Brilliant blue G, a P2X7 receptor antagonist, attenuates early phase of renal inflammation, interstitial fibrosis and is associated with renal cell proliferation in ureteral obstruction in rats

Pereira, José Monteiro Sad; Barreira, André Luis; Gomes, Conrado Rodrigues; Ornellas, Felipe M.; Ornellas, Débora S.; Miranda, Luiz Carlos; Cardoso, Lucio R.; Coutinho‐Silva, Robson; Schanaider, Alberto; Morales, Marcelo M.; Leite, Maurilo; Takiya, Christina Maeda

doi:10.1186/s12882-020-01861-2

Cited by 14 publications

(11 citation statements)

References 33 publications

(48 reference statements)

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“…Our experiments in both T1D and T2D podocytes with specific inhibitors provide compelling evidence that P2X 4 and P2X 7 receptors play a major role in ATP-induced [Ca 2+ ] i levels in diabetic podocytes. Previous research has established that P2X 7 receptor expression increases are linked to PKD, glomerulonephritis, human lupus nephritis, and hypertension-associated renal injury ( Arkhipov et al., 2019 ; Hillman et al., 2005 ; Pereira et al., 2020 ; Vallon et al., 2020 ). In addition, the upregulation of glomerular P2X 7 receptor mRNA and protein expression has been reported in STZ-induced diabetic and ren-2 transgenic hypertensive rat models, and was associated with inflammatory cytokine release and cell death ( Vonend et al., 2004a ).…”

Section: Discussionmentioning

confidence: 99%

“…In addition, the upregulation of glomerular P2X 7 receptor mRNA and protein expression has been reported in STZ-induced diabetic and ren-2 transgenic hypertensive rat models, and was associated with inflammatory cytokine release and cell death ( Vonend et al., 2004a ). Studies have also shown that pharmacological inhibition or deletion of P2X 7 receptor offers varying degrees of protection in these pathologies ( Arkhipov et al., 2019 ; Ji et al., 2012 ; Menzies et al., 2015 , 2017a , 2017b ; Pereira et al., 2020 ; Taylor et al., 2009b ). Here we show that podocytes in late-stage diabetes mellitus have direct ionotropic P2 calcium entry through the pore-forming P2X 4 , and P2X 7 channels in addition to metabotropic signaling through P2Y 1 .…”

Section: Discussionmentioning

confidence: 99%

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Characterization of purinergic receptor 2 signaling in podocytes from diabetic kidneys

et al. 2021

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Summary Growing evidence suggests that renal purinergic signaling undergoes significant remodeling during pathophysiological conditions such as diabetes. This study examined the renal P2 receptor profile and ATP-mediated calcium response from podocytes in glomeruli from kidneys with type 1 or type 2 diabetic kidney disease (DKD), using type 2 diabetic nephropathy (T2DN) rats and streptozotocin-injected Dahl salt-sensitive (type 1 diabetes) rats. A dramatic increase in the ATP-mediated intracellular calcium flux in podocytes was observed in both models. Pharmacological inhibition established that P2X 4 and P2X 7 are the major receptors contributing to the augmented ATP-mediated intracellular calcium signaling in diabetic podocytes. The transition in purinergic receptor composition from metabotropic to ionotropic may disrupt intracellular calcium homeostasis in podocytes resulting in their dysfunction and potentially further aggravating DKD progression.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Characterization of purinergic receptor 2 signaling in podocytes from diabetic kidneys

et al. 2021

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“…Multiple studies indicate that the activation of P2X7Rs in macrophages is involved in peripheral inflammatory diseases, including rheumatoid arthritis [ 53 ], Crohn’s disease [ 108 ], liver fibrosis [ 109 , 110 ], sepsis [ 101 , 111 ], renal inflammation [ 112 , 113 ], and pulmonary inflammation [ 114 ]. Almost all peripheral inflammatory diseases share the same, classic inflammatory pathway in macrophages with the following components: P2X7R stimulation, NLRP3 and caspase-1 activation, and IL-1β/IL-18 release.…”

