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6 results on '"Barbara Lunghi"'

1. Modulation of factor VIII pharmacokinetics by genetic components in factor VIII receptors

Author

Barbara Lunghi, Massimo Morfini, Nicola Martinelli, Alessio Branchini, Silvia Linari, Giancarlo Castaman, and Francesco Bernardi

Subjects
Hematology, General Medicine, Genetics (clinical)
Abstract

Gene variation in receptors for circulating factor VIII (FVIII) is candidate to explain the large inter-patient variability of infused FVIII pharmacokinetics (PK) in haemophilia A (HA).To compare in an Italian HA cohort (n = 26) the influence on FVIII PK of genetic components in four von Willebrand factor (VWF)/FVIII receptors.Genotypes of low-density lipoprotein receptor (LDLR), asialoglycoprotein receptor minor subunit (ASGR2), family 4 member M (CLEC4M), stabilin2 (STAB2) and ABO blood-group, and VWF:Ag levels were included as independent variables in linear regression analyses of two-compartment model (TCM) - standard half-life (SHL) FVIII PK parameters.In the initial FVIII distribution phase, the STAB2 rs4981022 AA, ASGR2 rs2289645 TT and LDLR rs688 TT genotypes may contribute to increase CWith the limitation of the small number of HA patients, these observations highlight multiple genetic components acting in distinct phases of FVIII PK and contributing to explain FVIII PK variability. This analysis provides candidates for genotype-based, individual tailoring of FVIII substitutive treatment.

Published
2022

2. The p.P1127S pathogenic variant lowers von Willebrand factor levels through higher affinity for the macrophagic scavenger receptor LRP1: Clinical phenotype and pathogenic mechanisms

Author

Monica Sacco, Stefano Lancellotti, Alessio Branchini, Maira Tardugno, Maria Francesca Testa, Barbara Lunghi, Francesco Bernardi, Mirko Pinotti, Betti Giusti, Giancarlo Castaman, and Raimondo De Cristofaro

Subjects
Factor VIII, asialoglycoprotein receptor 2, scavenger receptors, Settore MED/09 - MEDICINA INTERNA, Hematology, von Willebrand factor, Young Adult, von Willebrand Diseases, HEK293 Cells, Phenotype, Platelet Glycoprotein GPIb-IX Complex, protein conformation, lipoprotein receptor-related protein 1, Humans, Female, von Willebrand disease, Low Density Lipoprotein Receptor-Related Protein-1
Abstract

The index case is a 21-year-old Italian woman with a mild hemorrhagic syndrome and von Willebrand factor antigen (VWF:Ag) = 34.3 U/dl, VWF recombinant glycoprotein Ib (VWF:GpIbR) = 32.8 U/dl, and factor VIII (FVIII) = 55.3 IU/dl.The aim of this study is to characterize from a genetic and biochemical standpoint this low VWF phenotype.Coagulation and biochemical methods were used to study the structural and functional pattern of VWF multimers in the index case's plasma. Recombinant wild-type and p.P1127S VWF variants were produced using human embryonic kidney (HEK)-293 cells. In addition, genetic screening was carried out to detect single nucleotide variants of some scavenger VWF/FVIII receptor genes such as CLEC4M, STAB2, and ASGR2.Genetic investigation revealed that the index case inherited from her mother the heterozygous missense mutation c.3379C T (VWF exon 25), causing the p.P1127S substitution in the VWF D'D3 domain. The index case was also homozygous for the scavenger receptor ASGR2 c.-95 CC-genotype. Desmopressin normalized the VWF level of the patient, although its clearance was faster (tThe p.P1127S variant may cause a low VWF phenotype, stemming from an increased VWF affinity for the scavenger receptor LRP1 and, consequently, an accelerated clearance of VWF.

