Samenvatting
Fibrin is the major extracellular component of blood clots and a proteinaceous hydrogel used as a versatile biomaterial. Fibrin forms branched networks built of laterally associated double-stranded protofibrils. This multiscale hierarchical structure is crucial for the extraordinary mechanical resilience of blood clots, yet the structural basis of clot mechanical properties remains largely unclear due, in part, to the unresolved molecular packing of fibrin fibers. Here the packing structure of fibrin fibers is quantitatively assessed by combining Small Angle X-ray Scattering (SAXS) measurements of fibrin reconstituted under a wide range of conditions with computational molecular modeling of fibrin protofibrils. The number, positions, and intensities of the Bragg peaks observed in the SAXS experiments were reproduced computationally based on the all-atom molecular structure of reconstructed fibrin protofibrils. Specifically, the model correctly predicts the intensities of the reflections of the 22.5 nm axial repeat, corresponding to the half-staggered longitudinal arrangement of fibrin molecules. In addition, the SAXS measurements showed that protofibrils within fibrin fibers have a partially ordered lateral arrangement with a characteristic transverse repeat distance of 13 nm, irrespective of the fiber thickness. These findings provide fundamental insights into the molecular structure of fibrin clots that underlies their biological and physical properties.
Originele taal-2 | Engels |
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Pagina's (van-tot) | 8272-8283 |
Aantal pagina's | 12 |
Tijdschrift | Soft Matter |
Volume | 16 |
Nummer van het tijdschrift | 35 |
DOI's | |
Status | Gepubliceerd - 21 sep. 2020 |
Financiering
We thank Baldomero Alonso Latorre (AMOLF) for help with SAXS data analysis, and Federica Burla (AMOLF) and Fabio Ferri (Universitàdell’Insubria) for help with analysis of the turbidimetry data. This work was part of the research program of the Foundation for Fundamental Research on Matter (FOM), which is financially supported by the Netherlands Organization for Scientific Research (NWO). We gratefully acknowledge access to the DUBBLE BM26B beamline at the ESRF made possible by NWO. WB’s contribution is based upon work supported by Oak Ridge National Laboratory, managed by UT-Battelle, LLC, for the U.S. Department of Energy. NK was supported by a Marie Curie IIF fellowship and a grant from the European Research Council (851960). This work was further supported by the American Heart Association grants 15GRNT23150000 and 13GRNT16960013, NIH grants HL135254 and UO1-HL116330, the University of Pennsylvania Perelman School of Medicine Bridge Funding, the NSF grants DMR 1505662 and DMR 1505316, and the Program for Competitive Growth at Kazan Federal University.
Financiers | Financiernummer |
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H2020 Marie Skłodowska-Curie Actions | |
National Science Foundation(NSF) | DMR 1505662, DMR 1505316 |
National Institutes of Health, NIH | HL135254, UO1-HL116330 |
U.S. Department of Energy | |
American Heart Association | 13GRNT16960013, 15GRNT23150000 |
Oak Ridge National Laboratory | |
Perelman School of Medicine, University of Pennsylvania | |
European Research Council | 851960 |
Foundation for Fundamental Research on Matter | |
Nederlandse Organisatie voor Wetenschappelijk Onderzoek | |
Kazan Federal University |