Your search keyword '"Bovill E"' showing total 13 results

1. Genetic variants associated with protein C levels.

Author

Vossen CY, Koeleman BP, Hasstedt SJ, Nijman IJ, Renkens IJ, Callas PW, Rosendaal FR, and Bovill EG

Subjects

Case-Control Studies, Genetic Linkage, Humans, Protein C genetics, Polymorphism, Single Nucleotide, Protein C metabolism

Abstract

Background: Normal protein C (PC) plasma levels range widely in the general population. Factors influencing normal PC levels are thought to influence the risk of venous thrombosis. Little is known about the underlying genetic variants., Objectives: We performed a genome scan of normal PC levels to identify genes that regulate normal PC levels., Patients/methods: We performed a variance components linkage analysis for normal PC levels in 275 individuals from a single, large family. We then sequenced candidate genes under the identified linkage peak in eight family members: four with high and four with low, but normal, PC levels. For variants showing a difference in carriers between those with high and low PC levels, we re-evaluated linkage in the 275 family members conditional on the measured genotype effect. Genotype-specific mean PC levels were determined using likelihood analysis. Findings were replicated in the Leiden Thrombophilia Study (LETS)., Results: We identified a quantitative trait locus at chromosome 5q14.1 affecting normal PC plasma level variability. Next-generation sequencing of 113 candidate genes under the linkage peak revealed four SNPs in BHMT2, ACOT12, SSBP2 and XRCC4, which significantly increased PC levels in our thrombophilic family, but not in LETS., Conclusions: We identified four genes at chromosome 5q14.1 that might influence normal PC levels. BHMT2 seems the most likely candidate to regulate PC levels via homocysteine, a competitive inhibitor to thrombin. Failure to replicate our findings in LETS might be due to differences between the studies in genetic background and linkage disequilibrium patterns., (© 2013 International Society on Thrombosis and Haemostasis.)

Published

2013

2. Genome scan of clot lysis time and its association with thrombosis in a protein C-deficient kindred.

Author

Meltzer ME, Hasstedt SJ, Vossen CY, Callas PW, DE Groot PG, Rosendaal FR, Lisman T, and Bovill EG

Subjects

Blood Coagulation Tests, Carboxypeptidase B2 genetics, Chromosomes, Human, Pair 11, Chromosomes, Human, Pair 13, Family, Genetic Linkage, Humans, Mutation, Protein C Deficiency genetics, Prothrombin genetics, Quantitative Trait Loci, Fibrinolysis genetics, Genome, Human physiology, Protein C Deficiency physiopathology, Thrombosis genetics

Abstract

Background:  Previously, we found increased clot-lysis time (CLT), as measured with a plasma-based assay, to increase the risk of venous thrombosis in two population-based case-control studies. The genes influencing CLT are as yet unknown., Patients/methods:  We tested CLT as risk factor for venous thrombosis in Kindred Vermont II (n = 346), a pedigree suffering from a high thrombosis risk, partially attributable to a type I protein C deficiency. Furthermore, we tested for quantitative trait loci (QTLs) for CLT, using variance component linkage analysis., Results:  Protein C-deficient family members had shorter CLTs than non-deficient members (median CLT 67 min vs. 75 min). One standard deviation increase in CLT increased the risk of venous thrombosis 2.4-fold in non-deficient family members. Protein C deficiency without elevated CLT increased the risk 6.9-fold. Combining both risk factors yielded a 27.8-fold increased risk. The heritability of CLT was 42-52%. We found suggestive evidence of linkage on chromosome 11 (62 cM), partly explained by the prothrombin 20210A mutation, and on chromosome 13 (52 cM). Thrombin-activatable fibrinolysis inhibitor genotypes did not explain the variation in CLT., Conclusion: Hypofibrinolysis appears to increase thrombosis risk in this family, especially in combination with protein C deficiency. Protein C deficiency is associated with short CLT. CLT is partly genetically regulated. Suggestive QTLs were found on chromosomes 11 and 13., (© 2011 International Society on Thrombosis and Haemostasis.)

