4.8 Article

IFITM3 regulates fibrinogen endocytosis and platelet reactivity in nonviral sepsis

JOURNAL OF CLINICAL INVESTIGATION (2022)

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Journal

JOURNAL OF CLINICAL INVESTIGATION
Volume 132, Issue 23, Pages -

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/JCI153014

Keywords

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Categories

Medicine, Research & Experimental

Funding

  1. US Department of Veterans Affairs Clinical Sciences RD (CSRD) [I01 CX001696]
  2. NIH [K01AG059892, R01HL163019, K08HL153953, 1K08HG010061, R01HL142804, R01AG048022, R56AG059877, R01HL130541]
  3. Fonds voor Wetenschappelijk Onderzoek Vlaanderen [FWO 12U7818N]
  4. American Heart Foundation [22POST902619, 21POST830138, 20POST35210319, 18POST340300200]
  5. National Center for Research Resources of the NIH [1S10RR026802-01]
  6. National Cancer Institute of the NIH [P30CA042014]
  7. Flow Cytometry Core at the University of Utah

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IFITM3 acts as a regulator of platelet endocytosis, hyperreactivity, and thrombosis during inflammatory stress.
Platelets and megakaryocytes are critical players in immune responses. Recent reports suggest infection and inflammation alter the megakaryocyte and platelet transcriptome to induce altered platelet reactivity. We determined whether nonviral sepsis induces differential platelet gene expression and reactivity. Nonviral sepsis upregulated IFN-induced transmembrane protein 3 (IFITM3), an IFN-responsive gene that restricts viral replication. As IFITM3 has been linked to clathrin-mediated endocytosis, we determined whether IFITM3 promoted endocytosis of alpha-granule proteins. IFN stimulation enhanced fibrinogen endocytosis in megakaryocytes and platelets from Ifitm(+/+) mice, but not Ifitm(-/-) mice. IFITM3 overexpression or deletion in megakaryocytes demonstrated IFITM3 was necessary and sufficient to regulate fibrinogen endocytosis. Mechanistically, IFITM3 interacted with clathrin and alpha(IIb) and altered their plasma membrane localization into lipid rafts. In vivo IFN administration increased fibrinogen endocytosis, platelet reactivity, and thrombosis in an IFITM-dependent manner. In contrast, Ifitm(-/-) mice were completely rescued from IFN-induced platelet hyperreactivity and thrombosis. During murine sepsis, platelets from Ifitm(+/+) mice demonstrated increased fibrinogen content and platelet reactivity, which was dependent on IFN-alpha and IFITMs. Platelets from patients with nonviral sepsis had increases in platelet IFITM3 expression, fibrinogen content, and hyperreactivity. These data identify IFITM3 as a regulator of platelet endocytosis, hyperreactivity, and thrombosis during inflammatory stress.

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