Your search keyword '"Bovill E"' showing total 12 results

1. Combined coagulation phase-directed factor Xa inhibition with heparin compounds and DX-9065a - a direct and selective antagonist.

Author

Becker RC, Alexander J, Li YF, Bovill E, Spencer FA, Robertson TL, Kunitada S, Dyke CK, and Harrington RA

Subjects

Anticoagulants administration & dosage, Blood Coagulation Tests, Calcium Chloride pharmacology, Camptothecin administration & dosage, Drug Synergism, Factor Xa chemistry, Heparin administration & dosage, Heparin blood, Heparin metabolism, Heparin, Low-Molecular-Weight blood, Humans, Sensitivity and Specificity, Anticoagulants pharmacology, Camptothecin analogs & derivatives, Camptothecin pharmacology, Enoxaparin pharmacology, Factor Xa Inhibitors, Heparin pharmacology

Published

2004

2. Quality of life in venous disease.

Author

van Korlaar I, Vossen C, Rosendaal F, Cameron L, Bovill E, and Kaptein A

Subjects

Chronic Disease, Female, Humans, Leg Ulcer psychology, Longitudinal Studies, Male, Quality of Life, Severity of Illness Index, Surveys and Questionnaires, Thrombophlebitis psychology, Varicose Veins psychology, Venous Insufficiency psychology, Venous Thrombosis therapy, Venous Thrombosis psychology

Abstract

Quality of life (QOL) can be defined as the functional effect of an illness and its consequent therapy upon a patient, as perceived by the patient. Studies on the impact of chronic venous disease on quality of life are scarce compared to quality of life research in other diseases. The purpose of this paper was to describe instruments that assess the quality of life in patients with chronic venous disease and to review the literature on this topic. A computer search of the MedLine database was performed to identify papers; the bibliographies of relevant articles were reviewed to obtain additional papers. Papers were included if they described the development or use of a quality of life instrument for patients with chronic venous disease. A total of 25 papers were identified that fit the inclusion criteria. The studies described in the papers used six different generic instruments and ten disease-specific instruments. Quality of life in chronic venous disease was assessed in 12 studies. Six studies compared different types of treatment for chronic venous disease where QOL was an outcome measure. Despite the wide variety of measures used, results indicate that the quality of life of patients with chronic venous disease is affected in the physical domain mostly with regard to pain, physical functioning and mobility, and that they suffer from negative emotional reactions and social isolation. We feel that QOL should be a standard measure in future studies in patients with chronic venous disease, preferably with a combination of generic and disease-specific measures.

Published

2003

3. Evidence of a founder effect for the protein C gene 3363 inserted C mutation in thrombophilic pedigrees of French origin.

Author

Couture P, Bovill EG, Demers C, Simard J, Delage R, Scott BT, Valliere JE, Callas PW, Jomphe M, Rosendaal FR, Aiach M, and Long GL

Subjects

Consanguinity, Emigration and Immigration history, Exons genetics, Female, France epidemiology, France ethnology, Heterozygote, History, 17th Century, Humans, Male, Microsatellite Repeats, Pedigree, Quebec ethnology, Registries, Thrombophilia epidemiology, Thrombophilia history, Vermont epidemiology, Founder Effect, Mutagenesis, Insertional, Protein C genetics, Thrombophilia genetics

Abstract

We have previously reported that the 3363 inserted (Ins) C mutation in exon 6 of the protein C gene was present in four unrelated French patients and in four French Canadian families with type I protein C deficiency as well as in a large Vermont protein C deficient kindred of French Canadian origin. The present study was designed to investigate the likelihood of the existence of a founder effect for this mutation in protein C deficient individuals of French origin living in France, Quebec and Vermont. In order to demonstrate a possible founder effect for the 3363 InsC mutation, we have previously constructed a high-resolution genetic map to locate several highly polymorphic markers close to the protein C locus. Thereafter, the markers D2S347, D2S2339, D2S383, D2S2271 and D2S2215 were genotyped in 117 heterozygotes from France (n = 7), Quebec (n = 36) or Vermont (n = 74). The allelic frequency distribution of these five markers was also determined in fifty control French Canadian subjects and thirty-two unaffected members of the Vermont kindred with normal protein C levels and compared with their frequency in our cohort of heterozygotes. Our data suggest that patients from Quebec and Vermont carry a common haplotype at the protein C locus. Moreover, in order to study the evolutionary history of the 3363 InsC mutation, we traced back the ascending genealogy of one proband in each of the families with this mutation. These results showed that the 3363 InsC mutation was most probably introduced in North America by a couple of French settlers who established themselves in 1669 on Isle d'Orleans located near Quebec City. All heterozygotes for the 3363 InsC mutation living in North America are related to these founders within 10 generations. Thus, these families afford a unique opportunity to evaluate the role of the protein C system in thrombophilia due to the high degree of linkage disequilibrium at the protein C gene, which in essence holds that variable more constant than in a more heterogeneous population.