Published

2011

3. Risk factors for peripheral venous disease resemble those for venous thrombosis: the San Diego Population Study.

Author

Cushman M, Callas PW, Denenberg JO, Bovill EG, and Criqui MH

Subjects

Age Factors, Aged, California, Case-Control Studies, Factor V genetics, Female, Genetic Predisposition to Disease, Hemostasis, Humans, Male, Middle Aged, Odds Ratio, Prothrombin genetics, Risk Factors, Peripheral Vascular Diseases diagnosis, Peripheral Vascular Diseases epidemiology, Venous Thrombosis diagnosis, Venous Thrombosis epidemiology

Abstract

Background: Clinically silent deep vein thrombosis (DVT) is common and may cause chronic venous disease that resembles post-thrombotic syndrome., Objective: We evaluated whether peripheral venous disease in a general population shares risk factors with DVT., Methods: In an established cohort of 2404 men and women, the San Diego Population Study, peripheral venous disease was evaluated using physical examination, symptom assessment and venous ultrasound. We performed a case-control study including 308 cases in four hierarchical groups by severity and 346 controls without venous abnormalities, frequency matched to cases by 10-year age group, race and gender. Cases and controls had no prior history of venous thrombosis. Hemostatic risk factors were measured in cases and controls., Results: Accounting for age, obesity and family history of leg ulcer, odds ratios (ORs) of venous disease for elevated factor VIII, von Willebrand factor (VWF), D-dimer and for factor V Leiden were 1.4 (95% CI 0.9-2.1), 1.5 (CI 1.0-2.3), 1.7 (CI 1.1-2.8) and 1.1 (CI 0.5-2.4), respectively. These associations were larger for the two most severe case groups; ORs 2.0 (CI 1.0-3.8), 1.7 (CI 0.9-3.3), 2.7 (CI 1.2-6.1) and 2.3 (CI 0.8-7.1). Each hemostatic factor was also associated with severity of venous disease, for example elevated D-dimer was associated with a 2.2-fold increased odds of being in one higher severity case group. Prothrombin 20210A was not associated with venous disease., Conclusions: DVT risk factors are associated with presence and severity of peripheral venous disease. Results support a hypothesis that peripheral venous disease may sometimes be post-thrombotic syndrome as a result of a previous unrecognized DVT., (© 2010 International Society on Thrombosis and Haemostasis.)

Published

2010

4. Computational candidate gene prioritization for venous thrombosis.

Author

Vossen CY, Elbers CC, Koeleman BP, Rosendaal FR, and Bovill EG

Subjects

Chromosomes, Human, Pair 11, Computational Biology methods, Genetic Linkage, Genetic Predisposition to Disease, Humans, Models, Genetic, Sequence Analysis, DNA, Software, Venous Thrombosis genetics

Published

2010

5. A genetic basis for the interrelation of coagulation factors.

Author

Vossen CY, Callas PW, Hasstedt SJ, Long GL, Rosendaal FR, and Bovill EG

Subjects

Adolescent, Adult, Aged, Child, Preschool, Humans, Infant, Middle Aged, Multigene Family, Mutation, Protein C genetics, Prothrombin genetics, Radioimmunoassay, Blood Coagulation Factors genetics

Abstract

Background: Evidence found in the literature for a strong correlation between coagulation factors suggests that single genes might influence the plasma concentrations of multiple coagulation factors (i.e. pleiotropically acting genes)., Objective: To determine whether there is a genetic basis for the correlation among coagulation factors by assessing the heritability of interrelated coagulation factors., Patients/methods: We performed principal components analysis, and subsequently variance components analysis, to estimate the heritability of principal components of coagulation factors in family members of a large French-Canadian kindred., Results: Four clusters were identified by principal components analysis in 200 family members who did not carry the protein C 3363C mutation. Cluster 1 consisted of prothrombin, factor VII (FVII), FIX, FX and protein S; cluster 2 consisted of FV, FIX, protein C and tissue factor pathway inhibitor; cluster 3 consisted of FVIII and von Willebrand factor; and cluster 4 consisted of antithrombin, protein C and FVII. The heritability of the principal components estimated by variance components analysis was, respectively, 37%, 100%, 37%, and 37%., Conclusion: Our findings support the hypothesis that genes can influence plasma levels of interrelated coagulation factors.

