Tspan18 is a novel regulator of the Ca<sup>2+</sup> channel Orai1 and von Willebrand factor release in endothelial cells

Noy, Peter J.; Gavin, Rebecca L.; Colombo, Dario; Haining, Elizabeth J.; Reyat, Jasmeet S.; Payne, Holly; Thielmann, Ina; Lokman, Adam; Neag, Georgiana; Yang, Jing; Lloyd, Tammy; Harrison, Neale; Heath, Victoria L.; Gardiner, Chris; Whitworth, Katharine; Robinson, J. A.; Koo, Chek Ziu; Maio, Alessandro Di; Harrison, Paul; Lee, Steven P.; Michelangeli, Francesco; Kalia, Neena; Rainger, G. Ed; Nieswandt, Bernhard; Brill, Alexander; Watson, Steve P.; Tomlinson, Michael G.

doi:10.3324/haematol.2018.194241

Cited by 20 publications

(28 citation statements)

References 59 publications

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“…In the current absence of an effective Tspan18 antibody, we used RT-PCR to demonstrate Tspan18 expression in human endothelial cells, but not most other cell types. This was supported by our analyses of publicly available RNA-Seq data from mouse lung and brain, which showed that Tspan18 is most highly expressed in endothelial cells of these organs [6]. Analysis of single-cell RNA-Seq data from 20 mouse organs provides further support, since 9 of the 14 most highly Tspan18-expressing cell types are endothelial cells (Fig.…”

Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellssupporting

confidence: 57%

“…We further showed that Tspan18 knockdown in primary human umbilical vein endothelial cells (HUVECs) impairs Ca 2+ signaling by 55-70% following stimulation with the GPCR agonists histamine or thrombin, similar to Orai1 knockdown [6]. Orai1 surface localisation is 70% reduced following Tspan18 knockdown, suggesting a role for Tspan18 in trafficking Orai1 from the ER.…”

Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellsmentioning

confidence: 74%

“…In addition to their thrombo-inflammatory phenotypes, Tspan18-knockout mice have a haemostasis defect, as detected by increased blood loss in a tail bleeding assay [6]. Consistent with a role for Tspan18 in endothelial cells, this bleeding phenotype is the result of Tspan18 deletion from non-haematopoietic cells only; this was determined using wild-type/Tspan18-knockout fetal liver chimeric mice [6]. The underlying mechanism remains unclear, since there is no evidence that an acute release of VWF from endothelial cells following injury is critical for haemostasis.…”

Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellsmentioning

confidence: 99%

“…VWF is constitutively released at a relatively low level by WPB exocytosis, but can be acutely exocytosed in larger quantities via a mechanism involving Ca 2+ signaling following endothelial cell activation [5]. We have recently discovered that tetraspanin Tspan18 is important for endothelial cell Ca 2+ signaling, acute VWF release, and thrombo-inflammation, by interacting with the store-operated Ca 2+ entry channel Orai1 and promoting its trafficking to the cell surface [6]. This review will describe our current knowledge of Tspan18 expression and function, and will speculate on the molecular mechanism by which Tspan18 regulates Orai1.…”

Section: Introductionmentioning

confidence: 99%

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Tspan18 is a novel regulator of thrombo-inflammation

Gavin

Koo

Tomlinson

2020

Med Microbiol Immunol

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The interplay between thrombosis and inflammation, termed thrombo-inflammation, causes acute organ damage in diseases such as ischaemic stroke and venous thrombosis. We have recently identified tetraspanin Tspan18 as a novel regulator of thrombo-inflammation. The tetraspanins are a family of 33 membrane proteins in humans that regulate the trafficking, clustering, and membrane diffusion of specific partner proteins. Tspan18 partners with the store-operated Ca 2+ entry channel Orai1 on endothelial cells. Orai1 appears to be expressed in all cells and is critical in health and disease. Orai1 mutations cause human immunodeficiency, resulting in chronic and often lethal infections, while Orai1-knockout mice die at around the time of birth. Orai1 is a promising drug target in autoimmune and inflammatory diseases, and Orai1 inhibitors are in clinical trials. The focus of this review is our work on Tspan18 and Orai1 in Tspan18-knockout mice and Tspan18-knockdown primary human endothelial cells. Orai1 trafficking to the cell surface is partially impaired in the absence of Tspan18, resulting in impaired Ca 2+ signaling and impaired release of the thrombo-inflammatory mediator von Willebrand factor following endothelial stimulation. As a consequence, Tspan18-knockout mice are protected in ischemia-reperfusion and deep vein thrombosis models. We provide new evidence that Tspan18 is relatively highly expressed in endothelial cells, through the analysis of publicly available single-cell transcriptomic data. We also present new data, showing that Tspan18 is required for normal Ca 2+ signaling in platelets, but the functional consequences are subtle and restricted to mildly defective platelet aggregation and spreading induced by the platelet collagen receptor GPVI. Finally, we generate structural models of human Tspan18 and Orai1 and hypothesize that Tspan18 regulates Orai1 Ca 2+ channel function at the cell surface by promoting its clustering.