Published
2022

3. Asymptomatic carriership of factor V Leiden and genotypes of the fibrinogen gene cluster

Author

Francesco Bernardi, Gualtiero Palareti, Paolo Ferraresi, Cristina Legnani, Mirko Pinotti, Sergio Coccheri, Giovanna Marchetti, Chiara Scapoli, Donato Gemmati, and Barbara Lunghi

Subjects
Genetics, medicine.medical_specialty, biology, business.industry, Factor V, Hematology, medicine.disease, Fibrinogen, Thrombophilia, Asymptomatic, Gastroenterology, Internal medicine, Genotype, Coagulopathy, biology.protein, Factor V Leiden, Medicine, medicine.symptom, business, Asymptomatic carrier, medicine.drug
Abstract

Summary. We investigated the role of frequent fibrinogen polymorphisms in venous thromboembolic disease in conjunction with inherited thrombophilia. Two hundred unrelated subjects, all carriers of the factor V R506Q mutation (FV Leiden), were genotyped at the fibrinogen gene cluster. Among these subjects, 100 had experienced previous venous thromboembolism (VTE) and 100 were still asymptomatic for VTE. Significant differences were observed between the groups for the BclI polymorphism (P = 0·004). Scanning, by sequencing the DNA regions flanking the BclI marker, revealed new polymorphisms, a C to T transition and a G to T transversion at 1520 and 3369 base pairs 3′ to the β gene stop codon respectively. These markers showed less association with the clinical phenotype than BclI itself. A combined genotype including 10 markers was more frequent among the asymptomatic subjects (17%) than among patients (3%), and was associated with a reduction in fibrinogen antigen level (2·42 ± 0·35 vs 2·69 ± 0·41 g/l, P = 0·028) among the asymptomatic subjects. Our data suggest that, in the presence of inherited thrombophilia, frequent fibrinogen polymorphisms may interact to modulate the risk of venous thromboembolism.

Published
2003

4. Molecular bases of CRM+factor X deficiency: a frequent mutation (Ser334Pro) in the catalytic domain and a substitution (Glul02Lys) in the second EGF-like domain

Author

M. G. Di Iasio, Giancarlo Castaman, Francesco Bernardi, M. Ruggieri, Barbara Lunghi, Giovanna Marchetti, Francesco Rodeghiero, and Mirko Pinotti

Subjects
Genetics, Serine protease, Mutation, biology, EGF-like domain, Factor X, factor X deficiency, Hematology, Gene mutation, Compound heterozygosity, medicine.disease_cause, chemistry.chemical_compound, dysfunctional proteins, gene mutations, chemistry, medicine, biology.protein, Missense mutation, Gene
Abstract

Summary. The presence of gene lesions in coagulation factor X (FX, Stuart factor) was investigated in asymptomatic subjects with FX deficiency characterized by the presence of dysfunctional molecules in plasma, as demonstrated by the discrepancy between clotting activity and antigen level. A missense mutation (Ser334Pro) in the catalytic domain was found in three unrelated families in both the homozygous and the heterozygous conditions, and also in the compound heterozygous form with the substitution of Lys for 102 Glu. None of the mutations was detected in 40 unrelated subjects from the same geographic area. The Ser334Pro mutation affects a serine protease region characterized by extensive variation in the coagulation factors but conserved in mammalian factor X molecules. The Glul02Lys mutation affects a residue of the second EGF-like module also conserved in protein C. Both mutated residues are surface-exposed and found in protein regions suggested to be involved in macromolecular interactions which are impaired in the dysfunctional molecules.

Published
1995

6. A highly polymorphic microsatellite in the factor V gene is an informative tool for the study of factor V-related disorders

Author

Antonio Girolami, Elisabetta Castoldi, Francesco Bernardi, Barbara Lunghi, Federico Mingozzi, and Paolo Simioni

Subjects
Factor V gene, Genetic Markers, Male, Factor V Deficiency, VNTR, Thrombophilia, Polymerase Chain Reaction, Gene Frequency, Factor V Leiden, medicine, Humans, Allele, Gene, Genetics, Factor V deficiency, R2 allele, Polymorphism, Genetic, biology, Factor V, Hematology, medicine.disease, Molecular biology, Pedigree, Italy, Genetic marker, biology.protein, Microsatellite, Female, Microsatellite Repeats
Abstract

The role of factor V (FV) mutations in activated protein C (APC) resistance and FV deficiency is well established. We report on the identification of a highly polymorphic (AT)n microsatellite marker in the FV gene, which represents an informative tool for the investigation of the origin and evolution of pathologically relevant FV genetic components. A high number of different microsatellite alleles were found to be associated with FV R506Q and FV H1299R, two single-origin mutations. An example of the use of the microsatellite marker in family studies of thrombophilia and FV deficiency is also provided.

Published
2001

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