P2Y<sub>2</sub> nucleotide receptor activation enhances the aggregation and self-organization of dispersed salivary epithelial cells

El-Sayed, Farid G.; Camden, Jean M.; Woods, Lucas T.; Khalafalla, Mahmoud G.; Petris, Michael J.; Erb, Laurie; Weisman, Gary A.

doi:10.1152/ajpcell.00380.2013

Cited by 13 publications

(15 citation statements)

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“…In rodent salivary glands, P2Y 2 R expression is negligible under physiological conditions. Interestingly, freshly dispersed salivary epithelial cells significantly upregulated P2Y 2 R expression and activity as a function of time when placed in culture El-Sayed et al, 2014), consistent with a possible role for P2Y 2 R in the cellular response to stress. P2Y 2 R upregulation also occurs in the in vivo ductal ligation model of salivary gland inflammation and fibrosis (Ahn et al, 2000) and has been similarly seen in other in vivo models of stress and inflammation, i.e., intestinal inflammation (Grbic et al, 2008), rat vascular neointima formation after balloon angioplasty (Seye et al, 1997), collared rabbit carotid arteries (Seye et al, 2002), glomerulonephritis (Rennert et al, 2018), myocardium of rats with congestive heart failure (Granado et al, 2015) and mouse models of the autoimmune disease SS Woods et al, 2018).…”

Section: The Role Of P2 Receptors In Salivary Gland Inflammationsupporting

confidence: 61%

“…Following de-ligation, residual cells in damaged salivary glands can regenerate the gland through proliferation, migration and self-organization (Takahashi et al, 1998;Man et al, 2001;Kishi et al, 2006;Aure et al, 2015), thereby restoring salivary gland function, i.e., increasing the secretion rate of saliva with a normal ion and protein composition (Scott et al, 1999;Osailan et al, 2006). Concurrent with these glandular changes, functional P2Y 2 R expression, which is very low under homeostatic conditions, is robustly increased in salivary epithelial cells in response to ductal ligation and P2Y 2 R expression returns to basal low levels following de-ligation and subsequent recovery of the salivary gland (Ahn et al, 2000;El-Sayed et al, 2014). These findings are in agreement with previous studies demonstrating P2Y 2 R upregulation in epithelial cells in response to tissue damage and inflammation Schrader et al, 2005;Degagne et al, 2009;Woods et al, 2018), suggesting that the P2Y 2 R is an important component in the repair and regeneration of damaged salivary glands.…”

Section: P2 Receptors In Salivary Gland Regenerationmentioning

confidence: 99%

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P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

et al. 2020

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Although often overlooked in our daily lives, saliva performs a host of necessary physiological functions, including lubricating and protecting the oral cavity, facilitating taste sensation and digestion and maintaining tooth enamel. Therefore, salivary gland dysfunction and hyposalivation, often resulting from pathogenesis of the autoimmune disease Sjögren's syndrome or from radiotherapy of the head and neck region during cancer treatment, severely reduce the quality of life of afflicted patients and can lead to dental caries, periodontitis, digestive disorders, loss of taste and difficulty speaking. Since their initial discovery in the 1970s, P2 purinergic receptors for extracellular nucleotides, including ATP-gated ion channel P2X and G protein-coupled P2Y receptors, have been shown to mediate physiological processes in numerous tissues, including the salivary glands where P2 receptors represent a link between canonical and non-canonical saliva secretion. Additionally, extracellular nucleotides released during periods of cellular stress and inflammation act as a tissue alarmin to coordinate immunological and tissue repair responses through P2 receptor activation. Accordingly, P2 receptors have gained widespread clinical interest with agonists and antagonists either currently undergoing clinical trials or already approved for human use. Here, we review the contributions of P2 receptors to salivary gland function and describe their role in salivary gland dysfunction. We further consider their potential as therapeutic targets to promote physiological saliva flow, prevent salivary gland inflammation and enhance tissue regeneration.

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Section: The Role Of P2 Receptors In Salivary Gland Inflammationsupporting

confidence: 61%

Section: P2 Receptors In Salivary Gland Regenerationmentioning

confidence: 99%

P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

et al. 2020

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“…These results reinforce the emerging view of P2Y 2 R as pro-proliferative in various experimental models including hepatocytes 15, 44 , corneal endothelial cells 45 and pancreatic duct epithelial cells 46 . In addition, P2Y 2 R-induced migration in hCPCs is consistent with pro-migratory responses of P2Y 2 R in fibroblasts 24 , salivary 14 and corneal epithelial cells 13 . Whether ex vivo manipulation of hCPCs by UTP preconditioning or P2Y 2 R overexpression improves transplanted hCPC homing, expansion and overall reparative potential for injured myocardium remains to be assessed.…”

Section: Discussionsupporting

confidence: 71%

“…P2Y 2 R plays a central role in intracellular signaling by enabling extracellular ATP and UTP to promote regenerative responses in a variety of tissues. P2Y 2 R regulates corneal epithelia wound healing 13 and salivary gland reconstitution 14 by inducing cell migration, liver regeneration by promoting hepatocyte proliferation 15 , and reepithelialization following experimental colitis 16 and inflammatory bowel disease 17 . On the stem cell level, UTP is a potent stimulant of human hematopoietic stem cell (hHSC) migration 18 .…”

