Your search keyword '"Coagulation Protein Disorders genetics"' showing total 74 results

1. Thrombin and plasmin generation in patients with plasminogen or plasminogen activator inhibitor type 1 deficiency.

Author

Saes JL, Schols SEM, Betbadal KF, van Geffen M, Verbeek-Knobbe K, Gupta S, Hardesty BM, Shapiro AD, and van Heerde WL

Subjects

Adult, Child, Coagulation Protein Disorders genetics, Female, Genotype, Hemorrhagic Disorders genetics, Humans, Male, Middle Aged, Phenotype, Plasminogen Activator Inhibitor 1 genetics, Plasminogen Activator Inhibitor 1 metabolism, Coagulation Protein Disorders metabolism, Fibrinolysin biosynthesis, Hemorrhagic Disorders metabolism, Plasminogen Activator Inhibitor 1 deficiency, Thrombin biosynthesis

Abstract

Introduction: Deficiencies of plasminogen and plasminogen activator inhibitor type 1 (PAI-1) are rare disorders of fibrinolysis. Current laboratory assays for analysis of activity of plasminogen and PAI-1 do not provide an accurate correlation with clinical phenotype., Methods: The Nijmegen Hemostasis Assay (NHA) was used to simultaneously measure thrombin and plasmin generation in 5 patients with plasminogen deficiency (PLGD) and 10 patients with complete PAI-1 deficiency. Parameters analysed included: lag time ratio, thrombin peak time ratio, thrombin peak height, thrombin potential (AUC), fibrin lysis time, plasmin peak height and plasmin potential. Parameters were expressed as a percentage compared to a reference value of 53 healthy normal controls., Results: Patients with PLGD demonstrated a short lag time and thrombin peak time, with normal thrombin peak height but an increased AUC. Plasmin generation was able to be detected in only one (23% plasminogen activity) of the five PLGD patients. All ten PAI-1 deficient patients demonstrated a short lag and thrombin peak time, low thrombin peak height with normal AUC. Plasmin generation revealed an increased plasmin peak and plasmin potential; interestingly, there was a large variation between individual patients despite all patients having the same homozygous defect., Conclusion: Patients with either PLGD or PAI-1 deficiency show distinct abnormalities in plasmin and thrombin generation in the NHA. The differences observed in the propagation phase of thrombin generation may be explained by plasmin generation. These results suggest that disorders of fibrinolysis also influence coagulation and a global assay measuring both activities may better correlate with clinical outcome., (© 2019 The Authors. Haemophilia published by John Wiley & Sons Ltd.)

Published

2019

2. Elevated thrombin generation in patients with congenital disorder of glycosylation and combined coagulation factor deficiencies.

Author

Pascreau T, de la Morena-Barrio ME, Lasne D, Serrano M, Bianchini E, Kossorotoff M, Boddaert N, Bruneel A, Seta N, Vicente V, de Lonlay P, Corral J, and Borgel D

Subjects

Adolescent, Blood Coagulation genetics, Blood Coagulation Disorders, Inherited diagnosis, Blood Coagulation Disorders, Inherited genetics, Child, Child, Preschool, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders genetics, Congenital Disorders of Glycosylation diagnosis, Congenital Disorders of Glycosylation genetics, Female, Genetic Predisposition to Disease, Humans, Male, Paris, Phenotype, Retrospective Studies, Spain, Blood Coagulation Disorders, Inherited blood, Coagulation Protein Disorders blood, Congenital Disorders of Glycosylation blood, Thrombin metabolism

Abstract

Background: Congenital disorders of glycosylation are rare inherited diseases affecting many different proteins. The lack of glycosylation notably affects the hemostatic system and leads to deficiencies of both procoagulant and anticoagulant factors., Objective: To assess the hemostatic balance in patients with multiple coagulation disorders by using a thrombin generation assay., Method: We performed conventional coagulation assays and a thrombin generation assay on samples from patients with congenital disorder of glycosylation. The thrombin generation assay was performed before and after activation of the protein C system by the addition of soluble thrombomodulin., Results: A total of 35 patients were included: 71% and 57% had low antithrombin and factor XI levels, respectively. Protein C and protein S levels were abnormally low in 29% and 26% of the patients, respectively, whereas only 11% displayed low factor IX levels. Under baseline conditions, the thrombin generation assay revealed a significantly higher endogenous thrombin potential and thrombin peak in patients, relative to controls. After spiking with thrombomodulin, we observed impaired involvement of the protein C system. Hence, 54% of patients displayed a hypercoagulant phenotype in vitro. All the patients with a history of stroke-like episodes or thrombosis displayed this hypercoagulant phenotype., Conclusion: A thrombin generation assay revealed a hypercoagulant in vitro phenotype under baseline condition; this was accentuated by impaired involvement of the protein C system. This procoagulant phenotype may thus reflect the risk of severe vascular complications. Further research will have to determine whether the thrombin generation assay is predictive of vascular events., (© 2019 French National Institute of Health and Medical Research. © 2019 International Society on Thrombosis and Haemostasis.)