Published

2007

6. Linkage analysis for three coagulation factors clustering on chromosome 13q34: factor VII, factor X and protein Z.

Author

Vossen CY, Hasstedt SJ, Demers C, Rosendaal FR, and Bovill EG

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Female, Genetic Linkage, Humans, Infant, Infant, Newborn, Male, Middle Aged, Multigene Family, Polymorphism, Single Nucleotide, Protein C Deficiency blood, Protein C Deficiency genetics, Blood Proteins genetics, Chromosomes, Human, Pair 13 genetics, Factor VII genetics, Factor X genetics

Published

2007

7. A genome search for genetic determinants of markers of protein C activation.

Author

Vossen CY, Hasstedt SJ, Scott BT, Rosendaal FR, and Bovill EG

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, Chromosome Mapping, Female, Humans, Infant, Inheritance Patterns, Lod Score, Male, Middle Aged, Protein C Deficiency blood, Protein C Inhibitor blood, Quantitative Trait Loci, alpha 1-Antitrypsin metabolism, Genetic Markers, Protein C metabolism, Protein C Deficiency genetics

Published

2006

8. Attitudes toward genetic testing for thrombophilia in asymptomatic members of a large family with heritable protein C deficiency.

Author

van Korlaar IM, Vossen CY, Rosendaal FR, Bovill EG, Naud S, Cameron LD, and Kaptein AA

Subjects

Adolescent, Adult, Aged, Anxiety, Female, Genetic Predisposition to Disease, Humans, Incidence, Intention, Male, Middle Aged, North America, Pedigree, Protein C Deficiency complications, Protein C Deficiency epidemiology, Risk Factors, Stress, Psychological, Thrombophilia etiology, Venous Thrombosis etiology, Genetic Testing psychology, Health Knowledge, Attitudes, Practice, Protein C Deficiency genetics, Thrombophilia genetics, Venous Thrombosis genetics

Abstract

Background: Little research has been performed regarding the psychological consequences of knowing that one is at an increased risk for venous thrombosis., Objectives: The aim of this study was to explore attitudes toward genetic testing for protein C deficiency., Methods: Questionnaires about genetic testing attitudes, dispositional anxiety, risk perception, and thrombosis-related worry were completed by 168 asymptomatic members of a North-American kindred with a high incidence of heritable protein C deficiency conferring a high lifetime risk of venous thrombosis. A total of 76 subjects (45%) had not been tested for protein C deficiency before participating in our study whereas the other 92 subjects (55%) had been tested prior to filling in the questionnaire, of whom 34 people had protein C deficiency, while 58 did not., Results: Family members with protein C deficiency perceived a higher risk of suffering venous thrombosis and scored higher on thrombosis-related worry than family members without protein C deficiency. Participants who had not been tested did not report excessive thrombosis-related worry. Participants with protein C deficiency reported a belief in the psychological and health benefits of testing, and felt that they experienced low psychological distress following the genetic test. High psychological distress following the test was related to dispositional anxiety and thrombosis-related worry. Participants without protein C deficiency were relieved after finding out that they did not have the deficiency., Conclusion: There seem to be few negative psychological consequences of knowing that one is at an increased risk for venous thrombosis, except in vulnerable individuals.