Published

2001

4. Genetic screening of candidate genes for a prothrombotic interaction with type I protein C deficiency in a large kindred.

Author

Scott BT, Bovill EG, Callas PW, Hasstedt SJ, Leppert MF, Valliere JE, Varvil TS, and Long GL

Subjects

Blood Coagulation Factors genetics, Blood Proteins genetics, Family Health, Female, Gene Frequency, Genetic Linkage, Genetic Markers, Genetic Predisposition to Disease genetics, Genome, Humans, Male, Mutation, Pedigree, Polymorphism, Genetic, Protein C Deficiency complications, Tandem Repeat Sequences, Thrombosis etiology, Thrombosis genetics, Genetic Testing, Protein C Deficiency genetics, Thrombophilia genetics

Abstract

The incomplete penetrance of thrombosis in familial protein C deficiency suggests disease occurs when this deficit is combined with additional abnormalities in the hemostatic system. The pattern of inherited thrombophilia in the Vermont II kindred, which is affected by a clinically dominant type I protein C deficiency, provides strong evidence for a second unidentified gene that segregates independently of protein C deficiency and increases susceptibility to thrombosis. To test the second gene hypothesis, thirty-four candidate genes for proteins involved in hemostasis or inflammation were tested as the unknown defect, using highly polymorphic short tandem repeat (STR) markers in an informative subset (n = 31) of the kindred. The genes considered are; alpha-fibrinogen, beta-fibrinogen, gamma-fibrinogen, prothrombin, tissue factor, factor V, protein S, complement component 4 binding protein, factor XI, factor XII, factor XIIIa, factor XIIIb, histidine rich glycoprotein, high molecular weight kininogen, kallikrein, von Willebrands factor, platelet factor 4, thrombospondin, antithrombin III, alpha-1-antitrypsin, thrombomodulin, plasminogen, tissue plasminogen activator, urokinase plasminogen activator, plasminogen activator inhibitor-1, plasminogen activator inhibitor-2, protein C inhibitor, alpha-2-plasmin inhibitor, kallistatin, lipoprotein a, interleukin 6, interleukin 1, cystathionine-beta-synthase, and methylenetetrahydrofolate reductase. Mutations in many of these genes have been previously established as independent risk factors for thrombosis. However, linkage analysis provided no evidence to implicate any of the candidate genes as the second inherited factor that promotes thrombophilia in this kindred.

Published

2001

5. The G20210A prothrombin polymorphism is not associated with increased thromboembolic risk in a large protein C deficient kindred.

Author

Bovill EG, Hasstedt SJ, Callas PW, Valliere JE, Scott BT, Bauer KA, and Long GL

Subjects

Female, Genotype, Humans, Male, Pedigree, Point Mutation, Protein C Deficiency blood, Risk Factors, Thromboembolism blood, Polymorphism, Genetic, Protein C Deficiency complications, Protein C Deficiency genetics, Prothrombin genetics, Thromboembolism etiology, Thromboembolism genetics

Abstract

Likelihood analysis was used to test the effect of the G20210A prothrombin mutation and the His107Pro protein C mutation (resulting from a C insertion) on thrombosis status and prothrombin level in a large kindred of French Canadian descent with type I protein C deficiency. Genotypes were available on 279 pedigree members or their spouses. Of this total, 36 pedigree members were heterozygous for the G20210A variant and one pedigree member was homozygous for G20210A, while 64 were heterozygous for the His107Pro protein C mutation. The factor V Leiden mutation (Arg506Gln) was observed in only one of 181 tested family members. Objectively verified thrombosis was present in 26 of the 279 pedigree members. Thrombosis was suspected in an additional 19 pedigree members. The transmission disequilibrium test of Spielman, 1996, as extended to pedigrees, was used to test for excess transmission of G20210A or His107Pro to thrombosis cases, with transmission of 0.5 specifying no effect. Although the His107Pro mutation was over transmitted (0.837 +/- 0.075 p <0.001) to thrombosis cases in this pedigree, the G20210A variant was not (0.491 +/- 0.130 NS). Measured genotype analysis was used to examine a total of 184 individuals for the relationship between prothrombin level and both the G20210A variant and thrombosis. The G20210A variant increased prothrombin level from 97 +/- 2% to 124 +/- 4% (p <0.0001), but thrombosis status was not associated with any additional increase in prothrombin level. Thus, in a large thrombophilic, protein C deficient kindred, with the G20210A variant present in a proportion (13%) far higher than the general Caucasian population (approximately 2%), neither the presence of the variant nor the plasma concentration of prothrombin were associated with increased risk for thrombosis. These findings contrast with those of others who have established the G20210A variant as a thrombophilic risk factor; and emphasize the complex nature of the multigenic pathogenesis of thrombophilia.