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Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellssupporting

confidence: 57%

Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellsmentioning

confidence: 74%

Section: Tspan18 Regulates Orai1/ca 2+ Signaling On Endothelial Cellsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Tspan18 is a novel regulator of thrombo-inflammation

Gavin

Koo

Tomlinson

2020

Med Microbiol Immunol

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“…Other recent biomarkers have been or are currently explored for the diagnosis or venous thrombosis and they may be grouped into those with limited or no signal, mixed results or strong results, but they require further validation before considering their use in clinical practice [7,142,143] (Table 4). Although many of these biomarkers are very promising, currently, they cannot be used to make decisions in the management of patients with venous thromboembolism because they do not have an established cut-off point in order to validate them, and most of them have not been used in clinical trials.…”

Section: Other Biomarkersmentioning

confidence: 99%

From Classical Laboratory Parameters to Novel Biomarkers for the Diagnosis of Venous Thrombosis

Anghel

Sascău

Radu

et al. 2020

IJMS

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Venous thrombosis is a common and potentially fatal disease, because of its high morbidity and mortality, especially in hospitalized patients. To establish the diagnosis of venous thrombosis, in the last years, a multi-modality approach that involves not only imaging modalities but also serology has been evolving. Multiple studies have demonstrated the use of some biomarkers, such as D-dimer, selectins, microparticles or inflammatory cytokines, for the diagnosis and treatment of venous thrombosis, but there is no single biomarker available to exclusively confirm the diagnosis of venous thrombosis. Considering the fact that there are some issues surrounding the management of patients with venous thrombosis and the duration of treatment, recent studies support the idea that these biomarkers may help guide the length of appropriate anticoagulation treatment, by identifying patients at high risk of recurrence. At the same time, biomarkers may help predict thrombus evolution, potentially identifying patients that would benefit from more aggressive therapies. This review focuses on classic and novel biomarkers currently under investigation, discussing their diagnostic performance and potential benefit in guiding the therapy for venous thrombosis.

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Tetraspanins in the regulation of mast cell function

Orinska

Hagemann

Hálová

et al. 2020

Med Microbiol Immunol

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Mast cells (MCs) are long-living immune cells highly specialized in the storage and release of different biologically active compounds and are involved in the regulation of innate and adaptive immunity. MC degranulation and replacement of MC granules are accompanied by active membrane remodelling. Tetraspanins represent an evolutionary conserved family of transmembrane proteins. By interacting with lipids and other membrane and intracellular proteins, they are involved in organisation of membrane protein complexes and act as “molecular facilitators” connecting extracellular and cytoplasmic signaling elements. MCs express different tetraspanins and MC degranulation is accompanied by changes in membrane organisation. Therefore, tetraspanins are very likely involved in the regulation of MC exocytosis and membrane reorganisation after degranulation. Antiviral response and production of exosomes are further aspects of MC function characterized by dynamic changes of membrane organization. In this review, we pay a particular attention to tetraspanin gene expression in different human and murine MC populations, discuss tetraspanin involvement in regulation of key MC signaling complexes, and analyze the potential contribution of tetraspanins to MC antiviral response and exosome production. In-depth knowledge of tetraspanin-mediated molecular mechanisms involved in different aspects of the regulation of MC response will be beneficial for patients with allergies, characterized by overwhelming MC reactions.

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Tspan18 is a novel regulator of the Ca²⁺ channel Orai1 and von Willebrand factor release in endothelial cells

Cited by 20 publications

References 59 publications

Tspan18 is a novel regulator of thrombo-inflammation

Tspan18 is a novel regulator of thrombo-inflammation

From Classical Laboratory Parameters to Novel Biomarkers for the Diagnosis of Venous Thrombosis

Tetraspanins in the regulation of mast cell function

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Tspan18 is a novel regulator of the Ca2+ channel Orai1 and von Willebrand factor release in endothelial cells

Cited by 20 publications

References 59 publications

Tspan18 is a novel regulator of thrombo-inflammation

Tspan18 is a novel regulator of thrombo-inflammation

From Classical Laboratory Parameters to Novel Biomarkers for the Diagnosis of Venous Thrombosis

Tetraspanins in the regulation of mast cell function

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Tspan18 is a novel regulator of the Ca²⁺ channel Orai1 and von Willebrand factor release in endothelial cells