Published

2005

9. Chronic venous abnormalities in symptomatic and asymptomatic protein C deficiency.

Author

Emmerich J, Vossen CY, Callas PW, Demers C, Naud S, Long GL, Couture P, Rosendaal FR, and Bovill EG

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Body Mass Index, Family Health, Female, Genotype, Humans, Male, Middle Aged, Mutation, Phenotype, Protein C genetics, Pulmonary Embolism complications, Pulmonary Embolism diagnosis, Risk, Thrombophilia complications, Thrombophilia diagnosis, Thrombosis, Ultrasonography, Venous Thrombosis diagnosis, Protein C Deficiency complications, Protein C Deficiency diagnosis, Venous Thrombosis complications

Abstract

Background: Thrombophilia is a frequent medical condition associated with symptomatic deep vein thrombosis (DVT). Unlike other clinical risk factors associated with DVT, such as surgery, thrombophilia has not been demonstrated to be associated with asymptomatic venous thrombotic events. Our aim was to search for asymptomatic sequelae of DVT in a protein C (PC)-deficient family., Methods: We studied 228 individuals from a large kindred with PC deficiency and performed a systematic ultrasound examination., Results: Among the 203 patients without a known history of venous thrombosis we found seven patients with abnormalities indicative of prior asymptomatic thrombosis: six (7.4%) in the PC-deficient group (n = 81) and only one (0.8%) in the non-deficient group (n = 122). The relative risk for these sequelae associated with PC deficiency was 9.0 (95% CI: 1.1-73.7)., Conclusions: These data suggest that chronic venous abnormalities are frequently present and that thrombotic events in asymptomatic individuals with familial PC deficiency may be underestimated.

Published

2005

10. First experience with direct, selective factor Xa inhibition in patients with non-ST-elevation acute coronary syndromes: results of the XaNADU-ACS Trial.

Author

Alexander JH, Yang H, Becker RC, Kodama K, Goodman S, Dyke CK, Kleiman NS, Hochman JS, Berger PB, Cohen EA, Lincoff AM, Burton JR, Bovill EG, Kawai C, Armstrong PW, and Harrington RA

Subjects

Acute Disease, Adult, Aged, Aged, 80 and over, Coronary Artery Disease complications, Coronary Artery Disease mortality, Dose-Response Relationship, Drug, Electrocardiography, Female, Hemorrhage chemically induced, Heparin administration & dosage, Heparin toxicity, Humans, Ischemia prevention & control, Male, Middle Aged, Myocardial Infarction prevention & control, Naphthalenes administration & dosage, Naphthalenes toxicity, Partial Thromboplastin Time, Propionates administration & dosage, Propionates toxicity, Serine Endopeptidases therapeutic use, Coronary Artery Disease drug therapy, Factor Xa Inhibitors, Serine Endopeptidases administration & dosage

Abstract

Background: Unfractionated heparin is widely used in patients with non-ST-elevation acute coronary syndromes but has important limitations. Anticoagulants with predictable kinetics and anticoagulant effects, better efficacy, and greater safety are needed., Objective: To investigate the efficacy and safety of a direct, selective factor Xa inhibitor, DX-9065a (Daiichi Pharmaceuticals LTD, Inc.) compared with heparin, in patients with non-ST-elevation acute coronary syndromes., Patients and Methods: Patients (n = 402) from the USA, Canada, and Japan were randomized to blinded, weight-adjusted heparin, low-dose DX-9065a, or high-dose DX-9065a., Results: The primary efficacy endpoint of death, myocardial infarction, urgent revascularization, or ischemia on continuous ST-segment monitoring occurred in 33.6%, 34.3%, and 31.3% of patients assigned to heparin, low-dose DX-9065a, and high-dose DX-9065a (P = 0.91 for heparin vs. combined DX-9065a). The composite of death, myocardial infarction, or urgent revascularization occurred in 19.5%, 19.3%, and 11.9% (P = 0.125 for heparin vs. high-dose DX-9065a) of patients; major or minor bleeding occurred in 7.7%, 4.2%, and 7.0% of patients; and major bleeding in 3.3%, 0.8%, and 0.9% of patients. Higher concentrations of DX-9065a were associated with a lower likelihood of ischemic events (P = 0.03) and a non-significant tendency toward a higher likelihood of major bleeding (P = 0.32)., Conclusions: In this small phase II trial, there was a non-significant tendency toward a reduction in ischemic events and bleeding with DX-9065a compared with heparin in patients with acute coronary syndromes. The absence of an effect on ST-monitor ischemia warrants further investigation. These data provide the rationale for adequately powered studies of DX-9065a in acute coronary syndromes or percutaneous intervention.