Published

2000

6. Hereditary thrombophilia as a model for multigenic disease.

Author

Bovill EG, Hasstedt SJ, Leppert MF, and Long GL

Subjects

Humans, Multigene Family, Pedigree, Risk Factors, Thrombophilia epidemiology, Thrombophilia genetics

Published

1999

7. Plasmin-alpha2-antiplasmin complex in patients with atrial fibrillation. Stroke Prevention in Atrial Fibrillation Investigators.

Author

Feinberg WM, Macy E, Cornell ES, Nightingale SD, Pearce LA, Tracy RP, and Bovill EG

Subjects

Aged, Anticoagulants therapeutic use, Atrial Fibrillation drug therapy, Atrial Fibrillation physiopathology, Cerebrovascular Disorders etiology, Female, Fibrinolysin analysis, Humans, Male, Middle Aged, Multivariate Analysis, Risk Factors, Warfarin therapeutic use, alpha-2-Antiplasmin analysis, Antifibrinolytic Agents, Atrial Fibrillation blood, Fibrinolysin metabolism, alpha-2-Antiplasmin metabolism

Abstract

Plasmin-alpha2-antiplasmin complex (PAP) is an index of recent fibrinolytic activity. We examined PAP levels in patients with atrial fibrillation (AF) to determine whether these levels are correlated with clinical characteristics associated with stroke risk. We obtained blood for measurement of PAP in a non-random sample of 586 patients with AF on entering the Stroke Prevention in Atrial Fibrillation III Study. PAP levels were measured with an ELISA assay. PAP values were transformed with a natural logarithm (PAPln) prior to all analyses. Older age, female gender, recent congestive heart failure, decreasing fractional shortening, recent onset of AF, and coronary artery disease were each univariately associated with higher levels of PAP (all p<0.05, two-sample t-test, simple linear regression). Older age, recent congestive heart failure, decreasing fractional shortening, and recent onset of AF were independently associated with higher PAP levels by multivariate analysis (linear regression). Among patients receiving warfarin, PAP levels were not correlated with INR levels (linear regression, p=0.60). Patients classified as high-risk for thromboembolism by our risk stratification criteria (systolic blood pressure > 160 mm Hg, prior thromboembolism, recent congestive heart failure, poor left ventricular function, and women over age 75) had higher PAP levels than low-risk patients (antilog mean PAPln 5.6 vs 4.9. p<0.001, two-sample t-test). PAP levels in patients with AF are associated with clinical characteristics predictive of thromboembolism. Elevated PAP levels are particularly associated with poor left ventricular function and are not affected by anticoagulation. PAP levels may be a marker of stroke risk in patients with AF.

Published

1999

8. Dietary vitamin K1 and stability of oral anticoagulation: proposal of a diet with constant vitamin K1 content.

Author

Booth SL, Charnley JM, Sadowski JA, Saltzman E, Bovill EG, and Cushman M

Subjects

Administration, Oral, Anticoagulants administration & dosage, Anticoagulants adverse effects, Coumarins administration & dosage, Coumarins adverse effects, Drug Interactions, Humans, Nutritional Status, Warfarin administration & dosage, Warfarin adverse effects, Warfarin therapeutic use, Anticoagulants therapeutic use, Coumarins therapeutic use, Diet, Vitamin K 1 pharmacology

Abstract

Case reports cited in Medline or Biological Abstracts (1966-1996) were reviewed to evaluate the impact of vitamin K1 dietary intake on the stability of anticoagulant control in patients using coumarin derivatives. Reported nutrient-drug interactions cannot always be explained by the vitamin K1 content of the food items. However, metabolic data indicate that a consistent dietary intake of vitamin K is important to attain a daily equilibrium in vitamin K status. We report a diet that provides a stable intake of vitamin K1 equivalent to the current U.S. Recommended Dietary Allowance, using food composition data derived from high-performance liquid chromatography. Inconsistencies in the published literature indicate that prospective clinical studies should be undertaken to clarify the putative dietary vitamin K1-coumarin interaction. The dietary guidelines reported here may be used in such studies.

Published

1997

9. The pharmacokinetics and lipoprotein fraction distribution of intramuscular vs. oral vitamin K1 supplementation in women of childbearing age: effects on hemostasis.

