Your search keyword '"Gandrille, Sophie"' showing total 5 results

1. Antithrombotic potential of a single-domain antibody enhancing the activated protein C-cofactor activity of protein S.

Author

Sedzro JC, Adam F, Auditeau C, Bianchini E, De Carvalho A, Peyron I, Daramé S, Gandrille S, Thomassen S, Hackeng TM, Christophe OD, Lenting PJ, Denis CV, Borgel D, and Saller F

Subjects

Animals, Factor VIIIa chemistry, Fibrinolytic Agents pharmacology, Humans, Mice, Protein C metabolism, Protein S metabolism, Single-Domain Antibodies

Abstract

Background: Protein S (PS) is a natural anticoagulant acting as a cofactor for activated protein C (APC) in the proteolytic inactivation of activated factors V (FVa) and VIII (FVIIIa), but also for tissue factor pathway inhibitor α (TFPIα) in the inhibition of activated factor X (FXa)., Objective: For therapeutic purposes, we aimed at generating single-domain antibodies (sdAbs) that could specifically modulate the APC-cofactor activity of PS in vivo., Methods: A llama-derived immune library of sdAbs was generated and screened on recombinant human PS by phage display. PS binders were tested in a global activated partial thromboplastin time (APTT)-based APC-cofactor activity assay., Results: A PS-specific sdAb (PS003) was found to enhance the APC-cofactor activity of PS in our APTT-based assay, and this enhancing effect was greater for a bivalent form of PS003 (PS003biv). Further characterization of PS003biv demonstrated that PS003biv also enhanced the APC-cofactor activity of PS in a tissue factor (TF)-induced thrombin generation assay and stimulated APC in the inactivation of FVa, but not FVIIIa, in plasma-based assays. Furthermore, PS003biv was directed against the sex hormone-binding globulin (SHBG)-like domain but did not inhibit the binding of PS to C4b-binding protein (C4BP) and did not interfere with the TFPIα-cofactor activity of PS. In mice, PS003biv exerted an antithrombotic effect in a FeCl 3 -induced thrombosis model, while not affecting physiological hemostasis in a tail-clip bleeding model., Discussion: Altogether, these results showed that pharmacological enhancement of the APC-cofactor activity of PS through an original anti-PS sdAb might constitute a promising and safe antithrombotic strategy., (© 2022 International Society on Thrombosis and Haemostasis.)

Published

2022

2. Induced forms of α 2 -macroglobulin neutralize heparin and direct oral anticoagulant effects.

Author

Jourdi G, Abdoul J, Siguret V, Decleves X, Frezza E, Pailleret C, Gouin-Thibault I, Gandrille S, Neveux N, Samama CM, Pasquali S, and Gaussem P

Subjects

Administration, Oral, Animals, Disease Models, Animal, Female, Healthy Volunteers, Hemorrhage chemically induced, Humans, Methylamines pharmacology, Mice, Molecular Docking Simulation, Pregnancy, Pregnancy-Associated alpha 2-Macroglobulins chemistry, Pregnancy-Associated alpha 2-Macroglobulins pharmacology, Protein Domains, Factor Xa chemistry, Factor Xa Inhibitors adverse effects, Hemorrhage drug therapy, Heparin adverse effects, Pregnancy-Associated alpha 2-Macroglobulins administration & dosage

Abstract

Alpha 2 -macroglobulin (α 2 M) is a physiological macromolecule that facilitates the clearance of many proteinases, cytokines and growth factors in human. Here, we explored the effect of induced forms of α 2 M on anticoagulant drugs. Gla-domainless factor Xa (GDFXa) and methylamine (MA)-induced α 2 M were prepared and characterized by electrophoresis, immunonephelometry, chromogenic, clot waveform and rotational thromboelastometry assays. Samples from healthy volunteers and anticoagulated patients were included. In vivo neutralization of anticoagulants was evaluated in C57Bl/6JRj mouse bleeding-model. Anticoagulant binding sites on induced α 2 M were depicted by computer-aided energy minimization modeling. GDFXa-induced α 2 M neutralized dabigatran and heparins in plasma and whole blood. In mice, a single IV dose of GDFXa-induced α 2 M following anticoagulant administration significantly reduced blood loss and bleeding time. Being far easier to prepare, we investigated the efficacy of MA-induced α 2 M. It neutralized rivaroxaban, apixaban, dabigatran and heparins in spiked samples in a concentration-dependent manner and in samples from treated patients. Molecular docking analysis evidenced the ability of MA-induced α 2 M to bind non-covalently these compounds via some deeply buried binding sites. Induced forms of α 2 M have the potential to neutralize direct oral anticoagulants and heparins, and might be developed as a universal antidote in case of major bleeding or urgent surgery., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

3. Alternative mRNA is favored by the A3 haplotype of the EPCR gene PROCR and generates a novel soluble form of EPCR in plasma.

