Plasminogen on the surfaces of fibrin clots prevents adhesion of leukocytes and platelets

Lishko, Valeryi K.; Yermolenko, Ivan S.; Ugarova, Tatiana P.

doi:10.1111/j.1538-7836.2010.03778.x

Cited by 16 publications

(17 citation statements)

References 43 publications

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“…Plasminogen thus bound adopts an open conformation that is readily transformed into plasmin. Recently published studies [4][5][6] are in agreement with these hitherto unknown fibrinolytic pathways and potentially novel biomarkers in clinical practice.…”

Section: 2supporting

confidence: 62%

Membrane microvesicles: a circulating source for fibrinolysis, new antithrombotic messengers

Laurent

Anglès-Cano

2013

Haematologica

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Section: 2supporting

confidence: 62%

Membrane microvesicles: a circulating source for fibrinolysis, new antithrombotic messengers

Laurent

Anglès-Cano

2013

Haematologica

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“…Although self-association of fibrinogen is readily induced, suggesting its potential significance, no physiologic role has been ascribed to this process. We have recently proposed that the fibrinogen matrix deposited on the surface of fibrin clots may play an important role in normal hemostasis by preventing excessive adhesion of circulating blood cells, thus limiting thrombus propagation (6,43). The finding of the present study that the fibrinogen molecules without the ␣C regions are incapable of developing the multilayer with ensuing sustained cell adhesion may have significant implications with respect to the role of these derivatives in several pathological conditions.…”

Section: Discussionmentioning

confidence: 61%

The Assembly of Nonadhesive Fibrinogen Matrices Depends on the αC Regions of the Fibrinogen Molecule

Yermolenko

Gorkun

Fuhrmann

et al. 2012

Journal of Biological Chemistry

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Background: Surface-induced aggregation of fibrinogen results in the assembly of an extensible multilayered matrix, which prevents integrin-mediated cell adhesion. Results: Without the ␣C regions, the fibrinogen molecules assemble a defective, poorly extensible matrix supporting sustained cell adhesion. Conclusion:The assembly of nonadhesive fibrinogen multilayer requires the ␣C regions of the molecule. Significance: The molecular mechanism for the assembly of the fibrinogen multilayer is identified.

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“…The THP-1 cells were cultured in RPMI containing 10% FBS, antibiotics, and 0.05 mM 2-mercaptoethanol. The THP-1 were differentiated by adding 10 ng/ml of PMA into the medium for 48 h. Human neutrophils were isolated under sterile conditions from peripheral blood obtained from healthy volunteers as described (51). Human monocytes were isolated from peripheral blood obtained from healthy volunteers using the EasySep Human monocyte isolation kit (StemCell Technologies, Cambridge, MA) according to the manufacturer's protocol.…”

Section: Cellsmentioning

confidence: 99%

Leukocyte integrin Mac-1 (CD11b/CD18, αMβ2, CR3) acts as a functional receptor for platelet factor 4

Lishko

Yakubenko

Ugarova

et al. 2018

Journal of Biological Chemistry

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Platelet factor 4 (PF4) is one of the most abundant cationic proteins secreted from α-granules of activated platelets. Based on its structure, PF4 was assigned to the CXC family of chemokines and has been shown to have numerous effects on myeloid leukocytes. However, the receptor for PF4 remains unknown. Here, we demonstrate that PF4 induces leukocyte responses through the integrin Mac-1 (αβ, CD11b/CD18). Human neutrophils, monocytes, U937 monocytic and HEK293 cells expressing Mac-1 strongly adhered to immobilized PF4 in a concentration-dependent manner. The cell adhesion was partially blocked by anti-Mac-1 mAb and inhibition was enhanced when anti-Mac-1 antibodies were combined with glycosaminoglycans, suggesting that cell-surface proteoglycans act cooperatively with Mac-1. PF4 also induced Mac-1-dependent migration of human neutrophils and murine WT, but not Mac-1-deficient macrophages. Coating of bacteria or latex beads with PF4 enhanced their phagocytosis by macrophages by ∼4-fold, and this process was blocked by different Mac-1 antagonists. Furthermore, PF4 potentiated phagocytosis by WT, but not Mac-1-deficient macrophages. As determined by biolayer interferometry, PF4 directly bound the αI-domain, the major ligand-binding region of Mac-1, and this interaction was governed by a of 1.3 ± 0.2 μm Using the PF4-derived peptide library, synthetic peptides duplicating the αI-domain recognition sequences and recombinant mutant PF4 fragments, the binding sites for αI-domain were identified in the PF4 segments Cys-Ser and Ala-Ser These results identify PF4 as a ligand for the integrin Mac-1 and suggest that many immune-modulating effects previously ascribed to PF4 are mediated through its interaction with Mac-1.

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Plasminogen on the surfaces of fibrin clots prevents adhesion of leukocytes and platelets

Cited by 16 publications

References 43 publications

Membrane microvesicles: a circulating source for fibrinolysis, new antithrombotic messengers

Membrane microvesicles: a circulating source for fibrinolysis, new antithrombotic messengers

The Assembly of Nonadhesive Fibrinogen Matrices Depends on the αC Regions of the Fibrinogen Molecule

Leukocyte integrin Mac-1 (CD11b/CD18, αMβ2, CR3) acts as a functional receptor for platelet factor 4

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