Published

2019

3. Molecular Mechanisms and Determinants of Innovative Correction Approaches in Coagulation Factor Deficiencies.

Author

Balestra D and Branchini A

Subjects

Animals, Blood Coagulation Factors genetics, CRISPR-Cas Systems, DNA genetics, Gene Editing methods, Humans, RNA, Messenger genetics, Coagulation Protein Disorders genetics, Coagulation Protein Disorders therapy, Genetic Therapy methods

Abstract

Molecular strategies tailored to promote/correct the expression and/or processing of defective coagulation factors would represent innovative therapeutic approaches beyond standard substitutive therapy. Here, we focus on the molecular mechanisms and determinants underlying innovative approaches acting at DNA, mRNA and protein levels in inherited coagulation factor deficiencies, and in particular on: (i) gene editing approaches, which have permitted intervention at the DNA level through the specific recognition, cleavage, repair/correction or activation of target sequences, even in mutated gene contexts; (ii) the rescue of altered pre-mRNA processing through the engineering of key spliceosome components able to promote correct exon recognition and, in turn, the synthesis and secretion of functional factors, as well as the effects on the splicing of missense changes affecting exonic splicing elements; this section includes antisense oligonucleotide- or siRNA-mediated approaches to down-regulate target genes; (iii) the rescue of protein synthesis/function through the induction of ribosome readthrough targeting nonsense variants or the correction of folding defects caused by amino acid substitutions. Overall, these approaches have shown the ability to rescue the expression and/or function of potentially therapeutic levels of coagulation factors in different disease models, thus supporting further studies in the future aimed at evaluating the clinical translatability of these new strategies.

Published

2019

4. Replacement Therapy with Glu-Plasminogen for the Treatment of Severe Respiratory and Auditory Complications of Congenital Plasminogen Deficiency.

Author

Tenbrock K, Lehmann S, Schrading S, and Moran J

Subjects

Adolescent, Coagulation Protein Disorders genetics, Codon, Terminator, Hearing Disorders etiology, Hearing Disorders genetics, Humans, Male, Pneumonia, Bacterial etiology, Pneumonia, Bacterial genetics, Pseudomonas Infections etiology, Pseudomonas Infections genetics, Coagulation Protein Disorders drug therapy, Enzyme Replacement Therapy, Hearing Disorders drug therapy, Plasminogen therapeutic use, Pneumonia, Bacterial drug therapy, Pseudomonas Infections drug therapy

Published

2019

5. Rare bleeding disorders-old diseases in the era of novel options for therapy.

Author

Livnat T, Barg AA, Levy-Mendelovich S, and Kenet G

Subjects

Animals, Blood Coagulation, Blood Coagulation Factors therapeutic use, Coagulation Protein Disorders blood, Coagulation Protein Disorders genetics, Coagulation Protein Disorders therapy, Genetic Therapy methods, Hemorrhage blood, Hemorrhage genetics, Hemorrhage therapy, Humans, Rare Diseases blood, Rare Diseases genetics, Rare Diseases therapy, Coagulation Protein Disorders diagnosis, Hemorrhage diagnosis, Rare Diseases diagnosis

