Platelet Interaction with Innate Immune Cells

Kral, Julia B.; Schrottmaier, Waltraud C.; Salzmann, Manuel; Assinger, Alice

doi:10.1159/000444807

Cited by 203 publications

(198 citation statements)

References 117 publications

(136 reference statements)

Supporting

Mentioning

182

Contrasting

Unclassified

Order By: Relevance

“…The exact mechanisms inducing platelet activation and then formation of PMPs in cancer are not well understood, but it seems that there is a direct activation by the tumoral cells releasing procoagulant molecules such as the tissue factor [2] as well as an indirect activation by immune cells. [5,6] In our study, we did not find any association between the plasma level of PMPs and tumor burden using RECIST criteria or radiographic contouring, for all sizes of PMPs in patients with stage IV melanoma. We do not have any clear explanation but we may hypothesise that PMPs reflect the tumor microenvironment, including angiogenesis, inflammatory reaction and antitumoral immunity rather than tumor burden.…”

Section: Letter To the Editorcontrasting

confidence: 55%

Increased levels of circulating platelet‐derived microparticles are associated with metastatic cutaneous melanoma

Moreau

Pelletier

Biichlé

et al. 2017

Experimental Dermatology

View full text Add to dashboard Cite

We investigated the plasma levels of PMPs in patients with 45 stage III and 45 stage IV melanoma. PMPs were characterised by flow cytometry and their thrombogenic activity. We also investigated the link between PMPs circulating levels and tumor burden. The circulating levels of PMPs were significantly higher in stage IV (8500 μL | BACKGROUNDMicroparticles (MPs) are membrane vesicles generated from different cellular compartments and released by any cell type into the vascular compartment during activation or apoptosis processes. In cancer, MPs are involved in metastatic progression through angiogenesis, immune escape and thrombogenicity. [1,2] We previously demonstrated [3] that the plasma levels of PMPs were significantly higher, and the clotting time-PPL was significantly lower in patients with melanoma than in healthy controls. However, MPs levels did not significantly differ between the different stages of melanoma. | QUESTIONS ADDRESSEDPrevious data prompted us to compare the level of circulating PMPs in patients with stage III and IV melanoma as stage III patients are considered as high-risk of disease recurrence. | EXPERIMENTAL DESIGNIn a monocentric prospective study, we investigated the plasma levels of PMPs by flow cytometry and evaluated their thrombogenic activity by measuring the clotting time (3, s4, s5 | RESULTSThere was a significant difference between the plasma levels of PMPs in patients with stage III and in stage IV melanoma (Table S1, Figures | CONCLUSIONSAlthough PMPs level has been correlated with metastatic tumors, [2,4] the function of high PMPs levels in advanced melanoma still need to be explored. Our study demonstrates that circulating PMPs are | LETTER TO THE EDITORsignificantly increased in patients with stage IV compared to stage III melanoma with no correlation to tumor burden. In addition, we calculated a threshold value of PMPs plasma level that differentiates stages III and IV with a high specificity and PPV. The exact mechanisms inducing platelet activation and then formation of PMPs in cancer are not well understood, but it seems that there is a direct activation by the tumoral cells releasing procoagulant molecules such as the tissue factor [2] as well as an indirect activation by immune cells. [5,6] In our study, we did not find any association between the plasma level of PMPs and tumor burden using RECIST criteria or radiographic contouring, for all sizes of PMPs in patients with stage IV melanoma. We do not have any clear explanation but we may hypothesise that PMPs reflect the tumor microenvironment, including angiogenesis, inflammatory reaction and antitumoral immunity rather than tumor burden. [5] It may also be suggested that PMPs may not be representative of tumor burden as recently suggested by Willms et al. [4] Cancer-associated venous thromboembolism constitutes the second cause of death after cancer. [7] We previously observed an inverse correlation between PMPs and clotting times with a lower clotting time in stage IV patients as compared to stage II...

show abstract

Section: Letter To the Editorcontrasting

confidence: 55%

Increased levels of circulating platelet‐derived microparticles are associated with metastatic cutaneous melanoma

Moreau

Pelletier

Biichlé

et al. 2017

Experimental Dermatology

View full text Add to dashboard Cite

show abstract

“…Most importantly receptors involved in direct interactions include platelet P-selectin (CD62P) and CD40 ligand (CD40L), as well as PSGL-1, CD40 and Mac-1 (integrin α M β 2 , CD11b/CD18) on leukocytes (2–4). Platelet-leukocyte interactions are further stabilised by crosstalk of numerous additional receptor/ligand pairs that were reviewed previously (1,5) and trigger mutual activation and release of granular content by both platelets and leukocytes, thereby modulating leukocyte function and fine-tuning immune responses (5). Importantly, platelet-leukocyte interactions facilitate leukocyte recruitment and extravasation to sites of inflammation (6,7), promote leukocyte release of pro-inflammatory mediators (8,9), oxidative burst, phagocytosis, release of neutrophil extracellular traps (NETs) (10,11), and may also dampen inflammation under some pathological conditions (12–14).…”

