Agonists of toll-like receptor (TLR)2 and TLR4 are unable to modulate platelet activation by adenosine diphosphate and platelet activating factor

Ward, Julian; Bingle, Lynne; Judge, Heather M; Brown, Simon; Storey, Robert F.; Whyte, Moira K. B.; Dower, Steven K.; Buttle, David J.; Sabroe, Ian

doi:10.1160/th05-01-0009

Cited by 126 publications

(129 citation statements)

References 36 publications

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“…19 Platelets have been reported previously to express TLR2 on the surface of 4% to 16% platelets. [14][15][16] However, in our study, these levels were lower with 1.3% to 3% TLR2-positive platelets, which strongly correlated with the percentage of HCMV-bound platelets. Despite the low percentage of TLR2-positive platelets, ≈20% of platelets became P-selectin positive in response to HCMV, indicating that activation of the TLR2-positive subpopulation triggered further platelet activation in a TLR2-independent fashion.…”

Section: Discussioncontrasting

confidence: 64%

“…[13][14][15] Interestingly, not all platelets express TLRs: 55% to 60% are positive for TLR4, 10% to 40% are positive for TLR9, and only 4% to 16% are positive for TLR2. [14][15][16] It was speculated that platelet expression of TLR might be due to the adsorption of free TLR in the plasma. However, megakaryocytes are also positive for TLRs, 14,17 and platelet TLR1/2, TLR4, and TLR9 have been proven to be functional because they trigger intracellular signaling, resulting in platelet activation.…”

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confidence: 99%

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Human Cytomegalovirus–Platelet Interaction Triggers Toll-Like Receptor 2–Dependent Proinflammatory and Proangiogenic Responses

Assinger

Kral

Yaiw

et al. 2014

ATVB

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Objective— Human cytomegalovirus (HCMV) is a widespread pathogen that correlates with various clinical complications, including atherosclerosis. HCMV is released into the circulation during primary infection and periodic viral reactivation, allowing virus–platelet interactions. Platelets are important in the onset and development of atherosclerosis, but the consequences of platelet–HCMV interactions are unclear. Approach and Results— We studied the effects of HCMV–platelet interactions in blood from healthy donors using the purified clinical HCMV isolate VR1814. We demonstrated that HCMV bound to a Toll-like receptor (TLR) 2–positive platelet subpopulation, which resulted in signal transduction, degranulation, and release of proinflammatory CD40L and interleukin-1β and proangiogenic vascular endothelial–derived growth factor. In mice, murine CMV activated wild-type but not TLR2-deficient platelets. However, supernatant from murine CMV–stimulated wild-type platelets also activated TLR2-deficient platelets, indicating that activated platelets generated soluble mediators that triggered further platelet activation, independent of TLR2 expression. Inhibitor studies, using ADP receptor antagonists and apyrase, revealed that ADP release is important to trigger secondary platelet activation in response to HCMV. HCMV-activated platelets rapidly bound to and activated neutrophils, supporting their adhesion and transmigration through endothelial monolayers. In an in vivo model, murine CMV induced systemic upregulation of platelet–leukocyte aggregates and plasma vascular endothelial–derived growth factor in mice and showed a tendency to enhance neutrophil extravasation in a TLR2-dependent fashion. Conclusions— HCMV is a well-adapted pathogen that does not induce immediate thrombotic events. However, HCMV–platelet interactions lead to proinflammatory and proangiogenic responses, which exacerbate tissue damage and contribute to atherogenesis. Therefore, platelets might contribute to the effects of HCMV in accelerating atherosclerosis.

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Section: Discussioncontrasting

confidence: 64%

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confidence: 99%

Human Cytomegalovirus–Platelet Interaction Triggers Toll-Like Receptor 2–Dependent Proinflammatory and Proangiogenic Responses

Assinger

Kral

Yaiw

et al. 2014

ATVB

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“…However, rhodocytin, in our assays, activated DCs primarily via a MyD88-dependent mechanism, possibly due to contamination with TLR agonists, which obscured the putative CLEC-2/Syk-dependent response. This has not been seen in studies with platelets, in which the effect of rhodocytin is completely CLEC-2 dependent [20] but it should be noted that TLR agonists do not induce platelet aggregation [39] such that CLEC-2-independent effects of rhodocytin preparations might not be important for platelet studies. To circumvent this problem, we resorted to using our new mAb to selectively crosslink CLEC-2, inducing Syk-dependent calcium signaling and NFAT activation in both reporter and myeloid cells (Fig.…”