Abstract

Rare diseases are defined as life-threatening or chronically debilitating diseases with a prevalence of less than one per 2000 according to the European Union or one per 1250 according to the USA. Congenital rare bleeding disorders RBD are reported in most populations, with incidence varying from 1 in 5000 (Hemophilia A), 1:30,000 (Hemophilia B) to much rarer (1:500,000 for FVII deficiency, 1-3 million for Prothrombin or FXIII deficiency). Acquired Hemophilia A is also a rare bleeding disorder with estimated frequency of 1 in million. Most RBDs are inherited as autosomal recessive (AR); however, heterozygous carriers with varying degrees of corresponding factor deficiency may render an unpredictable propensity for bleeding. In patients with bleeding symptoms, laboratory assessment and especially molecular techniques currently enable accurate diagnosis and may provide tools for prenatal and family counseling. Currently hemostasis control is mainly based upon replacement of the missing coagulation factors (unless presence of inhibitors renders it impossible), however future gene therapy and disruptive, non-replacement alternatives may be promising for patients with RBD., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

6. New clotting disorders that cast new light on blood coagulation and may play a role in clinical practice.

Author

Girolami A, Cosi E, Ferrari S, Lombardi AM, and Girolami B

Subjects

Humans, Blood Coagulation Factors genetics, Blood Coagulation Factors metabolism, Coagulation Protein Disorders blood, Coagulation Protein Disorders classification, Coagulation Protein Disorders genetics, Coagulation Protein Disorders therapy

Abstract

Recently several variants of clotting factors have shown a peculiar behavior so that they appear as new defects. The factors involved are FII, FV and FIX. Prothrombin deficiency is usually associated with bleeding. Recently a few prothrombin abnormalities involving Arg396 mutations, have been demonstrated to show antithrombin resistance with the consequent appearance of a thrombophilic state and venous thromboses in young age. The same is true for an abnormal FIX (FIX Padua). The thrombotic manifestations in the latter condition are also venous. The abnormal FIX (FIX Padua) is characterized by a great increase in FIX activity whereas FIX antigen is only slightly increased. The condition is due to an Arg338Lys mutation. The increased intrinsic clotting activity of this abnormal FIX is being investigated as a useful therapeutic approach in homophile B patients. Another new clotting disorder is represented by two abnormal FV (FV East Texas and FV Amsterdam). These are characterized by a deletion of part of the B domain of FV resulting in a "short" FV. The condition is characterized by a mild bleeding tendency due to high levels of Tissue Factor pathway inhibitor. The "short" factor V is in fact resistant to the action of Tissue Factor pathway inhibitor which is sharply increased in these patients. These new clotting entities have again demonstrated that the study of patients who show a tendency to venous thrombosis or a mild bleeding condition that cannot be explained on the basis of our current concepts of blood coagulation, may represent "new" coagulation disorders. All persons interested in thrombotic or hemorrhagic disorders should be informed about these new clinical and laboratory conditions.

Published

2017

7. Autosomal recessive inherited bleeding disorders in Pakistan: a cross-sectional study from selected regions.

Author

Naz A, Jamal MY, Amanat S, Din Ujjan I, Najmuddin A, Patel H, Raziq F, Ahmed N, Imran A, and Shamsi TS

Subjects

Adolescent, Child, Consanguinity, Cross-Sectional Studies, Female, Humans, Male, Pakistan epidemiology, Coagulation Protein Disorders epidemiology, Coagulation Protein Disorders genetics, Genes, Recessive

Abstract

Background: Autosomal recessive bleeding disorders (ARBDs) include deficiencies of clotting factors I, II, V, VII, X, XI, XIII, vitamin K dependent clotting factors, combined factor V & VIII, Von Willebrand Disease (vWD) type 3, Glanzmann's thrombasthenia (GT) and Bernard-Soulier syndrome. Patients with primary bleeding disorders from all the major provincial capitals of Pakistan were screened for ARBDs. Prothrombin (PT), activated partial thromboplastin time (APTT), bleeding time (BT) and fibrinogen levels were measured. Cases with isolated prolonged APTT were tested for factors VIII and IX using factor assays This was followed by FXI:C level assessment in cases with normal FVIII and FIX levels. vWD was screened in patients with low FVIII levels. Factors II, V and X were tested in patients with simultaneous prolongation of PT and APTT. Peripheral blood film examination and platelet aggregation studies were performed to assess platelet disorders. Urea clot solubility testing was done to detect Factor XIII levels where platelet function tests were normal. Descriptive analysis was done using SPSS version 16., Results: Of the 429 suspected bleeding disorder patients, 148 (35%) were diagnosed with hemophilia A and 211 (49.1%) patients had ARBDs. 70 patients (16.3%) remained undiagnosed. Out of 211 patients with ARBD; 95 (33.8%) had vWD type 3. Fibrinogen deficiency was found in 34 patients (12%), GT in 27 (9.6%), factor XIII deficiency in 13 (4.6%), factor VII deficiency in 12 (4.3%), factor V deficiency in 9 (3.2%). Eight patients (2.8%) had vitamin K-dependent clotting factor deficiency, Bernard-Soulier syndrome was diagnosed in seven patients (2.5%), factor X deficiency in 2 (0.7%), factor II deficiency in 2 (0.7%), factor XI deficiency and combined factor V and VIII deficiency in 1 (0.4%) patient each., Conclusion: vWD type 3 was the most common ARBD found in our sample of patients in Pakistan, followed by fibrinogen deficiency and GT in respective order.