Author

Hagstrom JN, Bovill EG, Soll RF, Davidson KW, and Sadowski JA

Subjects

Administration, Oral, Adult, Chemical Fractionation, Female, Humans, Injections, Intramuscular, Vitamin K 1 administration & dosage, Hemostasis drug effects, Lipoproteins blood, Vitamin K 1 pharmacokinetics

Abstract

Prenatal maternal vitamin K1 supplementation to improve the hemostatic status of the fetus may depend upon the route of administration and subsequent presentation at the placental barrier. We investigated intramuscular (IM) vs oral (PO) vitamin K1 supplementation in eight healthy, nonpregnant women of childbearing age. Pharmacokinetics were studied in each subject after a 5 mg IM dose and after a 5 mg oral dose of vitamin K1 approximately one month later. Plasma collected at the peak vitamin K level for each treatment was separated into very low density lipoproteins (VLDL), low density lipoprotein (LDL), high density lipoprotein (HDL) and lipoprotein-free fractions by density gradient ultracentrifugation. Vitamin K1 was measured in the plasma and lipoprotein fractions using HPLC. The concentration of vitamin K1 in plasma reached a peak 2 h after an IM dose and remained high throughout the 30 h course of the study. In contrast, the oral dose of vitamin K1 peaked at 4 h and rapidly decreased to near baseline by 18 to 30 h. The distribution of vitamin K1 in the lipid fractions was different for IM compared to PO. The percentage of vitamin K1 in the VLDL fraction at the peak for an oral dose was significantly higher than for an IM dose (80.8% +/- 3.5 vs 10.8% +/- 6.5, p < 0.0001). After the oral absorption stage, the subjects took 5 mg of vitamin K1 orally, once a day, for 12 days. No significant differences were observed for the following coagulation proteins and hemostatic markers measured immediately before and after long-term oral vitamin K supplementation: factor II, factor VII, protein C, and thrombin-antithrombin III complex. In conclusion, physiological processing of supplemented vitamin K1 differs in the IM vs PO routes of administration and 12 days of oral vitamin K1 does not alter the concentration of selected vitamin K-dependent coagulation proteins or thrombin-antithrombin complex generation.

Published

1995

10. Plasma resistance to activated protein C in venous and arterial thrombosis.

Author

Cushman M, Bhushan F, Bovill E, and Tracy R

Subjects

Adult, Arteries, Disease Susceptibility, Factor V Deficiency complications, Factor V Deficiency epidemiology, Factor V Deficiency genetics, Humans, Prevalence, Thromboembolism epidemiology, Thromboembolism etiology, Thrombophlebitis blood, Blood Coagulation Tests, Factor V Deficiency blood, Protein C pharmacology, Thromboembolism blood

Published

1994

11. Factor VII antigen levels in a healthy blood donor population.

Author

Howard PR, Bovill EG, Pike J, Church WR, and Tracy RP

Subjects

Adolescent, Adult, Age Distribution, Aged, Female, Humans, Immunoenzyme Techniques, Lipids blood, Male, Middle Aged, Reference Values, Reproducibility of Results, Sex Distribution, Antigens blood, Blood Donors, Factor VII immunology

Abstract

We determined factor VII antigen (FVIIag) levels in 705 healthy blood donors ranging in age from 17 to 79 years using a two-site solid-phase enzyme immunoassay developed in our laboratory. The mean (+/- SD) FVIIag level for the total population was 102 +/- 31%. FVIIag levels for men (n = 375) and women (n = 330) were 101 +/- 28% and 103 +/- 33%, respectively. A significant increase in FVIIag was observed with age in both men (r = 0.25, p < 0.0001) and women (r = 0.35, p < 0.0001). FVIIag levels were significantly higher in women > 60 years when compared to men (median women: 125%; median men: 111%; p < 0.05). On a subset of the study group (n = 45), FVIIag levels were correlated to total cholesterol (r = 0.27, p = 0.08) and triglyceride (r = 0.41, p < 0.01). Assuming the commonly used reference interval of 60-140% for FVII, the frequencies of FVIIag values for < 60% and > 140% using our assay were 2.1% and 9.2%, respectively. Gender and age-related differences in FVIIag levels must be considered in a reference interval. We further suggest that assay-specific reference ranges be established, which may include values outside the commonly used values of 60-140%.

Published

1994

12. Pathologic fibrinolysis as a cause of clinical bleeding.

Author

Stump DC, Taylor FB Jr, Nesheim ME, Giles AR, Dzik WH, and Bovill EG

Subjects

Antifibrinolytic Agents therapeutic use, Blood Coagulation Tests, Disseminated Intravascular Coagulation blood, Endothelium, Vascular injuries, Fibrinolytic Agents adverse effects, Hemorrhage blood, Hemorrhagic Disorders drug therapy, Hemorrhagic Disorders genetics, Hemostasis, Humans, Leukemia blood, Liver Transplantation physiology, Plasminogen Activators physiology, Plasminogen Inactivators metabolism, Platelet Aggregation, alpha-2-Antiplasmin deficiency, Fibrinolysis physiology, Hemorrhage etiology

Published

1990