Section: Discussionmentioning

confidence: 93%

CLEC‐2 signaling via Syk in myeloid cells can regulate inflammatory responses

et al. 2011

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Myeloid cells express a plethora of C-type lectin receptors (CLRs) that can regulate immune responses. CLEC-2 belongs to the Dectin-1 sub-family of CLRs that possess an extracellular C-type lectin-like domain and a single intracellular hemITAM motif. CLEC-2 is highly expressed on mouse and human platelets where it signals via Syk to promote aggregation. We generated a monoclonal antibody (mAb) against mouse CLEC-2 and found that CLEC-2 is additionally widely expressed on leukocytes and that its expression is upregulated during inflammation. MAb-mediated crosslinking of CLEC-2 leads to hemI-TAM-dependent signaling via Syk, Ca 21 and NFAT and, in myeloid cells, modulates the effect of toll-like receptor (TLR) agonists to selectively potentiate production of IL-10. A macrophage/dendritic cell-dependent increase in IL-10 is also observed in mice given anti-CLEC-2 mAb together with LPS. Collectively, these data indicate that CLEC-2 is expressed in myeloid cells and acts as a Syk-coupled CLR able to modulate TLR signaling and inflammatory responses.Key words: CLEC-2 . C-type lectin . HemITAM . IL-10 . Syk Supporting Information available online IntroductionSignaling by some members of the C-type lectin receptor (CLR) superfamily plays a key role in innate immunity and in regulation of myeloid cell function [1,2]. A classical example is Dectin-1, which is expressed by macrophages (MØs), neutrophils and dendritic cells (DCs) and acts as a pattern recognition receptor for b-glucans present on fungal and some bacterial cell walls. Dectin-1 signals via a phospho-tyrosine-based hemITAM motif in its intracellular domain that recruits spleen tyrosine kinase (Syk) [3,4]. Dectin-1 signaling through Syk in myeloid cells can variably lead to phagocytosis, production of reactive oxygen species (ROS) and/or induction of innate response genes, including those encoding pro-inflammatory cytokines [5,6]. 3040Pro-inflammatory Dectin-1 signaling requires CARD9-dependent activation of NF-kB [7] although Dectin-1 can also signal to NF-kB via a Syk-independent pathway [8]. Although many DC types are potently activated by Dectin-1 agonists, in other myeloid cells Dectin-1 signaling only weakly activates the proinflammatory gene program [9]. In those cells, Dectin-1 acts primarily in synergy with other innate immune receptors such as toll-like receptors (TLRs) [10,11]. Notably, both Dectin-1 and CARD9 are important for resistance to fungal infection in both mice [7,12,13] and humans [14,15], indicating the importance of the CLR/Syk signaling pathway in immunity.The features of Dectin-1, including type II membrane topology, single Dectin-1-like C-type lectin-like domain and intracellular hemITAM are shared by two other CLRs, DNGR-1 (CLEC9A) and CLEC-2 (CLEC1B). DNGR-1 is selectively expressed by DCs and acts as a receptor for dead cells, facilitating cross-priming to cell-associated antigens [16]. CLEC-2 was first identified in a screen for natural killer (NK) cell receptors and its mRNA was found in myeloid cells and in some NK-cell clones [...

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“…An increasing body of literature supports the role of HA-mediated signaling through several receptors, including CD44, RHAMM, and TLR-2 and TLR-4, all of which are expressed by MKs. 30,57,62 In particular, both RHAMM and . n Z 8 WT and 12 Hyal-2 KO mice (A); n Z 12 (B).…”

Section: Hyal-2 and Efficient Thrombopoiesismentioning

confidence: 99%

Hyaluronan Depolymerization by Megakaryocyte Hyaluronidase-2 Is Required for Thrombopoiesis

Petrey

Obery

Kessler

et al. 2016

The American Journal of Pathology

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Hyaluronan is the predominant glycosaminoglycan component of the extracellular matrix with an emerging role in hematopoiesis. Modulation of hyaluronan polymer size is responsible for its control over cellular functions, and the balance of hyaluronan synthesis and degradation determines its molecular size. Although two active somatic hyaluronidases are expressed in mammals, only deficiency in hyaluronidase-2 (Hyal-2) results in thrombocytopenia of unknown mechanism. Our results reveal that Hyal-2 knockout mice accumulate hyaluronan within their bone marrow and within megakaryocytes, the cells responsible for platelet generation. Proplatelet formation by Hyal-2 knockout megakaryocytes was disrupted because of abnormal formation of the demarcation membrane system, which was dilated and poorly developed. Importantly, peptide-mediated delivery of exogenous hyaluronidase rescued deficient proplatelet formation in murine and human megakaryocytes lacking Hyal-2. Together, our data uncover a previously unsuspected mechanism of how hyaluronan and Hyal-2 control platelet generation.

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Agonists of toll-like receptor (TLR)2 and TLR4 are unable to modulate platelet activation by adenosine diphosphate and platelet activating factor

Cited by 126 publications

References 36 publications

Human Cytomegalovirus–Platelet Interaction Triggers Toll-Like Receptor 2–Dependent Proinflammatory and Proangiogenic Responses

Human Cytomegalovirus–Platelet Interaction Triggers Toll-Like Receptor 2–Dependent Proinflammatory and Proangiogenic Responses

CLEC‐2 signaling via Syk in myeloid cells can regulate inflammatory responses

Hyaluronan Depolymerization by Megakaryocyte Hyaluronidase-2 Is Required for Thrombopoiesis

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