Published

2017

8. [Pseudoxanthoma elasticum-like disease with deficiency of vitamin K-dependent clotting factors and cutis laxa features].

Author

Gusdorf L, Mitcov M, Maradeix S, Cunat S, Martin L, and Cribier B

Subjects

Biopsy, Carbon-Carbon Ligases genetics, Coagulation Protein Disorders genetics, Coagulation Protein Disorders pathology, Cutis Laxa genetics, Cutis Laxa pathology, Female, Heterozygote, Humans, Mutation, Missense, Protein Processing, Post-Translational, Pseudoxanthoma Elasticum genetics, Pseudoxanthoma Elasticum pathology, Skin pathology, Weight Loss, Young Adult, Carbon-Carbon Ligases deficiency, Coagulation Protein Disorders diagnosis, Cutis Laxa diagnosis, Pseudoxanthoma Elasticum diagnosis

Abstract

Background: Pseudoxanthoma elasticum (PXE)-like syndrome is characterized by the association of PXE and cutis laxa (CL) features with a deficiency of vitamin K-dependent clotting factors. It was first described in 1971 and was identified as a distinct genetic entity in 2007 with analysis of the GGCX (γ-glutamyl carboxylase) gene, which is involved in congenital deficiency in vitamin K-dependent clotting factors. Here we report a new case of this extremely rare syndrome., Patients and Methods: A 23-year-old female patient was seen for the emergence of loose and redundant skin following extensive weight loss. She also presented a deficiency of vitamin K-dependent clotting factors. Physical examination revealed excessive, leathery skin folds in the axillary and neck regions. A skin biopsy revealed polymorphous and fragmented elastic fibers in the reticular dermis. These were mineralized, as was demonstrated by Von Kossa staining. The clinical features of CL associated with the histopathological features of PXE and vitamin K-dependent clotting factor deficiency led us to a diagnosis of PXE-like syndrome. A molecular study of the GGCX gene showed compound heterozygosity., Discussion: The GGCX gene is usually responsible for PXE-like syndrome. GGCX encodes a γ-glutamyl carboxylase necessary for activation of gla-proteins. Gla-proteins are involved both in coagulation factors in the liver and in the prevention of ectopic mineralization of soft tissues. Uncarboxylated forms of gla-proteins in fibroblast would thus enable mineralization and fragmentation of elastic fibers., (Copyright © 2016 Elsevier Masson SAS. All rights reserved.)

Published

2016

9. Guideline for the diagnosis and management of the rare coagulation disorders: a United Kingdom Haemophilia Centre Doctors' Organization guideline on behalf of the British Committee for Standards in Haematology.

Author

Mumford AD, Ackroyd S, Alikhan R, Bowles L, Chowdary P, Grainger J, Mainwaring J, Mathias M, and O'Connell N

Subjects

Adult, Child, Female, Humans, Male, Pregnancy, Afibrinogenemia diagnosis, Afibrinogenemia epidemiology, Afibrinogenemia genetics, Afibrinogenemia therapy, Blood Coagulation Factors administration & dosage, Blood Coagulation Factors genetics, Blood Coagulation Factors therapeutic use, Blood Coagulation Tests, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders epidemiology, Coagulation Protein Disorders genetics, Coagulation Protein Disorders therapy, Disease Management, Fibrinogen genetics, Fibrinogen therapeutic use, Hemorrhage prevention & control, Pregnancy Complications, Hematologic therapy, Recombinant Proteins therapeutic use, Hemorrhagic Disorders diagnosis, Hemorrhagic Disorders epidemiology, Hemorrhagic Disorders genetics, Hemorrhagic Disorders therapy

