The growing complexity of platelet aggregation

Jackson, Shaun P.

doi:10.1182/blood-2006-12-027698

Cited by 626 publications

(557 citation statements)

References 93 publications

(115 reference statements)

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“…For comparison purposes, we also study Y polymers, which correspond to u ¼ 0.41 k B T 19,20 . The monomers interact with the colloids at discrete binding sites on the colloid surfaces that mimic the actual GPIb-a receptor on the surface of platelets that specifically binds to the A1 domain of vWF [10][11][12] . The binding process is modelled through the classical model of Bell 21 (see Fig.…”

Section: Resultsmentioning

confidence: 99%

“…There are some instances in nature, however, in which forming a composite very rapidly is necessary, and such conditions are met during blood clotting. During this process, our body forms a polymer-platelet composite called the plug within seconds of injury 10,11 . This aggregate composed of von Willebrand factor (vWF), which is a long biopolymer, and platelets forms the scaffold for the formation of a clot at the site of the lesion.…”

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confidence: 99%

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Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

et al. 2013

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Blood clotting is a process by which a haemostatic plug is assembled at the site of injury. The formation of such a plug, which is essentially a (bio)polymer-colloid composite, is believed to be driven by shear flow in its initial phase, and contrary to our intuition, its assembly is enhanced under stronger flowing conditions. Here, inspired by blood clotting, we show that polymer-colloid composite assembly in shear flow is a universal process that can be tailored to obtain different types of aggregates including loose and dense aggregates, as well as hydrodynamically induced 'log'-type aggregates. The process is highly controllable and reversible, depending mostly on the shear rate and the strength of the polymer-colloid binding potential. Our results have important implications for the assembly of polymercolloid composites, an important challenge of immense technological relevance. Furthermore, flow-driven reversible composite formation represents a new paradigm in non-equilibrium self-assembly.

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Section: Resultsmentioning

confidence: 99%

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confidence: 99%

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

et al. 2013

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“…In this assay, human melanoma A375 cells and mouse melanoma B16F10 cells both stably expressing GFP (A375-GFP cells and B16F10-GFP cells) were used. It has been reported that mouse platelets could interact with tumor cells in a P-selectin dependent manner [25][26][27][28][29] and B16F10 cells do not express P-selectin ligand. 12 In order to observe the tumor cell-platelet interactions in lung vessels, platelets were labeled with PKH26 (red), which can not activate platelets and can guarantee the molecules on the platelet surface in its native conformation.…”

Section: The Tumor Cell-platelet Interactions and Lung Metastasis Canmentioning

confidence: 99%

Modified heparins inhibit integrin α_IIbβ₃ mediated adhesion of melanoma cells to platelets in vitro and in vivo

Zhang

Liu

Gao

et al. 2009

Intl Journal of Cancer

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The adhesion of tumor cells with platelets is important in the process of tumor metastasis. A huge work has indicated that antiadhesion is an effective strategy for metastasis inhibition. In this article, we assess the role of platelet integrin a IIb b 3 in adhesion of melanoma cells to platelets and the effects of heparin and modified heparins on the adhesion in vitro and in vivo. We show that platelet integrin a IIb b 3 is involved in the interaction of human melanoma A375 cells with platelets, and the high affinity epitope resides on the a IIb subunit rather than b 3 subunit. Heparin sulfatelike proteoglycans on tumor cell surface are implicated in the adhesion of A375 cells to integrin a IIb b 3 . We also show that RO-heparin, CR-heparin, N-2,3-DS-heparin and 2,3-O-DS-heparin can significantly inhibit A375 cells binding to the CHO cells expressing integrin a IIb b 3 under static and flow conditions, and remarkably inhibit the adhesion of A375 cells to the immobilized platelet layers under flow conditions. We find that A375 cells and B16F10 cells are arrested in the pulmonary vessels and adhered to platelets, and the initial interaction of tumor cells with platelets in lung vessel and long-term establishment of metastatic foci can be inhibited by heparin as well as CR-heparin and N-2,3-DS-heparin. These data suggest that modified heparins can inhibit tumor cellplatelet interaction mediated by platelet integrin a IIb b 3 and modified heparins may be a potential substitute for heparin in inhibiting tumor metastasis. ' UICCKey words: metastasis; adhesion; platelet; Integrin a IIb b 3; ; modified heparin Hematogenous metastasis of tumor cells is a cascade of events in which tumor cells separate from a primary tumor, intravasate into the bloodstream, evade innate immune surveillance, adhere to vascular endothelial cells of distant organs, and extravasate into tissue to generate new colonies. 1,2 It is well accepted that within vasculature circulating the interactions of tumor cells with platelets enhance tumor dissemination. Platelets may limit the ability of NK cells to lyse tumor cells and shield tumor cells from high shear forces that could potentially damage the tumor cells. 3,4 Furthermore, platelets facilitate the adhesion of tumor cells to vascular endothelium and release a number of growth factors, such as platelet-derived growth factor (PDGF), angiogenic growth factor, vascular endothelial growth factor (VEGF) and angiopoietin-1, which are required for metastasis and angiogenesis.Several studies support the view that tumor cell-associated platelets facilitate tumor cell metastasis. It has been shown that the elimination of circulating platelets with anti-platelet antibody result in a significant diminution of metastasis in several transplantable murine tumor models. 5,6 In addition, inhibition of platelet activation can decrease the metastatic potential of circulating tumor cells. 7,8 It is well known that platelets specifically express a IIb b 3, which has been reported to be involved in the interactio...