Section: Introductionmentioning

confidence: 99%

P2Y ₂ Nucleotide Receptor Prompts Human Cardiac Progenitor Cell Activation by Modulating Hippo Signaling

Khalafalla

Greene

Khan

et al. 2017

Circulation Research

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Rationale Autologous stem cell therapy using human c-Kit+ cardiac progenitor cells (hCPCs) is a promising therapeutic approach for treatment of heart failure (HF). However, hCPCs derived from aged HF patients with genetic predispositions and/or comorbidities of chronic diseases exhibit poor proliferative and migratory capabilities, which impairs overall reparative potential for injured myocardium. Therefore, empowering functionally compromised hCPCs with pro-regenerative molecules ex vivo is crucial for improving the therapeutic outcome in HF patients. Objective To improve hCPC proliferation and migration responses that are critical for regeneration by targeting pro-regenerative P2Y2 nucleotide receptor (P2Y2R) activated by extracellular ATP and UTP molecules released following injury/stress. Methods and Results c-Kit+ hCPCs were isolated from cardiac tissue of HF patients undergoing left ventricular assist device (LVAD) implantation surgery. Correlations between P2 nucleotide receptor expression and hCPC growth kinetics revealed downregulation of select P2 receptors, including P2Y2R, in slow-growing hCPCs compared to fast-growers. hCPC proliferation and migration significantly improved by overexpressing or stimulating P2Y2R. Mechanistically, P2Y2R-induced proliferation and migration were dependent upon activation of yes-associated protein (YAP), the downstream effector of Hippo signaling pathway. Conclusions Proliferation and migration of functionally impaired hCPCs are enhanced by P2Y2R-mediated YAP activation, revealing a novel link between extracellular nucleotides released during injury/stress and Hippo signaling, a central regulator of cardiac regeneration. Functional correlations exist between hCPC phenotypic properties and P2 purinergic receptor expression. Lack of P2Y2R and other crucial purinergic stress detectors could compromise hCPC responsiveness to presence of extracellular stress signals. These findings set the stage for subsequent studies to assess purinergic signaling modulation as a potential strategy to improve therapeutic outcome for use of hCPCs in HF patients.

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“…Also within the C-terminus of the P2Y 2 R, two Src-homology-3 (SH3) binding sites directly interact with and activate the tyrosine kinase Src, enabling P2Y 2 R-mediated transactivation of growth factor receptors, including the EGFR (Liu et al, 2004). Lastly, the P2Y 2 R has been shown to activate the α-secretases, ADAM10 and ADAM17, which promotes the release of membrane-bound receptor ligands, including growth factors (Ratchford et al, 2010; El-Sayed et al, 2014), and the cleavage of APP to form non-amyloidogenic sAPPα peptide (Camden et al, 2005; Kong et al, 2009). …”

Section: P2 Receptors In Alzheimer’s Diseasementioning

confidence: 99%

Purinergic receptors as potential therapeutic targets in Alzheimer's disease

et al. 2016

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Alzheimer’s disease (AD) is a neurodegenerative disorder characterized by a progressive loss of memory and cognitive ability and is a serious cause of mortality. Many of the pathological characteristics associated with AD are revealed post-mortem, including amyloid-β plaque deposition, neurofibrillary tangles containing hyperphosphorylated tau proteins and neuronal loss in the hippocampus and cortex. Although several genetic mutations and risk factors have been associated with the disease, the causes remain poorly understood. Study of disease-initiating mechanisms and AD progression in humans is inherently difficult as most available tissue specimens are from late-stages of disease. Therefore, AD researchers rely on in vitro studies and the use of AD animal models where neuroinflammation has been shown to be a major characteristic of AD. Purinergic receptors are a diverse family of proteins consisting of P1 adenosine receptors and P2 nucleotide receptors for ATP, UTP and their metabolites. This family of receptors has been shown to regulate a wide range of physiological and pathophysiological processes, including neuroinflammation, and may contribute to the pathogenesis of neurodegenerative diseases like Parkinson’s disease, multiple sclerosis and AD. Experimental evidence from human AD tissue has suggested that purinergic receptors may play a role in AD progression and studies using selective purinergic receptor agonists and antagonists in vitro and in AD animal models have demonstrated that purinergic receptors represent novel therapeutic targets for the treatment of AD.

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P2Y₂ nucleotide receptor activation enhances the aggregation and self-organization of dispersed salivary epithelial cells

Cited by 13 publications

References 133 publications

P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

P2Y ₂ Nucleotide Receptor Prompts Human Cardiac Progenitor Cell Activation by Modulating Hippo Signaling

Purinergic receptors as potential therapeutic targets in Alzheimer's disease

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P2Y2 nucleotide receptor activation enhances the aggregation and self-organization of dispersed salivary epithelial cells

Cited by 13 publications

References 133 publications

P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

P2 Receptors as Therapeutic Targets in the Salivary Gland: From Physiology to Dysfunction

P2Y 2 Nucleotide Receptor Prompts Human Cardiac Progenitor Cell Activation by Modulating Hippo Signaling

Purinergic receptors as potential therapeutic targets in Alzheimer's disease

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Product

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P2Y₂ nucleotide receptor activation enhances the aggregation and self-organization of dispersed salivary epithelial cells

P2Y ₂ Nucleotide Receptor Prompts Human Cardiac Progenitor Cell Activation by Modulating Hippo Signaling