Published

2014

10. Dusart Syndrome in a Scandinavian family characterized by arterial and venous thrombosis at young age.

Author

Ramanathan R, Gram J, Feddersen S, Nybo M, Larsen A, and Sidelmann JJ

Subjects

Adolescent, Adult, Case-Control Studies, Child, Coagulation Protein Disorders blood, Coagulation Protein Disorders genetics, DNA Mutational Analysis, Female, Fibrin chemistry, Fibrinogens, Abnormal genetics, Fibrinogens, Abnormal metabolism, Humans, Male, Middle Aged, Pedigree, Protein Multimerization, Scandinavian and Nordic Countries, Syndrome, Thrombin Time, Thrombosis genetics, Young Adult, gamma-Glutamyltransferase blood, Coagulation Protein Disorders congenital, Thrombosis blood

Abstract

Background: Dysfibrinogenemia is a rare group of qualitative fibrinogen disorders caused by structural abnormalities in the fibrinogen molecule. The laboratory diagnosis of dysfibrinogenemia is controversial. Fibrinogen Paris V, clinically termed Dusart Syndrome, is a dysfibrinogenemia caused by a single base substitution in the gene coding for the Aα-chain of the fibrinogen molecule., Objectives: To diagnose the first Scandinavian family with Fibrinogen Paris V affecting several family members; the proband, a seven-year-old boy with cerebral vein thrombosis., Methods: The diagnosis was established following the ISTH guideline for laboratory testing supplemented with fibrin structure analysis and fibrinogen gene analysis., Results: Prolonged thrombin time and reduced ratio between the functional and the protein concentration of fibrinogen were observed in four family members who also were characterized by significantly reduced fibrin polymerization (p < 0.001), reduced fibrin fibre diameter (p < 0.001), reduced fibrin mass-length ratio (p < 0.001) and significantly reduced t-PA-induced fibrinolysis of the fibrin clots (p < 0.001) when compared to controls. Fibrinogen gene analysis demonstrated that five of the family members carried the Fibrinogen Paris V mutation. All laboratory tests were normal in the family members carrying the wild type of the fibrinogen gene. Four of the affected patients had suffered from thrombotic episodes. A noticeable feature in the present family was the presence of both venous and arterial thrombosis., Conclusions: Excellent concordance was observed between the screening and confirmatory tests, fibrin structure analysis and fibrinogen gene analysis. Fibrin structure analysis should be considered in the laboratory algorithm for diagnosis of dysfibrinogenemia.

Published

2013

11. Atypical hemolytic-uremic syndrome: the interplay between complements and the coagulation system.

Author

Nayer A and Asif A

Subjects

Atypical Hemolytic Uremic Syndrome, Coagulation Protein Disorders genetics, Coagulation Protein Disorders metabolism, Complement System Proteins genetics, Hemolytic-Uremic Syndrome complications, Hemolytic-Uremic Syndrome therapy, Humans, Kidney Failure, Chronic etiology, Prognosis, Coagulation Protein Disorders physiopathology, Complement System Proteins metabolism, Hemolytic-Uremic Syndrome pathology, Hemolytic-Uremic Syndrome physiopathology

Abstract

Hemolytic-uremic syndrome (HUS) is a rare life-threatening disorder characterized by microangiopathic hemolytic anemia, thrombocytopenia, and impaired renal function. A thrombotic microangiopathy underlies the clinical features of HUS. In the majority of cases, HUS follows an infection with toxin-producing bacteria such as verotoxin-producing Escherichia coli. In some cases, HUS is not preceded by a clinically apparent infection, and therefore, is named atypical HUS. The prognosis of atypical HUS is poor. While mortality approaches 25% during the acute phase, end-stage renal disease develops in nearly half of patients within a year. Evidence is accumulating that complement activation through the alternative pathway is at the heart of the pathophysiology leading to atypical HUS. Genetic abnormalities involving complement regulatory proteins and complement components form the molecular basis for complement activation. Since microvascular thrombosis is a quintessential feature of atypical HUS, complements and the coagulation system must work in tandem to give rise to the pathologic alterations observed in this condition. Here, a brief discussion of clinical and morphologic features of atypical HUS is followed by a concise presentation of the complement and coagulation systems. The interplay between complements and the coagulation system is graphically highlighted. Last but not least, conventional and emerging therapies for atypical HUS are outlined.