Published

2005

11. Genome scan of venous thrombosis in a pedigree with protein C deficiency.

Author

Hasstedt SJ, Scott BT, Callas PW, Vossen CY, Rosendaal FR, Long GL, and Bovill EG

Subjects

Adolescent, Adult, Aged, Chromosome Mapping, Chromosomes, Human, Pair 10, Chromosomes, Human, Pair 11, Family Health, Female, Genetic Linkage, Genetic Predisposition to Disease, Genotype, Humans, Male, Middle Aged, Mutation, Pedigree, Protein C Deficiency complications, Thrombophilia complications, Venous Thrombosis etiology, Genomics methods, Protein C Deficiency genetics, Thrombophilia genetics, Venous Thrombosis genetics

Abstract

Kindred Vermont II has a high frequency of venous thrombosis, occurring primarily in pedigree members with type I protein C deficiency due to a 3363 inserted (Ins) C mutation in exon 6 of the protein C gene. However, only a subset of 3363 InsC carriers have suffered thrombotic episodes, suggesting that the increased risk of thrombosis results upon the co-occurrence of 3363 InsC with a second, unknown, thrombophilic mutation that segregates independently within the pedigree. To test this hypothesis and to localize the co-occurring gene, we performed a genome scan of venous thrombosis in Kindred Vermont II. Non-parametric linkage statistics identified three potential gene locations, on chromosomes 11q23 (nominal P < 0.0001), 18p11.2-q11.2 (P < 0.0007), and 10p12 (P < 0.0003), supporting the presence of at least one additional thrombophilic mutation in the pedigree. Identification of the unknown mutation(s) promises to reveal a new genetic risk factor for thrombophilia, contribute to our understanding of the blood clotting mechanism, and expand our knowledge of the diversity of oligogenic disease.

Published

2004

12. Heritability of plasma concentrations of clotting factors and measures of a prethrombotic state in a protein C-deficient family.

Author

Vossen CY, Hasstedt SJ, Rosendaal FR, Callas PW, Bauer KA, Broze GJ, Hoogendoorn H, Long GL, Scott BT, and Bovill EG

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Blood Coagulation Factors analysis, Blood Proteins analysis, Child, Child, Preschool, Family Characteristics, Family Health, Female, Genetic Linkage, Humans, Infant, Inheritance Patterns, Male, Middle Aged, Phenotype, Protein C Deficiency blood, Blood Coagulation Factors genetics, Protein C Deficiency genetics, Thrombophilia genetics

Abstract

Background: Earlier studies found strong support for a genetic basis for regulation of coagulation factor levels and measures of a prethrombotic state (d-dimer, prothrombin fragment 1.2)., Objectives: Estimation of how much of the variation in the levels of coagulation factors and measures of a prethrombotic state, including measures of protein C activation and inactivation, could be attributed to heritability and household effect., Patients and Methods: Blood samples were collected from 330 members of a large kindred of French-Canadian origin with type I protein C deficiency. Heritability and common household effect were estimated for plasma concentrations of prothrombin, factor (F)V, factor VIII, factor (F)IX, fibrinogen, von Willebrand factor (VWF), antithrombin, protein C, protein S, protein Z, protein Z-dependent protease inhibitor (ZPI), fibrinopeptide A (FPA), protein C activation peptide (PCP), activated protein C-protein C inhibitor complex (APC-PCI), activated protein C-alpha1-antitrypsin complex (APC-alpha1AT), prothrombin fragment 1.2 (F1.2) and d-dimer, using the variance component method in sequential oligo-genic linkage analysis routines (SOLAR)., Results: The highest heritability was found for measures of thrombin activity (PCP and FPA). High estimates were also found for prothrombin, FV, FIX, protein C, protein Z, ZPI, APC-PCI and APC-alpha1AT. An important influence of shared household effect on phenotypic variation was found for VWF, antithrombin, protein S and F1.2., Conclusions: We found strong evidence for the heritability of single coagulation factors and measures of a prethrombotic state. Hemostatic markers with statistically significant heritability constitute potential targets for the identification of novel genes involved in the control of quantitative trait loci.

