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Localization of Short-Chain Polyphosphate Enhances its Ability to Clot Flowing Blood Plasma. | LitMetric

AI Article Synopsis

  • Short-chain polyphosphate (polyP) is released from activated platelets, but its role in thrombosis is unclear.
  • Numerical simulations and in vitro tests showed that localized synthetic polyP significantly speeds up clotting in flowing blood, especially at low shear rates typical of thrombotic conditions.
  • While localized polyP can accelerate clotting at very low concentrations, the biological reasons for its localization on platelet or vascular surfaces are still unknown.

Article Abstract

Short-chain polyphosphate (polyP) is released from platelets upon platelet activation, but it is not clear if it contributes to thrombosis. PolyP has increased propensity to clot blood with increased polymer length and when localized onto particles, but it is unknown whether spatial localization of short-chain polyP can accelerate clotting of flowing blood. Here, numerical simulations predicted the effect of localization of polyP on clotting under flow, and this was tested in vitro using microfluidics. Synthetic polyP was more effective at triggering clotting of flowing blood plasma when localized on a surface than when solubilized in solution or when localized as nanoparticles, accelerating clotting at 10-200 fold lower concentrations, particularly at low to sub-physiological shear rates typical of where thrombosis occurs in large veins or valves. Thus, sub-micromolar concentrations of short-chain polyP can accelerate clotting of flowing blood plasma under flow at low to sub-physiological shear rates. However, a physiological mechanism for the localization of polyP to platelet or vascular surfaces remains unknown.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5301195PMC
http://dx.doi.org/10.1038/srep42119DOI Listing

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