of paramount significance, distinct mRNA and miRNA signature models were devised tailored to AICD, both potentially autonomous prognostic factors. This study's elucidation of the molecular underpinnings of AICD in breast cancer enhances the arsenal of potential therapeutic tools, offering an unparalleled window for innovative interventions. Essentially, this paper reveals the hitherto enigmatic link between AICD and breast cancer, potentially leading to revolutionary progress in personalized oncology.

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“…Mice and humans differ in their expression and regulation of P2 receptors, particularly with respect to P2X7. P2X7 is expressed at lower levels in humans (at least on circulating T cells) than in mice, as shown, for example, for Tregs, which have a very high P2X7 expression in mice, but low expression in humans [ 189 , 190 ]. Compared to rodent P2X7, human P2X7 is around ten times less sensitive to ATP [ 58 ] and requires ATP concentrations in the high micromolar to low millimolar range for activation [ 191 ].…”

Section: Introductionmentioning

confidence: 99%

The role of the ATP-adenosine axis in ischemic stroke

et al. 2023

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In ischemic stroke, the primary neuronal injury caused by the disruption of energy supply is further exacerbated by secondary sterile inflammation. The inflammatory cascade is largely initiated by the purine adenosine triphosphate (ATP) which is extensively released to the interstitial space during brain ischemia and functions as an extracellular danger signaling molecule. By engaging P2 receptors, extracellular ATP activates microglia leading to cytokine and chemokine production and subsequent immune cell recruitment from the periphery which further amplifies post-stroke inflammation. The ectonucleotidases CD39 and CD73 shape and balance the inflammatory environment by stepwise degrading extracellular ATP to adenosine which itself has neuroprotective and anti-inflammatory signaling properties. The neuroprotective effects of adenosine are mainly mediated through A1 receptors and inhibition of glutamatergic excitotoxicity, while the anti-inflammatory capacities of adenosine have been primarily attributed to A2A receptor activation on infiltrating immune cells in the subacute phase after stroke. In this review, we summarize the current state of knowledge on the ATP-adenosine axis in ischemic stroke, discuss contradictory results, and point out potential pitfalls towards translating therapeutic approaches from rodent stroke models to human patients.

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P2X7 is expressed on human innate‐like T lymphocytes and mediates susceptibility to ATP‐induced cell death

Cited by 9 publications

References 76 publications

Adenosine triphosphate induced cell death: Mechanisms and implications in cancer biology and therapy

Adenosine triphosphate induced cell death: Mechanisms and implications in cancer biology and therapy

Elucidating the molecular basis of ATP-induced cell death in breast cancer: Construction of a robust prognostic model

The role of the ATP-adenosine axis in ischemic stroke

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