Published

2013

12. Molecular testing for disorders of hemostasis.

Author

Lillicrap D

Subjects

Blood Coagulation Factors genetics, Coagulation Protein Disorders blood, Coagulation Protein Disorders diagnosis, Genetic Predisposition to Disease genetics, Genetic Testing trends, Genome-Wide Association Study methods, Humans, Molecular Diagnostic Techniques trends, Reproducibility of Results, Sensitivity and Specificity, Coagulation Protein Disorders genetics, Genetic Testing methods, Hemostasis genetics, Molecular Diagnostic Techniques methods

Abstract

The investigation of inherited bleeding disorders with routine tests of hemostasis will yield clear diagnostic information in the majority of subjects with an unequivocal history of bleeding and especially in those where the phenotypic severity is severe and where an obvious family history of bleeding is present. Nevertheless, a significant minority of subjects with obvious bleeding symptoms will remain without a definite diagnosis after extensive hemostatic testing. With these facts in mind, the role of molecular testing for inherited disorders of hemostasis now includes the following: confirmation of a phenotypic diagnosis through targeted genetic analysis, the distinction of bleeding phenocopies by molecular analysis, and provision of genetic testing as the investigation of choice in situations such as prenatal diagnosis and detection of the carrier state for inherited bleeding traits. In addition, molecular testing can sometimes be used to provide supplementary knowledge that can be used to enhance clinical care. Finally, the utility of genome-wide approaches to identify novel genetic associations may provide new information to explain the cause of bleeding in the population of bleeders without established diagnoses., (© 2013 Blackwell Publishing Ltd.)

Published

2013

13. [Rare bleeding disorders and invasive procedures].

Author

Bonhomme F, Schved JF, Giansily-Blaizot M, Samama CM, and de Moerloose P

Subjects

Blood Coagulation Disorders, Inherited drug therapy, Blood Coagulation Disorders, Inherited epidemiology, Blood Coagulation Factors adverse effects, Blood Coagulation Factors analysis, Blood Coagulation Factors genetics, Blood Coagulation Factors therapeutic use, Coagulation Protein Disorders drug therapy, Coagulation Protein Disorders epidemiology, Disease Management, Emergencies, Female, Genes, Recessive, Hemorrhage prevention & control, Humans, Male, Postoperative Hemorrhage etiology, Postoperative Hemorrhage prevention & control, Postpartum Hemorrhage etiology, Postpartum Hemorrhage prevention & control, Pregnancy, Prevalence, Risk Assessment, Symptom Assessment, Thrombosis chemically induced, Blood Coagulation Disorders, Inherited genetics, Coagulation Protein Disorders genetics, Hemorrhage etiology

Abstract

Rare inherited bleeding disorders include fibrinogen disorders, and deficiencies of factors II (prothrombin), V, VII, X, XI, XIII, and combined V+VIII, and combined vitamin K-dependent factors, with general population prevalence rates between 1/500,000 and 1/2,000,000. These inherited disorders, transmitted as autosomal recessive traits, are characterized by a heterogeneous clinical presentation (asymptomatic, mild, moderate or severe bleeding tendency); this variability is more important for deficiencies with factor levels ranging from 5 to 50%. Individual bleeding risk assessment before an invasive procedure or during peri-partum period remains difficult, although an essential step to decide whether a substitution with clotting factor is necessary or not. Because there is a poor correlation between factor activity levels and the severity of bleeding symptoms, factor correction before an invasive procedure should not be based on factor level only, but physicians must also take into account the patient phenotype as well as the haemorrhagic risk of the procedure., (Copyright © 2013 Société française d’anesthésie et de réanimation (Sfar). Published by Elsevier SAS. All rights reserved.)