Published

2004

13. Initial experience with factor-Xa inhibition in percutaneous coronary intervention: the XaNADU-PCI Pilot.

Author

Alexander JH, Dyke CK, Yang H, Becker RC, Hasselblad V, Zillman LA, Kleiman NS, Hochman JS, Berger PB, Cohen EA, Lincoff AM, Saint-Jacques H, Chetcuti S, Burton JR, Buergler JM, Spence FP, Shimoto Y, Robertson TL, Kunitada S, Bovill EG, Armstrong PW, and Harrington RA

Subjects

Aged, Anticoagulants blood, Anticoagulants pharmacokinetics, Blood Coagulation Tests, Dose-Response Relationship, Drug, Drug Monitoring methods, Feasibility Studies, Female, Heparin administration & dosage, Humans, International Normalized Ratio, Intraoperative Care, Male, Middle Aged, Naphthalenes blood, Naphthalenes pharmacokinetics, Pilot Projects, Postoperative Complications prevention & control, Propionates blood, Propionates pharmacokinetics, Thrombosis etiology, Anticoagulants administration & dosage, Cardiac Surgical Procedures adverse effects, Factor Xa Inhibitors, Naphthalenes administration & dosage, Propionates administration & dosage, Thrombosis prevention & control

Abstract

Background: Direct factor (F)Xa inhibition is an attractive method to limit thrombotic complications during percutaneous coronary intervention (PCI)., Objectives: To investigate drug levels achieved, effect on coagulation markers, and preliminary efficacy and safety of several doses of DX-9065a, an intravenous, small molecule, direct, reversible FXa inhibitor during PCI., Patients and Methods: Patients undergoing elective, native-vessel PCI (n = 175) were randomized 4 : 1 to open-label DX-9065a or heparin in one of four sequential stages. DX-9065a regimens in stages I-III were designed to achieve concentrations of > 100 ng mL-1, > 75 ng mL-1, and > 150 ng mL-1. Stage IV used the stage III regimen but included patients recently given heparin., Results: At 15 min median (minimum) DX-9065a plasma levels were 192 (176), 122 (117), 334 (221), and 429 (231) ng mL-1 in stages I-IV, respectively. Median whole-blood international normalized ratios (INRs) were 2.6 (interquartile range 2.5, 2.7), 1.9 (1.8, 2.0), 3.2 (3.0, 4.1), and 3.8 (3.4, 4.6), and anti-FXa levels were 0.36 (0.32, 0.38), 0.33 (0.26, 0.39), 0.45 (0.41, 0.51), and 0.62 (0.52, 0.65) U mL-1, respectively. Stage II enrollment was stopped (n = 7) after one serious thrombotic event. Ischemic and bleeding events were rare and, in this small population, showed no clear relation to DX-9065a dose., Conclusions: Elective PCI is feasible using a direct FXa inhibitor for anticoagulation. Predictable plasma drug levels can be rapidly obtained with double-bolus and infusion DX-9065a dosing. Monitoring of DX-9065a may be possible using whole-blood INR. Direct FXa inhibition is a novel and potentially promising approach to anticoagulation during PCI that deserves further study.

Published

2004