A Role for Mitogen-activated Protein KinaseErk1/2 Activation and Non-selective Pore Formation in P2X7 Receptor-mediated Thymocyte Death

Auger, Rodolphe; Motta, Iris; Benihoud, Karim; Ojcius, David M.; Kanellopoulos, Jean

doi:10.1074/jbc.m501290200

Cited by 65 publications

(72 citation statements)

References 63 publications

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“…In addition, ␣-fodrin degradation is proposed to contribute to cell blebbing and other morphologic changes (40). Extracellular ATP stimulation is also reported to induce c-Src activation and tyrosine phosphorylation of intracellular proteins (41,42). However, we could not detect degradation in cytoskeletal proteins including ␣-fodrin, actin, c-Src, and Pyk2.…”

Section: Extracellular Atp Alters the Pattern Of Pyk2 Distribution Incontrasting

confidence: 51%

Intracellular and Extracellular ATP Coordinately Regulate the Inverse Correlation between Osteoclast Survival and Bone Resorption

Miyazaki

Iwasawa

Nakashima

et al. 2012

Journal of Biological Chemistry

107

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Background: Mature osteoclasts with a spontaneous tendency toward apoptosis resorb bone efficiently during their short lifespan. Results: Released ATP from intracellular stores has a negative impact on the bone resorption activity of osteoclasts by altering their cytoskeletal structures. Conclusion: ATP depletion leads to osteoclastic bone resorption. Significance: This study provides a new direction for investigating the mechanisms involved in physiological and pathological bone resorption.

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Section: Extracellular Atp Alters the Pattern Of Pyk2 Distribution Incontrasting

confidence: 51%

Intracellular and Extracellular ATP Coordinately Regulate the Inverse Correlation between Osteoclast Survival and Bone Resorption

Miyazaki

Iwasawa

Nakashima

et al. 2012

Journal of Biological Chemistry

107

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“…In contrast, Auger et al (9) reported that ERK1/2 phosphorylation plays a role in P2X 7 receptor-mediated necrotic cell death, and these events are independent of pore formation. Thus, we investigated the contributions of cell shrinkage and the ERK1/2 pathway to P2X 7 receptor-mediated splenocyte death.…”

Section: Dual Signaling Pathways Of P2x 7 Receptor-mediated Cell Deathmentioning

confidence: 94%

“…The P2X 7 receptor C-terminal region of C57BL/6 mice bears a Pro-451 to Leu mutation that impairs nonselective pore formation (30), but there are no differences between the two mouse strains in terms of P2X 7 receptor mRNA and protein expressions, and ATP-induced phosphorylation of ERK1/2 (9). Reduced sensitivity to ATP-induced pore formation, cell shrinkage, and cell death were observed in splenocytes from C57BL/6 mice compared with BALB/c mice (Fig.…”

Section: P2x 7 Receptor-mediated Cell Shrinkage In Lymphocytesmentioning

confidence: 99%

“…In contrast, P2X 7 receptor activation also leads to ERK1/2 phosphorylation (7) and this signaling cascade is dependent on the N terminus (8). Because the inhibition of ERK phosphorylation suppressed P2X 7 receptor-mediated necrotic cell death, an N terminus can also mediate cell death signaling (9). Activation of the P2X 7 receptor induces apoptotic DNA fragmentation, accompanied by the proteolytic processing of multiple caspases and caspase substrates.…”

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confidence: 99%

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P2X7 Receptor-Dependent Cell Death Is Modulated during Murine T Cell Maturation and Mediated by Dual Signaling Pathways

Tsukimoto

Maehata

Hishida

et al. 2006

The Journal of Immunology

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Extracellular ATP causes apoptosis and/or necrosis of the hemopoietic lineage through the activation of P2X7 receptors. In this study, we investigated P2X7 receptor-mediated cell death during murine T cell maturation. The expression level and activity of P2X7 receptors, as measured by induction of cell death and pore formation, were higher in splenocytes than thymocytes. Flow cytometric analysis revealed that cell shrinkage was induced by activation of the P2X7 receptor in murine lymphocytes and the responding cells were T cells. Splenic T cells were more responsive than their thymic counterpart. These observations indicate that the system of P2X7 receptor-mediated cell death in T cells could be modulated during T cell maturation. Furthermore, decreased extracellular Cl− suppressed ATP-induced cell shrinkage in splenocytes without inhibiting ERK1/2 phosphorylation, which is reported to mediate necrotic cell death. Treatment with U0126 (a MEK inhibitor) suppressed ATP-induced ERK1/2 phosphorylation without inhibiting cell shrinkage. Moreover, decreased extracellular Cl− and treatment with U0126 suppressed ATP-induced cell death. These observations indicate that the activation of P2X7 receptor leads to T cell death by two independent pathways, one of which is cell shrinkage dependent and the other of which involves the phosphorylation of ERK1/2. In conclusion, we demonstrate increasing P2X7 receptor activity during T cell maturation and the existence of two essential pathways in P2X7 receptor-mediated T cell death. Our findings suggest that ATP-induced cell death of peripheral T lymphocytes is important in P2X7 receptor-regulated immune responses.

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“…Other important functions where P2X7 has been implicated include killing of mycobacteria and Chlamydia residing inside macrophages [33][34][35], apoptosis of immune cells [14,36,37], cell fusion [38,39] and shedding of the CD62L homing receptor and other membrane proteins including CD23 and CD27 [14,40,41].…”

Section: Introductionmentioning

confidence: 99%

Characterisation of the R276A gain-of-function mutation in the ectodomain of murine P2X7

Adriouch

Scheuplein

Bähring

et al. 2009

Purinergic Signalling

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The cytolytic P2X7 purinoceptor is widely expressed on leukocytes and has sparked interest because of its key role in the activation of the inflammasome, the release of the pro-inflammatory cytokine IL-1β and cell death. We report here the functional characterisation of a R276A gainof-function mutant analysed for its capacities to induce membrane depolarisation, calcium influx and opening of a large membrane pore permeable to YO-PRO-1. Our results highlight the particular sensitivity of R276A mutant to low micromolar adenosine triphosphate (ATP) concentrations, which possibly reflect an increased affinity for its ligands, and a slower closing kinetics of the receptor channel. Our findings support the notion that evolutionary pressures maintain the low sensitivity of P2X7 to ATP. We also believe that the R276A mutant described here may be useful for the generation of new animal models with exacerbated P2X7 functions that will serve to better characterise its role in inflammation and in immune responses.

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A Role for Mitogen-activated Protein KinaseErk1/2 Activation and Non-selective Pore Formation in P2X7 Receptor-mediated Thymocyte Death

Cited by 65 publications

References 63 publications

Intracellular and Extracellular ATP Coordinately Regulate the Inverse Correlation between Osteoclast Survival and Bone Resorption

Intracellular and Extracellular ATP Coordinately Regulate the Inverse Correlation between Osteoclast Survival and Bone Resorption

P2X7 Receptor-Dependent Cell Death Is Modulated during Murine T Cell Maturation and Mediated by Dual Signaling Pathways

Characterisation of the R276A gain-of-function mutation in the ectodomain of murine P2X7

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