Section: Peripheral Inflammatory Diseasesmentioning

confidence: 99%

Inherent P2X7 Receptors Regulate Macrophage Functions during Inflammatory Diseases

Ren

Rubini

Tang

et al. 2021

IJMS

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Macrophages are mononuclear phagocytes which derive either from blood-borne monocytes or reside as resident macrophages in peripheral (Kupffer cells of the liver, marginal zone macrophages of the spleen, alveolar macrophages of the lung) and central tissue (microglia). They occur as M1 (pro-inflammatory; classic) or M2 (anti-inflammatory; alternatively activated) phenotypes. Macrophages possess P2X7 receptors (Rs) which respond to high concentrations of extracellular ATP under pathological conditions by allowing the non-selective fluxes of cations (Na+, Ca2+, K+). Activation of P2X7Rs by still higher concentrations of ATP, especially after repetitive agonist application, leads to the opening of membrane pores permeable to ~900 Da molecules. For this effect an interaction of the P2X7R with a range of other membrane channels (e.g., P2X4R, transient receptor potential A1 [TRPA1], pannexin-1 hemichannel, ANO6 chloride channel) is required. Macrophage-localized P2X7Rs have to be co-activated with the lipopolysaccharide-sensitive toll-like receptor 4 (TLR4) in order to induce the formation of the inflammasome 3 (NLRP3), which then activates the pro-interleukin-1β (pro-IL-1β)-degrading caspase-1 to lead to IL-1β release. Moreover, inflammatory diseases (e.g., rheumatoid arthritis, Crohn’s disease, sepsis, etc.) are generated downstream of the P2X7R-induced upregulation of intracellular second messengers (e.g., phospholipase A2, p38 mitogen-activated kinase, and rho G proteins). In conclusion, P2X7Rs at macrophages appear to be important targets to preserve immune homeostasis with possible therapeutic consequences.

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“…P2X7 receptor is an ATP-gated purinergic ion channel widely present in different cells and tissues, such as stem cells [ 1 ], brain [ 2 ], intestine [ 3 ], kidney [ 4 ] and mostly expressed in immune [ 5 ] and several cancer cells [ 6 , 7 , 8 ].…”

Section: Introductionmentioning

confidence: 99%

Cancer Metabostemness and Metabolic Reprogramming via P2X7 Receptor

Rabelo

Arnaud-Sampaio

Adinolfi

et al. 2021

Cells

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The heterogeneity of tumor cell mass and the plasticity of cancer cell phenotypes in solid tumors allow for the insurgence of resistant and metastatic cells, responsible for cancer patients’ clinical management’s main challenges. Among several factors that are responsible for increased cancer aggression, metabolic reprogramming is recently emerging as an ultimate cancer hallmark, as it is central for cancer cell survival and self-renewal, metastasis and chemoresistance. The P2X7 receptor, whose expression is upregulated in many solid and hematological malignancies, is also emerging as a good candidate in cancer metabolic reprogramming and the regulation of stem cell proliferation and differentiation. Metabostemness refers to the metabolic reprogramming of cancer cells toward less differentiated (CSCs) cellular states, and we believe that there is a strong correlation between metabostemness and P2X7 receptor functions in oncogenic processes. Here, we summarize important aspects of P2X7 receptor functions in normal and tumor tissues as well as essential aspects of its structure, regulation, pharmacology and its clinical use. Finally, we review current knowledge implicating P2X7 receptor functions in cancer-related molecular pathways, in metabolic reprogramming and in metabostemness.

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Brilliant blue G, a P2X7 receptor antagonist, attenuates early phase of renal inflammation, interstitial fibrosis and is associated with renal cell proliferation in ureteral obstruction in rats

Cited by 14 publications

References 33 publications

Characterization of purinergic receptor 2 signaling in podocytes from diabetic kidneys

Characterization of purinergic receptor 2 signaling in podocytes from diabetic kidneys

Inherent P2X7 Receptors Regulate Macrophage Functions during Inflammatory Diseases

Cancer Metabostemness and Metabolic Reprogramming via P2X7 Receptor

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