Published

2013

14. DPM2-CDG: a muscular dystrophy-dystroglycanopathy syndrome with severe epilepsy.

Author

Barone R, Aiello C, Race V, Morava E, Foulquier F, Riemersma M, Passarelli C, Concolino D, Carella M, Santorelli F, Vleugels W, Mercuri E, Garozzo D, Sturiale L, Messina S, Jaeken J, Fiumara A, Wevers RA, Bertini E, Matthijs G, and Lefeber DJ

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, Coagulation Protein Disorders genetics, Congenital Disorders of Glycosylation complications, DNA Mutational Analysis, Drug Resistance, Dystroglycans metabolism, Electromyography, Endoplasmic Reticulum, Epilepsy etiology, Female, Fibroblasts metabolism, Glycosylation, Humans, Infant, Isoelectric Focusing, Liver Diseases complications, Liver Diseases genetics, Male, Mannose metabolism, Microcephaly genetics, Microcephaly pathology, Middle Aged, Molecular Sequence Data, Muscular Dystrophies complications, Mutation genetics, Mutation physiology, Mutation, Missense genetics, Mutation, Missense physiology, Pregnancy, Vision Disorders genetics, Vision Disorders pathology, Young Adult, Congenital Disorders of Glycosylation genetics, Epilepsy genetics, Mannosyltransferases genetics, Muscular Dystrophies genetics

Abstract

Objective: Congenital disorders of glycosylation (CDG) are a group of metabolic diseases due to defects in protein and lipid glycosylation. We searched for the primary defect in 3 children from 2 families with a severe neurological phenotype, including profound developmental delay, intractable epilepsy, progressive microcephaly, severe hypotonia with elevated blood creatine kinase levels, and early fatal outcome. There was clinical evidence of a muscular dystrophy-dystroglycanopathy syndrome, supported by deficient O-mannosylation by muscle immunohistochemistry., Methods: Biochemical and molecular methods were combined to pinpoint the defect in the glycosylation pathway in the endoplasmic reticulum., Results: Metabolic investigations revealed CDG-I, pointing to a defect in protein N-glycosylation in the endoplasmic reticulum. Analysis of lipid-linked oligosaccharides in fibroblasts showed accumulation of Dol-PP-GlcNAc(2) -Man(5) . DNA analysis revealed mutations in DPM2, 1 of the subunits of the dolichol-phosphate-mannose (DPM) synthase; the patient in the first family is compound heterozygous for 2 mutations (c.68A>G, predicting a missense mutation p.Y23C and c.4-1G>C, a splice mutation), whereas the patients in the second family are homozygous for the same missense mutation (c.68A>G, p.Y23C)., Interpretation: We describe a new CDG, due to a deficiency of DPM2. Hence, mutations have now been described in the genes for the 3 subunits of DPM: DPM1, DPM2, and DPM3, whereby DPM2-CDG links the congenital disorders of glycosylation to the congenital muscular dystrophies., (Copyright © 2012 American Neurological Association.)

Published

2012

15. Rare factor deficiencies.

Author

Hsieh L and Nugent D

Subjects

Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders genetics, Humans, Rare Diseases diagnosis, Rare Diseases genetics, Blood Coagulation Factors therapeutic use, Coagulation Protein Disorders therapy, Rare Diseases therapy

Abstract

Purpose of Review: By definition, rare factor deficiencies have a prevalence of less than 200,000 in the US population, or an incidence of less than one in 2000 in Europe. The very small numbers of patients with rare disorders present challenges in diagnosis, evaluation of bleeding risk and treatment. Use of new assays, full genome sequencing, and global clotting assays will significantly improve diagnosis of patients with rare bleeding disorders., Recent Findings: In addition to new assays available for monitoring patients, new therapy, both recombinant and plasma derived, is now available. Registries and clinical trials have demonstrated decreased bleeding and improved outcomes when patients are treated with these agents. Expanding international registries have been initiated to correlate genotype and bleeding phenotype in conjunction with global assays., Summary: Ongoing research continues to expand our understanding of the pathophysiology of rare factor deficiencies. This work complements medical practice to incorporate early diagnosis and new treatment options for patients, resulting in safer and less sensitizing regimens and much improved clinical outcomes.