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“…Biochemical and hemodynamic factors contribute to thrombus formation at a vulnerable vessel wall (2)(3)(4). Thrombogenic components exposed upon plaque rupture-e.g.…”

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confidence: 99%

Atherosclerotic geometries exacerbate pathological thrombus formation poststenosis in a von Willebrand factor-dependent manner

Westein

Meer

Kuijpers

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

241

257

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Rupture of a vulnerable atherosclerotic plaque causes thrombus formation and precipitates cardiovascular diseases. In addition to the thrombogenic content of a plaque, also the hemodynamic microenvironment plays a major role in thrombus formation. How the altered hemodynamics around a plaque promote pathological thrombus formation is not well understood. In this study, we provide evidence that plaque geometries result in fluid mechanical conditions that promote platelet aggregation and thrombus formation by increased accumulation and activity of von Willebrand factor (vWF) at poststenotic sites. Resonant-scanning multiphoton microscopy revealed that in vivo arterial stenosis of a damaged carotid artery markedly increased platelet aggregate formation in the stenotic outlet region. Complementary in vitro studies using microfluidic stenotic chambers, designed to mimic the flow conditions in a stenotic artery, showed enhanced platelet aggregation in the stenotic outlet region at 60-80% channel occlusion over a range of input wall shear rates. The poststenotic thrombus formation was critically dependent on bloodborne vWF and autocrine platelet stimulation. In stenotic chambers containing endothelial cells, flow provoked increased endothelial vWF secretion in the stenotic outlet region, contributing to exacerbated platelet aggregation. Taken together, this study identifies a role for the shear-sensitive protein vWF in transducing hemodynamic forces that are present around a stenosis to a prothrombogenic microenvironment resulting in spatially confined and exacerbated platelet aggregation in the stenosis outlet region. The developed stenotic microfluidic chamber offers a realistic platform for in vitro evaluation of shear-dependent thrombus formation in the setting of atherosclerosis.

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The growing complexity of platelet aggregation

Cited by 626 publications

References 93 publications

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Modified heparins inhibit integrin α_IIbβ₃ mediated adhesion of melanoma cells to platelets in vitro and in vivo

Atherosclerotic geometries exacerbate pathological thrombus formation poststenosis in a von Willebrand factor-dependent manner

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The growing complexity of platelet aggregation

Cited by 626 publications

References 93 publications

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Blood-clotting-inspired reversible polymer–colloid composite assembly in flow

Modified heparins inhibit integrin αIIbβ3 mediated adhesion of melanoma cells to platelets in vitro and in vivo

Atherosclerotic geometries exacerbate pathological thrombus formation poststenosis in a von Willebrand factor-dependent manner

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Modified heparins inhibit integrin α_IIbβ₃ mediated adhesion of melanoma cells to platelets in vitro and in vivo