Platelet-derived LIGHT induces inflammatory responses in endothelial cells and monocytes

Otterdal, Kari; Smith, Camilla; Øie, Erik; Pedersen, Turid M.; Yndestad, Arne; Stang, Espen; Endresen, Knut; Solum, Nils Olav; Aukrust, Pål; Damås, J

doi:10.1182/blood-2005-09-010629

Cited by 113 publications

(132 citation statements)

References 33 publications

(52 reference statements)

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“…Our findings in experimental HF suggest that this receptor can also be expressed in cardiomyocytes, with particularly high expression in the failing myocardium. LIGHT has been reported to promote several effects relevant to HF, such as production of inflammatory cytokines, matrix degradation, and increased production of reactive oxygen species in leukocytes, endothelial cells, and fibroblasts [13,16,22]; some of these effects seem to involve LIGHT-HVEM interaction. Furthermore, studies in animal models suggest that LIGHT-HVEM interaction may play a major role in inflammatory bowel disease, allograft rejection, and graft-versus-host disease [9].…”

Section: Discussionmentioning

confidence: 99%

“…Primary human umbilical vein endothelial cells (HUVECs) were obtained from umbilical cord veins, cultured as described elsewhere [16], and stimulated with different concentrations of rhLIGHT (R&D Systems). At different time points, cell-free supernatants (PBMC and HUVEC) and cell pellets (HUVEC) were harvested and stored at − 80°C.…”

Section: Cell Culture Experimentsmentioning

confidence: 99%

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Increased expression of LIGHT/TNFSF14 and its receptors in experimental and clinical heart failure☆

Dahl

Gullestad

Fevang

et al. 2008

European J of Heart Fail

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Background: Clinical and experimental studies suggest a pathogenic role for inflammation in chronic heart failure (HF). LIGHT is a member of the tumour necrosis factor superfamily involved in innate and adaptive immune responses. Aims: We sought to investigate a potential pathogenic role of LIGHT in chronic HF. Methods: We used various clinical and experimental approaches including studies in post-infarction HF rats and in vitro studies of endothelial cells and peripheral blood mononuclear cells (PBMC). Results: Our main findings were: (i) LIGHT and its receptors (i.e., HVEM and lymphotoxin-β receptor) were regulated during experimental HF, with strong expression in the infarcted area accompanied by up-regulation of HVEM in cardiomyocytes and endothelial cells also in the non-ischaemic part of the left ventricle. (ii) Patients with chronic HF had significantly increased expression of LIGHT on CD3 + T-cells accompanied by increased expression of HVEM on monocytes and within the failing myocardium. (iii) LIGHT induced interleukin (IL)-6 expression in endothelial cells. In HF patients, but not in healthy controls, such an IL-6-inducing effect was also seen in LIGHT activated PBMC. Conclusion: Our findings in both clinical and experimental HF may suggest a role for LIGHT signalling pathways in the progression of chronic HF involving IL-6-related mechanisms.

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Section: Discussionmentioning

confidence: 99%

Section: Cell Culture Experimentsmentioning

confidence: 99%

Increased expression of LIGHT/TNFSF14 and its receptors in experimental and clinical heart failure☆

Dahl

Gullestad

Fevang

et al. 2008

European J of Heart Fail

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“…Previous data show expression of several TNF family members on platelets (25)(26)(27)(28)(29)(30)(31)(32)(33). In this study we set out to determine whether GITRL was expressed upon in vitro differentiation of megakaryocytes from CD34 + stem cells.…”

