Platelets at the vascular interface

Bergmeier, Wolfgang; Stefanini, Lucia

doi:10.1002/rth2.12061

Cited by 19 publications

(18 citation statements)

References 68 publications

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“…Platelets are specialized cells generated from the cytoplasmic fragmentation of megakaryocytes to ensure the integrity of the vascular system upon mechanical injury or any other vascular breach, occurring, for instance, at sites of inflammation. [1][2][3] Platelet stimulation triggers intracellular signaling cascades that promote cytoskeletal remodeling, secretion of granules, release of eicosanoids, and conversion of integrin receptors from a lowto a high-affinity state for their ligands (inside-out activation). Once active, integrins mediate platelet adhesion to the exposed extracellular matrix and aggregation to adjacent active platelets.…”

Section: Introductionmentioning

confidence: 99%

Functional redundancy between RAP1 isoforms in murine platelet production and function

Stefanini

Lee²,

Paul³

et al. 2018

Blood

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Section: Introductionmentioning

confidence: 99%

Functional redundancy between RAP1 isoforms in murine platelet production and function

Stefanini

Lee²,

Paul³

et al. 2018

Blood

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“…Adhesion is a rapid process that takes place within seconds of vascular injury and entails the deceleration of rapidly moving platelets to allow adherence to the vascular wall [52]. Owing to platelet margination by larger molecules, these cells are already in close proximity to the vascular endothelium and complexes can easily form between the platelet-specific receptors, such as glycoprotein (GP) Ib-V-IX, and the cell adhesion ligand von Willebrand factor (VWF), which acts as a bridge between the platelet surface and endothelial collagen [53].…”

Section: Platelet Function In Hemostasis and The Mechanisms Involvmentioning

confidence: 99%

“…Another important observation is that a positive charge on the surface of NPs can, in addition to warranting effective cellular drug delivery, also ensue immunotoxicity through the stimulation of inflammatory immune responses. Several researchers have found that cationic liposomes can stimulate neutrophils and induce oxidative bursts in these cells [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50,51,52,53,54,55,56,57,58,59,60,61,62,63,64,65,66,67,68,69,70,71,72,73,74,75,76,77,...…”

Section: Leukocyte Function In Hemostasis and The Mechanisms Involmentioning

confidence: 99%

The Hemocompatibility of Nanoparticles: A Review of Cell–Nanoparticle Interactions and Hemostasis

Harpe

Kondiah

Choonara

et al. 2019

Cells

238

143

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Understanding cell–nanoparticle interactions is critical to developing effective nanosized drug delivery systems. Nanoparticles have already advanced the treatment of several challenging conditions including cancer and human immunodeficiency virus (HIV), yet still hold the potential to improve drug delivery to elusive target sites. Even though most nanoparticles will encounter blood at a certain stage of their transport through the body, the interactions between nanoparticles and blood cells is still poorly understood and the importance of evaluating nanoparticle hemocompatibility is vastly understated. In contrast to most review articles that look at the interference of nanoparticles with the intricate coagulation cascade, this review will explore nanoparticle hemocompatibility from a cellular angle. The most important functions of the three cellular components of blood, namely erythrocytes, platelets and leukocytes, in hemostasis are highlighted. The potential deleterious effects that nanoparticles can have on these cells are discussed and insight is provided into some of the complex mechanisms involved in nanoparticle–blood cell interactions. Throughout the review, emphasis is placed on the importance of undertaking thorough, all-inclusive hemocompatibility studies on newly engineered nanoparticles to facilitate their translation into clinical application.

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“…High-throughput profiling studies[1–4] identified among the most abundant signaling proteins in platelets (Table 1), the Ras-related protein (RAP) GTPases, a subset (5 members in mammals: RAP1A, RAP1B, RAP2A, RAP2B, RAP2C) of the larger RAS family that includes key regulators of cell adhesion, cytoskeleton remodelling and MAP kinase signaling[5–7]. These functions are critical for platelets that, in order to maintain the integrity of the vascular system, must be able to rapidly shift from an anti-adhesive/patrolling state to a pro-adhesive state, required to form a hemostatic plug and to prevent bleeding[8]. Indeed, studies by our group and others identified RAP GTPases as the critical molecular switches, which drive platelet activation at sites of vascular injury by switching on multiple platelet responses, including integrin inside-out activation, secretion, and eicosanoid mediator formation[9–13].…”

Section: Ras/rap Gtpases Expressed In Plateletsmentioning

confidence: 99%

RAP GTPases and platelet integrin signaling

Stefanini

Bergmeier

2018

Platelets

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Platelets are highly specialized cells that continuously patrol the vasculature to ensure its integrity (hemostasis). At sites of vascular injury, they are able to respond to trace amounts of agonists and to rapidly transition from an anti-adhesive/patrolling to an adhesive state (integrin inside-out activation) required for hemostatic plug formation. Pathological conditions that disturb the balance in the underlying signaling processes can lead to unwanted platelet activation (thrombosis) or to an increased bleeding risk. The small GTPases of the RAP subfamily, highly expressed in platelets, are critical regulators of cell adhesion, cytoskeleton remodeling, and MAP kinase signaling. Studies by our group and others demonstrate that RAP GTPases, in particular RAP1A and RAP1B, are the key molecular switches that turn on platelet activation/adhesiveness at sites of injury. In this review, we will summarize major findings on the role of RAP GTPases in platelet biology with a focus on the signaling pathways leading to the conversion of integrins to a high-affinity state.

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Platelets at the vascular interface

Cited by 19 publications

References 68 publications

Functional redundancy between RAP1 isoforms in murine platelet production and function

Functional redundancy between RAP1 isoforms in murine platelet production and function

The Hemocompatibility of Nanoparticles: A Review of Cell–Nanoparticle Interactions and Hemostasis

RAP GTPases and platelet integrin signaling

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