Significance of P2X7 Receptor Variants to Human Health and Disease

Sluyter, Ronald; Stokes, Leanne

doi:10.2174/187221511794839219

Cited by 125 publications

(119 citation statements)

References 141 publications

(162 reference statements)

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“…The receptor exists in several splice isoforms (A–J) and single nucleotide polymorphisms (SNPs) correlate with several diseases 11, 12. The P2X7R is a ligand‐gated ion channel permeable to Ca 2+ , K + and Na + 13.…”

Section: Introductionmentioning

confidence: 99%

Targeting of the P2X7 receptor in pancreatic cancer and stellate cells

Giannuzzo

Saccomano

Napp

et al. 2016

Intl Journal of Cancer

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The ATP‐gated receptor P2X7 (P2X7R) is involved in regulation of cell survival and has been of interest in cancer field. Pancreatic ductal adenocarcinoma (PDAC) is a deadly cancer and new markers and therapeutic targets are needed. PDAC is characterized by a complex tumour microenvironment, which includes cancer and pancreatic stellate cells (PSCs), and potentially high nucleotide/side turnover. Our aim was to determine P2X7R expression and function in human pancreatic cancer cells in vitro as well as to perform in vivo efficacy study applying P2X7R inhibitor in an orthotopic xenograft mouse model of PDAC. In the in vitro studies we show that human PDAC cells with luciferase gene (PancTu‐1 Luc cells) express high levels of P2X7R protein. Allosteric P2X7R antagonist AZ10606120 inhibited cell proliferation in basal conditions, indicating that P2X7R was tonically active. Extracellular ATP and BzATP, to which the P2X7R is more sensitive, further affected cell survival and confirmed complex functionality of P2X7R. PancTu‐1 Luc migration and invasion was reduced by AZ10606120, and it was stimulated by PSCs, but not by PSCs from P2X7‐/‐ animals. PancTu‐1 Luc cells were orthotopically transplanted into nude mice and tumour growth was followed noninvasively by bioluminescence imaging. AZ10606120‐treated mice showed reduced bioluminescence compared to saline‐treated mice. Immunohistochemical analysis confirmed P2X7R expression in cancer and PSC cells, and in metaplastic/neoplastic acinar and duct structures. PSCs number/activity and collagen deposition was reduced in AZ10606120‐treated tumours.

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Section: Introductionmentioning

confidence: 99%

Targeting of the P2X7 receptor in pancreatic cancer and stellate cells

Giannuzzo

Saccomano

Napp

et al. 2016

Intl Journal of Cancer

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“…Therefore, this receptor may play an important role in the development of various diseased states, including inflammation, neuropathic pain and a number of neurological disorders [7][8][9]. In addition, P2X7 splice variants may alter receptor expression and function [10]. Furthermore, both loss-of-function and gain-of-function P2X7 polymorphisms have been described.…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, both loss-of-function and gain-of-function P2X7 polymorphisms have been described. Some of them are associated with different pathologies, including tuberculosis, Crohn's disease or bipolar affective disorders (reviewed by [10]). Genetically engineered mouse models lacking P2X7 expression in distinct tissues showed an attenuation of the release of pro-inflammatory cytokines [11], thereby decreasing the incidence and severity of arthritis [12] and reducing inflammatory and neuropathic pain sensitivity [13].…”

Section: Introductionmentioning

confidence: 99%

Natural compounds with P2X7 receptor-modulating properties

Fischer

Urban

Immig

et al. 2013

Purinergic Signalling

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The adenosine 5′-triphosphate (ATP)-gated P2X7 receptor is a membrane-bound, non-selective cation channel, expressed in a variety of cell types. The P2X7 senses high extracellular ATP concentrations and seems to be implicated in a wide range of cellular functions as well as pathophysiological processes, including immune responses and inflammation, release of gliotransmitters and cytokines, cancer cell growth or development of neurodegenerative diseases. In the present study, we identified natural compounds and analogues that can block or sensitize the ATP (1 mM)-induced Ca 2+ response using a HEK293 cell line stably expressing human P2X7 and fluorometric imaging plate reader technology. For instance, teniposide potently blocked the human P2X7 at sub-miromolar concentrations, but not human P2X4 or rat P2X2. A marked block of ATPinduced Ca 2+ entry and Yo-Pro-1 uptake was also observed in human A375 melanoma cells and mouse microglial cells, both expressing P2X7. On the other hand, agelasine (AGL) and garcinolic acid (GA) facilitated the P2X7 response to ATP in all three cell populations. GA also enhanced the YO-PRO-1 uptake, whereas AGL did not affect the ATP-stimulated intracellular accumulation of this dye. According to the pathophysiological role of P2X7 in various diseases, selective modulators may have potential for further development, e.g. as neuroprotective or antineoplastic drugs.

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“…P2X7 can be inhibited by broad-spectrum antagonists, including pyridoxalphosphate-6-azophenyl-2',4'-disulfonic acid (PPADS), Reactive Blue 2 and suramin, and by more specific antagonists, including Brilliant Blue G (BBG), KN-62, oxidised ATP and A 438079 [9]. P2X7 activity varies between human individuals and mouse strains due to single nucleotide polymorphisms, resulting in loss or gain of function variants, which can be used to establish the role of this receptor in nucleotide-induced responses [11]. P2Y2 is present on neural, bone, epithelial, endothelial, immune and renal cell types [12].…”

Section: Introductionmentioning

confidence: 99%

Roles of extracellular nucleotides and P2 receptors in ectodomain shedding

Pupovac

Sluyter

2016

Cell. Mol. Life Sci.

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Ectodomain shedding of integral membrane receptors results in the release of soluble molecules and modification of the transmembrane portions to mediate or modulate extracellular and intracellular signalling. Ectodomain shedding is stimulated by a variety of mechanisms, including the activation of P2 receptors by extracellular nucleotides. This review describes in detail the roles of extracellular nucleotides and P2 receptors in the shedding of various cell surface molecules, including amyloid precursor protein, CD23, CD62L, and members of the epidermal growth factor, immunoglobulin and tumour necrosis factor families. This review discusses the mechanisms involved in P2 receptor-mediated shedding, demonstrating central roles for the P2 receptors, P2X7 and P2Y2, and the sheddases, ADAM10 and ADAM17, in this process in a number of cell types.

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Significance of P2X7 Receptor Variants to Human Health and Disease

Cited by 125 publications

References 141 publications

Targeting of the P2X7 receptor in pancreatic cancer and stellate cells

Targeting of the P2X7 receptor in pancreatic cancer and stellate cells

Natural compounds with P2X7 receptor-modulating properties

Roles of extracellular nucleotides and P2 receptors in ectodomain shedding

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