Section: Thrombopoietic Cells Express Gitrlmentioning

confidence: 95%

GITR Ligand Provided by Thrombopoietic Cells Inhibits NK Cell Antitumor Activity

Placke

Salih

Kopp

2012

The Journal of Immunology

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Thrombocytopenia inhibits tumor growth and especially metastasis in mice, whereas additional depletion of NK cells reverts this antimetastatic phenotype. It has therefore been speculated that platelets may protect hematogenously disseminating tumor cells from NK-dependent antitumor immunity. Tumor cells do not travel through the blood alone, but are rapidly coated by platelets, and this phenomenon has been proposed to shield disseminating tumor cells from NK-mediated lysis. However, the underlying mechanisms remain largely unclear. In this study, we show that megakaryocytes acquire expression of the TNF family member glucocorticoid-induced TNF-related ligand (GITRL) during differentiation, resulting in GITRL expression by platelets. Upon platelet activation, GITRL is upregulated on the platelet surface in parallel with the α-granular activation marker P-selectin. GITRL is also rapidly mobilized to the platelet surface following interaction with tumor cells, which results in platelet coating. Whereas GITRL, in the fashion of several other TNF family members, is capable of transducing reverse signals, no influence on platelet activation and function was observed upon GITRL triggering. However, platelet coating of tumor cells inhibited NK cell cytotoxicity and IFN-γ production that could partially be restored by blocking GITR on NK cells, thus indicating that platelet-derived GITRL mediates NK-inhibitory forward signaling via GITR. These data identify conferment of GITRL pseudoexpression to tumor cells by platelets as a mechanism by which platelets may alter tumor cell immunogenicity. Our data thus provide further evidence for the involvement of platelets in facilitating evasion of tumor cells from NK cell immune surveillance.

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“…ReleaseofplateletderivedCD40L,which is stored in high amounts in plateletgranules and released within seconds after activation in vitro,induces inflammatoryr esponses in endothelium (9). Ligation of CD40 on endothelialcells (ECs) by CD40Lexpressed on the surfaceof activatedplatelets increased the releaseofinterleukin (IL)-8and monocyte chemoattractant protein 1(MCP-1), major chemoattractantsf or neutrophils and monocytes (9).O nlyr ecently,t he expression of LIGHT (TNFSF1 4, ap rotein,w hich belongs to the tumor necrosis factor super-familya nd causes pro-inflammatoryand pro-thromboticchangesqualitatively comparable to effectsofCD40 ligand) wasidentified on platelets upon exposure to ADP or TRAP-1 (10,11). Platelet-associatedLIGHT influenced adhesion of platelets to the endothelium, while soluble LIGHT inducedapro-inflammatory state in vascularECs, rendering this moleculeapotential therapeutic or diagnostic target in atherosclerosis (11).Asp atients with myocardiali nfarction revealed increased levels of solubleLIGHT,this molecule may be of clinicalimportancefor the pathogenesis of coronaryartery disease ( 11).…”

Section: Platelet Secretion Andgeneration Of Cytokinesmentioning

confidence: 99%

Platelet-vessel wall interactions in atherosclerotic disease

Langer¹,

Gawaz²

2008

Thromb Haemost

191

132

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SummaryDuring the prolonged course of atherosclerotic disease,platelets areofcentral importanceastheycontribute to the initiation of the disease,toi ts progressiona nd acutee xacerbation but also providep otentialr egenerativem echanisms. Platelets secrete chemokinesa nd cytokinest hatm ediatev ascular inflammation andare in turn activated by substances released from cells of the vascularwall.These interactions represent positive andnegative feedback loops, whichincaseofdysregulationmay lead to development andp rogression of disease.Furthermore, platelet adhesion to the endothelium is critical forthe initiation of atherosclerotic lesion formation in vivo.Evenp rior to endotheliald enudation, plateletadhesion governed by disturbedflowatpredilection sites foratherosclerosisinduces recruitment of proatheKeywords Atherothrombosis, plateletphysiology, stemcells rosclerotic cells andrelease of proinflammatory mediators from allinvolved cell types.Finally, the pathogenetic role of platelets for late atheroclerotic eventsincluding plaque rupture,microembolism or spasms withint he microcirculationi sw elle stablished. However, increasing evidence indicatesthatplatelets mediateon the other hand potential regenerativemechanisms. Platelets recruit circulating progenitor cells to sites of vasculari njury. Furthermore,theyinfluencetheir biological activity andmaturation. Therefore,platelets contribute at allstages of vasculardiseaseby interfering with highlyd ynamic processes. Understanding interactions of plateletswith othercirculatingcells andt he vascular wall is aprerequisite to understand cardiovascular disease andto identify potentialtherapeutic targets.

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Platelet-derived LIGHT induces inflammatory responses in endothelial cells and monocytes

Cited by 113 publications

References 33 publications

Increased expression of LIGHT/TNFSF14 and its receptors in experimental and clinical heart failure☆

Increased expression of LIGHT/TNFSF14 and its receptors in experimental and clinical heart failure☆

GITR Ligand Provided by Thrombopoietic Cells Inhibits NK Cell Antitumor Activity

Platelet-vessel wall interactions in atherosclerotic disease

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