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Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma.

Publication ,  Journal Article
Nellenbach, K; Mihalko, E; Nandi, S; Koch, DW; Shetty, J; Moretti, L; Sollinger, J; Moiseiwitsch, N; Sheridan, A; Pandit, S; Hoffman, M ...
Published in: Science translational medicine
April 2024

Uncontrolled bleeding after trauma represents a substantial clinical problem. The current standard of care to treat bleeding after trauma is transfusion of blood products including platelets; however, donated platelets have a short shelf life, are in limited supply, and carry immunogenicity and contamination risks. Consequently, there is a critical need to develop hemostatic platelet alternatives. To this end, we developed synthetic platelet-like particles (PLPs), formulated by functionalizing highly deformable microgel particles composed of ultralow cross-linked poly (N-isopropylacrylamide) with fibrin-binding ligands. The fibrin-binding ligand was designed to target to wound sites, and the cross-linking of fibrin polymers was designed to enhance clot formation. The ultralow cross-linking of the microgels allows the particles to undergo large shape changes that mimic platelet shape change after activation; when coupled to fibrin-binding ligands, this shape change facilitates clot retraction, which in turn can enhance clot stability and contribute to healing. Given these features, we hypothesized that synthetic PLPs could enhance clotting in trauma models and promote healing after clotting. We first assessed PLP activity in vitro and found that PLPs selectively bound fibrin and enhanced clot formation. In murine and porcine models of traumatic injury, PLPs reduced bleeding and facilitated healing of injured tissue in both prophylactic and immediate treatment settings. We determined through biodistribution experiments that PLPs were renally cleared, possibly enabled by ultrasoft particle properties. The performance of synthetic PLPs in the preclinical studies shown here supports future translational investigation of these hemostatic therapeutics in a trauma setting.

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Published In

Science translational medicine

DOI

EISSN

1946-6242

ISSN

1946-6234

Publication Date

April 2024

Volume

16

Issue

742

Start / End Page

eadi4490

Related Subject Headings

  • Tissue Distribution
  • Swine
  • Rodentia
  • Mice
  • Hemostatics
  • Hemorrhage
  • Fibrin
  • Blood Platelets
  • Animals
  • 4003 Biomedical engineering
 

Citation

APA
Chicago
ICMJE
MLA
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Nellenbach, K., Mihalko, E., Nandi, S., Koch, D. W., Shetty, J., Moretti, L., … Brown, A. C. (2024). Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma. Science Translational Medicine, 16(742), eadi4490. https://doi.org/10.1126/scitranslmed.adi4490
Nellenbach, Kimberly, Emily Mihalko, Seema Nandi, Drew W. Koch, Jagathpala Shetty, Leandro Moretti, Jennifer Sollinger, et al. “Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma.Science Translational Medicine 16, no. 742 (April 2024): eadi4490. https://doi.org/10.1126/scitranslmed.adi4490.
Nellenbach K, Mihalko E, Nandi S, Koch DW, Shetty J, Moretti L, et al. Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma. Science translational medicine. 2024 Apr;16(742):eadi4490.
Nellenbach, Kimberly, et al. “Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma.Science Translational Medicine, vol. 16, no. 742, Apr. 2024, p. eadi4490. Epmc, doi:10.1126/scitranslmed.adi4490.
Nellenbach K, Mihalko E, Nandi S, Koch DW, Shetty J, Moretti L, Sollinger J, Moiseiwitsch N, Sheridan A, Pandit S, Hoffman M, Schnabel LV, Lyon LA, Barker TH, Brown AC. Ultrasoft platelet-like particles stop bleeding in rodent and porcine models of trauma. Science translational medicine. 2024 Apr;16(742):eadi4490.

Published In

Science translational medicine

DOI

EISSN

1946-6242

ISSN

1946-6234

Publication Date

April 2024

Volume

16

Issue

742

Start / End Page

eadi4490

Related Subject Headings

  • Tissue Distribution
  • Swine
  • Rodentia
  • Mice
  • Hemostatics
  • Hemorrhage
  • Fibrin
  • Blood Platelets
  • Animals
  • 4003 Biomedical engineering