TFPIβ is the GPI-anchored TFPI isoform on human endothelial cells and placental microsomes

Girard, Thomas; Tuley, Elodee A.; Broze, George J.

doi:10.1182/blood-2011-10-388512

Cited by 53 publications

(57 citation statements)

References 29 publications

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“…This isoform is expressed in endothelial cells, albeit at lower levels than TFPI␣, and was identified as the major endothelial cell surface-associated form of TFPI (104). Given that it is easily cleaved from the phospholipid anchor, TFPI␤ may well be the predominant TFPI pool available in the body (104). A third TFPI isoform containing only Kunitz domains 1 and 2, TFPI␦, has only been identified at the mRNA level.…”

Section: Coagulation Protease Inhibitorsmentioning

confidence: 99%

“…In the second isoform, TFPI␤, the third Kunitz domain and COOH terminus are replaced by a neo COOH terminus containing a glycophosphatidylinositol anchor. This isoform is expressed in endothelial cells, albeit at lower levels than TFPI␣, and was identified as the major endothelial cell surface-associated form of TFPI (104). Given that it is easily cleaved from the phospholipid anchor, TFPI␤ may well be the predominant TFPI pool available in the body (104).…”

Section: Coagulation Protease Inhibitorsmentioning

confidence: 99%

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New Fundamentals in Hemostasis

Versteeg

Heemskerk

Levi

et al. 2013

Physiological Reviews

852

831

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Hemostasis encompasses the tightly regulated processes of blood clotting, platelet activation, and vascular repair. After wounding, the hemostatic system engages a plethora of vascular and extravascular receptors that act in concert with blood components to seal off the damage inflicted to the vasculature and the surrounding tissue. The first important component that contributes to hemostasis is the coagulation system, while the second important component starts with platelet activation, which not only contributes to the hemostatic plug, but also accelerates the coagulation system. Eventually, coagulation and platelet activation are switched off by blood-borne inhibitors and proteolytic feedback loops. This review summarizes new concepts of activation of proteases that regulate coagulation and anticoagulation, to give rise to transient thrombin generation and fibrin clot formation. It further speculates on the (patho)physiological roles of intra-and extravascular receptors that operate in response to these proteases. Furthermore, this review provides a new framework for understanding how signaling and adhesive interactions between endothelial cells, leukocytes, and platelets can regulate thrombus formation and modulate the coagulation process. Now that the key molecular players of coagulation and platelet activation have become clear, and their complex interactions with the vessel wall have been mapped out, we can also better speculate on the causes of thrombosis-related angiopathies.

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Section: Coagulation Protease Inhibitorsmentioning

confidence: 99%

Section: Coagulation Protease Inhibitorsmentioning

confidence: 99%

New Fundamentals in Hemostasis

Versteeg

Heemskerk

Levi

et al. 2013

Physiological Reviews

852

831

View full text Add to dashboard Cite

show abstract

“…Presumably the binding of TFPIα to FV-short in affected family members' plasma results in its retention in circulation, thus causing the higher TFPIα plasma concentrations. Even though the concentration of TFPIα in plasma is normally very low, significant amounts are present in the vasculature associated with the endothelium (25,26). Infusion of heparin releases part of the TFPIα from the endothelium to the circulation.…”

Section: Figurementioning

confidence: 99%

“…It circulates bound to the lipoproteins, mainly to LDL (25). Another truncated isoform denoted TFPIβ is present on endothelium, where it is bound with a GPI anchor (26). Recently, Ndonwi et al demonstrated that the positively charged C terminus of TFPIα contains the binding site for FV (27).…”

Section: Introductionmentioning

confidence: 99%

Coagulation factor VA2440G causes east Texas bleeding disorder via TFPIα

et al. 2013

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The autosomal dominantly inherited east Texas bleeding disorder is linked to an A2440G variant in exon 13 of the F5 gene. Affected individuals have normal levels of coagulation factor V (FV) activity, but demonstrate inhibition of global coagulation tests. We demonstrated that the A2440G mutation causes upregulation of an alternatively spliced F5 transcript that results in an in-frame deletion of 702 amino acids of the large activation fragment, the B domain. The approximately 250-kDa FV isoform (FV-short), which can be fully activated by thrombin, is present in all A2440G carriers' plasma (n = 16). FV-short inhibits coagulation through an indirect mechanism by forming a complex with tissue factor pathway inhibitor-α (TFPIα), resulting in an approximately 10-fold increase in plasma TFPIα, suggesting that the TFPIα:FV-short complexes are retained in circulation. The TFPIα:FV-short complexes efficiently inhibit thrombin generation of both intrinsic and extrinsic coagulation pathways. These data demonstrate that the east Texas bleeding disorder-associated F5 A2440G leads to the formation of the TFPIα:FV-short complex, which inhibits activation and propagation of coagulation. IntroductionCoagulation factor V (FV) is a cofactor protein that can both promote and inhibit coagulation (1, 2). Located on 1q24-25, the F5 gene is composed of 25 exons that transcribe a 6.8-kb mRNA (3-7). The translated 330-kDa glycoprotein precursor contains 2,196 amino acids organized into the domain structure A1-A2-B-A3-C1-C2 and is highly homologous to factor VIII (FVIII), sharing 35%-40% identity in the A and C domains (4, 5, 8). Human FV is primarily produced by hepatocytes and circulates in plasma as an intact 330-kDa precursor at a concentration of about 20 nM (7 μg/ml) (9-12). Approximately 20% of the total human FV found in whole blood is stored in platelet α granules in a partially proteolyzed form in conjunction with the binding protein multimerin. This platelet FV derives from the plasma FV pool and is secreted upon platelet activation to create a high, localized concentration of the cofactor at sites of injury (12)(13)(14)(15).The procoagulant cofactor function of FV is primarily dictated by its interaction and cleavage by thrombin and active factor X (FXa). Its cleavage by thrombin is deemed the most biologically important early event in the blood clot formation process (16)(17)(18)(19). As an intact single-chain precursor, FV expresses less than 1% of its potential procoagulant cofactor activity (20). Upon sequential cleavage of Arg-709, Arg-1018, and Arg-1545 by thrombin, the large connecting B domain is removed from the intact FV molecule to produce the heavy chain (A1-A2) and the light chain (A3-C1-C2) that have M r s of 105,000 and 74,000, respectively. The heavy chain and the light chain noncovalently associate in the presence of calcium to produce an active procoagulant cofactor (FVa). FVa and FXa assemble on negatively charged phospholipid (PL) membranes to form the prothrombinase (PTase) complex. The presence of FVa in...

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“…72 It is still disputed which TFPI isoform is the most abundantly expressed isoform, however TFPI-β, a GPI-AP expressed on ECs, is thought to exert 80% of anticoagulant activity. 72,73 Possible deficiency of the GPI anchor of TFPI-β in PNH may therefore reduce the anticoagulant properties of the endothelium in PNH and contribute to thrombus formation. 74,75 Anti-thrombin is enhanced by binding to the heparan sulphate receptor, a GPI-linked protein expressed on endothelial cells and hypothesized to be lost in patients with PNH.…”

Section: Free Hemoglobin and Endothelial Dysfunctionmentioning

confidence: 99%