4.7 Article

Membrane Ballooning in Aggregated Platelets is Synchronised and Mediates a Surge in Microvesiculation

Journal

SCIENTIFIC REPORTS
Volume 7, Issue -, Pages -

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41598-017-02933-4

Keywords

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Funding

  1. MRC
  2. Wolfson Foundation
  3. British Heart Foundation [RG/10/006/28299, RG/15/16/31758, PG/14/3/30565, PG/13/11/30016]
  4. United Kingdom National Institute for Health Research [II-LB-0313-20003]
  5. British Heart Foundation [PG/16/3/31833, PG/13/11/30016, RG/10/006/28299, RG/15/16/31758, PG/12/79/29884, PG/16/21/32083] Funding Source: researchfish
  6. National Institutes of Health Research (NIHR) [II-LB-0313-20003] Funding Source: National Institutes of Health Research (NIHR)

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Human platelet transformation into balloons is part of the haemostatic response and thrombus architecture. Here we reveal that in aggregates of platelets in plasma, ballooning in multiple platelets occurs in a synchronised manner. This suggests a mechanism of coordination between cells, previously unrecognised. We aimed to understand this mechanism, and how it may contribute to thrombus development. Using spinning-disc confocal microscopy we visualised membrane ballooning in human platelet aggregates adherent to collagen-coated surfaces. Within an aggregate, multiple platelets undergo ballooning in a synchronised fashion, dependent upon extracellular calcium, in a manner that followed peak cytosolic calcium levels in the aggregate. Synchrony was observed in platelets within but not between aggregates, suggesting a level of intra-thrombus communication. Blocking phosphatidylserine, inhibiting thrombin or blocking PAR1 receptor, largely prevented synchrony without blocking ballooning itself. In contrast, inhibition of connexins, P2Y(12), P2Y(1) or thromboxane formation had no effect on synchrony or ballooning. Importantly, synchronised ballooning was closely followed by a surge in microvesicle formation, which was absent when synchrony was blocked. Our data demonstrate that the mechanism underlying synchronised membrane ballooning requires thrombin generation acting effectively in a positive feedback loop, mediating a subsequent surge in procoagulant activity and microvesicle release.

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