Author

Saposnik B, Lesteven E, Lokajczyk A, Esmon CT, Aiach M, and Gandrille S

Subjects

ADAM Proteins genetics, ADAM Proteins metabolism, ADAM17 Protein, Amino Acid Substitution, Antigens, CD blood, Antigens, CD genetics, Cells, Cultured, Endothelial Cells cytology, Endothelial Protein C Receptor, Gene Expression, Haplotypes, Humans, Mutation, Missense, Plasma metabolism, Protease Inhibitors pharmacology, Protein Isoforms biosynthesis, Protein Isoforms blood, Protein Isoforms genetics, Protein Structure, Tertiary physiology, RNA, Messenger genetics, Receptors, Cell Surface blood, Receptors, Cell Surface genetics, Recombinant Proteins blood, Recombinant Proteins genetics, Recombinant Proteins metabolism, Umbilical Veins cytology, Alternative Splicing physiology, Antigens, CD biosynthesis, Endothelial Cells metabolism, RNA, Messenger metabolism, Receptors, Cell Surface biosynthesis, Umbilical Veins metabolism

Abstract

The endothelial cell protein C receptor also exists in soluble form in plasma (sEPCR), resulting from ADAM17 cleavage. Elevated sEPCR levels are observed in subjects carrying the A3 haplotype, which is characterized by a Ser219Gly substitution in the transmembrane domain, rendering the receptor more sensitive to cleavage. Because sEPCR production is not completely blocked by metalloprotease inhibition, we looked for another mechanism. Comparing mRNA expression patterns and levels in A3 and non-A3 cells from 32 human umbilical cord veins, we detected a truncated mRNA in addition to the full-length mRNA. This truncated mRNA was 16 times more abundant in A3 human umbilical vein endothelial cells than in non-A3 human umbilical vein endothelial cells and encoded a protein lacking the transmembrane domain. We stably expressed a recombinant form of this protein (rEPCRisoform) and a protein mimicking the plasma sEPCR (rEPCRsol). Functional studies of the purified recombinant proteins revealed that the rEPCRisoform bound to recombinant protein C with similar affinity than rEPCRsol and that it also inhibited the anticoagulant activity of APC. Trace amounts of the EPCR isoform were found in the plasma of A3 subjects. These results suggest that the sEPCRisoform could contribute to the regulatory effect of sEPCR in plasma.

Published

2008

4. The gamma-carboxyglutamic acid domain of anticoagulant protein S is involved in activated protein C cofactor activity, independently of phospholipid binding.

Author

Saller F, Villoutreix BO, Amelot A, Kaabache T, Le Bonniec BF, Aiach M, Gandrille S, and Borgel D

Subjects

Binding Sites, Cell Line, Humans, Models, Molecular, Mutation genetics, Protein Binding, Protein S genetics, Protein Structure, Tertiary, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Structure-Activity Relationship, 1-Carboxyglutamic Acid metabolism, Phospholipids metabolism, Protein C metabolism, Protein S chemistry, Protein S metabolism

Abstract

We expressed 2 chimeras between human protein S (PS) and human prothrombin (FII) in which the prothrombin gamma-carboxyglutamic acid (Gla) domain replaced the PS Gla domain in native PS (Gla(FII)-PS) or in PS deleted of the thrombin-sensitive region (TSR) (Gla(FII)-DeltaTSR-PS). Neither PS/FII chimera had activated protein C (APC) cofactor activity in plasma clotting assays or purified systems, but both bound efficiently to phospholipids. This pointed to a direct involvement of the PS Gla domain in APC cofactor activity through molecular interaction with APC. Using computational methods, we identified 2 opposite faces of solvent-exposed residues on the PS Gla domain (designated faces 1 and 2) as potentially involved in this interaction. Their importance was supported by functional characterization of a PS mutant in which the face 1 and face 2 PS residues were reintroduced into Gla(FII)-PS, leading to significant APC cofactor activity, likely through restored interaction with APC. Furthermore, by characterizing PS mutants in which PS face 1 and PS face 2 were individually replaced by the corresponding prothrombin faces, we found that face 1 was necessary for efficient phospholipid binding but that face 2 residues were not strictly required for phospholipid binding and were involved in the interaction with APC.

Published

2005

5. A haplotype of the EPCR gene is associated with increased plasma levels of sEPCR and is a candidate risk factor for thrombosis.

Author

Saposnik B, Reny JL, Gaussem P, Emmerich J, Aiach M, and Gandrille S

Subjects

Adolescent, Adult, Antigens, CD, Case-Control Studies, Endothelial Protein C Receptor, Female, Gene Frequency, Genetic Predisposition to Disease epidemiology, Glycoproteins, Haplotypes, Humans, Male, Middle Aged, Phenotype, Polymorphism, Genetic, Receptors, Cell Surface, Risk Factors, Solubility, Endothelins blood, Endothelins genetics, Venous Thrombosis epidemiology, Venous Thrombosis genetics

Abstract

The endothelial cell protein C (PC) receptor (EPCR) facilitates PC activation by the thrombin-thrombomodulin complex. A soluble form of this receptor (sEPCR) found in plasma inhibits both activated PC (aPC) activity and PC activation by competing for PC with membrane-associated EPCR. Elevated sEPCR levels are found in approximately 20% of healthy subjects, but the mechanisms underlying this interindividual variability are unknown. We measured sEPCR levels in 100 healthy male volunteers, and observed 2 phenotypic groups of subjects. The temporal stability of sEPCR levels suggested genetic control. Extensive analysis of the EPCR gene in these subjects revealed 13 polymorphisms in complete linkage disequilibrium; these defined 3 haplotypes, 1 of which (A3) was strongly associated with high sEPCR levels. The high constitutive sEPCR levels observed in A3 haplotype carriers might reduce the efficiency of the PC system and predispose these subjects to venous thrombosis. By studying 338 patients with venous thrombosis and 338 age- and sex-matched healthy subjects, we found that the A3 haplotype was overrepresented in the patients. In multivariate analysis, subjects carrying the A3 haplotype had an increased risk of thrombosis (odds ratio [OR] = 1.8; P =.004). Thus, the A3 haplotype, which is associated with elevated plasma sEPCR levels, is a candidate risk factor for venous thrombosis.

Published

2004