Section: Introductionmentioning

confidence: 99%

Measuring and interpreting platelet-leukocyte aggregates

et al. 2018

Self Cite

View full text Add to dashboard Cite

Platelets, besides their specialised role in haemostasis and atherothrombosis, actively modulate innate and adaptive immune responses with crucial roles in immune surveillance, inflammation and host defence during infection. An important prerequisite for platelet-mediated changes of immune functions involves direct engagement with different types of leukocytes. Indeed, increased platelet-leukocyte aggregates (PLAs) within the circulation and/or locally at the site of inflammation represent markers of many thrombo-inflammatory diseases, such as cardiovascular diseases, acute lung injury, renal and cerebral inflammation. Therefore, measurement of PLAs could provide an attractive and easily accessible prognostic and/or diagnostic tool for many diseases. To measure PLAs in different (patho-)physiological settings in human and animal models flow cytometric and microscopic approaches have been applied. These techniques represent complementary tools to study different aspects relating to the involvement of leukocyte subtypes and molecules, as well as location of PLAs within tissues, dynamics of their interactions and/or dynamic changes in leukocyte and platelet behaviour. This review summarises various approaches to measure and interpret PLAs and discusses potential experimental factors influencing platelet binding to leukocytes. Furthermore, we summarise insights gained from studies regarding the underlying mechanism of platelet-leukocyte interactions and discuss implications of these interactions in health and disease.

show abstract

“…These adhesion molecules also support in loco eukocyte recruitment and retention, as part of the immunological response to the damage [48]. Thanks to the soluble mediators secreted following activation, platelets may induce transendothelial leukocytes migration.…”

Section: Beyond Aggregation: New Insight In Platelet Physiology and Fmentioning

confidence: 99%

“…However, vessel injury represents a risk for infection, thus recruited platelets may activate leukocytes via direct cell-cell contacts and indirectly via cytokines and/or platelet-derived microvesicles. Interaction between activated platelets and leucocytes occurs by the binding of P-selectin with P-selectin glycoprotein ligand1 (PSGL-1) and is enhanced by interaction with other cofactors and local cytokine release, thus modulating immune responses and local inflammation [41,48]. Platelets store a variety of mediators in the α-granule such as cytokines, chemokines and growth factors.…”

Section: Beyond Aggregation: New Insight In Platelet Physiology and Fmentioning

confidence: 99%

The Two Faces of Thrombosis: Coagulation Cascade and Platelet Aggregation. Are Platelets the Main Therapeutic Target?

Cimmino¹,

Fischetti²,

Golino³

2017

J Thrombo Cir

View full text Add to dashboard Cite

Acute thrombus formation is the pathophysiological substrate underlying several clinical conditions, such as acute coronary syndrome (ACS) and stroke. Activation of coagulation cascade is a key step of the thrombotic process: vessel injury results in exposure of the glycoprotein tissue factor (TF) to the flowing blood. Once exposed, TF binds factor VII/VIIa (FVII/FVIIa) and in presence of calcium ions, it forms a tertiary complex able to activate FX to FXa, FIX to FIXa, and FVIIa itself. The final step is thrombin formation at the site of vessel injury with subsequent platelet activation, fibrinogen to fibrin conversion and ultimately thrombus formation.Platelets are the key cells in primary hemostasis. For years they have been considered only as cell fragments participating to primary hemostasis and onto which coagulation factors are assembled in the process of thrombus formation. However, recent advances in platelets pathophysiology have shown that these cells are able to regulate their gene and protein expression, make de novo protein synthesis, and release different mediators with paracrine effects that may interfere with different cell functions.Pharmacological modulation of both side of thrombosis, coagulation cascade and platelet activation, is of great clinical importance. Several clinical trials have clearly shown the efficacy of anticoagulation and/or anti platelet aggregation in different thrombotic disorders. This article aims at reviewing the recent advancements on the two faces of thrombosis focusing on the emerging role of platelets not only as clot-forming components, but highlighting their involvement in the inflammatory-immune system, as well as in modulation of different cell functions.

show abstract

Platelet Interaction with Innate Immune Cells

Cited by 203 publications

References 117 publications

Increased levels of circulating platelet‐derived microparticles are associated with metastatic cutaneous melanoma

Increased levels of circulating platelet‐derived microparticles are associated with metastatic cutaneous melanoma

Measuring and interpreting platelet-leukocyte aggregates

The Two Faces of Thrombosis: Coagulation Cascade and Platelet Aggregation. Are Platelets the Main Therapeutic Target?

Contact Info

Product

Resources

About