Published

2012

16. Inherited disorders of blood coagulation.

Author

Lippi G, Franchini M, Montagnana M, and Favaloro EJ

Subjects

Blood Coagulation physiology, Coagulation Protein Disorders genetics, Hemophilia A genetics, Hemophilia B genetics, Humans, von Willebrand Diseases genetics, Blood Coagulation Disorders genetics

Abstract

Hemostasis is traditionally defined as a physiological response to blood vessel injury and bleeding, which entails a co-ordinated process involving the blood vessel, platelets, and blood clotting proteins (i.e. coagulation factors). Hemostasis can be divided into primary and secondary components. The former rapidly initiates after endothelial damage and is characterized by vascular contraction, platelet adhesion, and formation of a soft aggregate plug. The latter is initiated following the release of tissue factor and involves a complex sequence of events known as the blood coagulation cascade, encompassing serial steps where each coagulation factor activates another in a chain reaction that culminates in the conversion of fibrinogen to fibrin. Patients carrying abnormalities of the coagulation cascade (i.e. deficiencies of coagulation factors) have an increased bleeding tendency, where the clinical severity is mostly dependent upon the type and the plasma level of the factor affected. These disorders also impose a heavy medical and economic burden on individual patients and society in general. The aim of this article is to provide a general overview on the pathophysiology, clinics, diagnostics, and therapy of inherited disorders of coagulation factors.

Published

2012

17. Novel phenotype and γ-glutamyl carboxylase mutations in combined deficiency of vitamin K-dependent coagulation factors.

Author

Lunghi B, Redaelli R, Caimi TM, Corno AR, Bernardi F, and Marchetti G

Subjects

Adolescent, DNA Mutational Analysis, Humans, Male, Phenotype, Vitamin K metabolism, Carbon-Carbon Ligases genetics, Coagulation Protein Disorders genetics, Mutation genetics, Vitamin K Deficiency genetics

Published

2011

18. [Molecular diagnostics and pathogenesis of hereditary blood coagulation factor deficiency].

Author

Suzuki K and Suwabe A

Subjects

Coagulation Protein Disorders blood, Coagulation Protein Disorders physiopathology, Humans, Molecular Diagnostic Techniques, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders genetics, Pathology, Molecular

Published

2010

19. Factor VIIa-antithrombin complexes in patients with arterial and venous thrombosis.

Author

Spiezia L, Rossetto V, Campello E, Gavasso S, Woodhams B, Tormene D, and Simioni P

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Antithrombins genetics, Coagulation Protein Disorders blood, Coagulation Protein Disorders genetics, Factor V metabolism, Factor VIIa genetics, Female, Humans, Male, Middle Aged, Protein Binding, Venous Thrombosis blood, Venous Thrombosis genetics, Antithrombins metabolism, Coagulation Protein Disorders metabolism, Factor VIIa metabolism, Multiprotein Complexes metabolism, Venous Thrombosis metabolism

Abstract

Antithrombin (AT), in the presence of heparin, is able to inhibit the catalytic activity of factor VIIa bound to tissue factor (TF) on cell surfaces. The clinical meaning of FVIIa-AT complexes plasma levels is unknown. It was the objective of this study to evaluate FVIIa-AT complexes in subjects with thrombosis. Factor VIIa-AT complexes plasma levels in 154 patients consecutively referred to our Department with arterial or venous thrombosis and in a group of 154 healthy subjects, were measured. Moreover, FVIIa-AT complexes were determined in: i) n = 53 subjects belonging to 10 families with inherited factor VII deficiency; ii) n = 58 subjects belonging to seven families with AT deficiency; iii) n = 49 patients undergoing oral anticoagulant therapy (OAT). Factor VIIa-AT levels were determined by a specific ELISA kit (R&D, Diagnostica Stago, Gennevilliers, France). Factor VIIa-AT complexes mean plasma levels were lower in patients with either acute arterial (136 +/- 40 pM) or venous (142 +/- 53 pM) thrombosis than subjects with previous thrombosis (arterial 164 +/- 33 pM and venous 172 +/- 61 pM, respectively) and than healthy controls (156 +/- 63 pM). Differences between acute and previous thrombosis, were statistically significant (p < 0.05). Subjects with inherited and acquired (under OAT) factor VII deficiency had statistically significant lower FVIIa-AT complexes plasma levels (80 +/- 23 pM and 55 +/- 22 pM, respectively) than controls (150 +/- 51 pM, p < 0.0001 and 156 +/- 63 pM, p < 0.00001, respectively). Factor VIIa-AT complexes are positively correlated with plasma factor VII/VIIa levels. Further investigations are needed to verify the possible role of higher FVIIa-AT complex plasma levels in predicting hypercoagulable states and thrombosis.

Published

2010

20. PML/RARalpha fusion protein transactivates the tissue factor promoter through a GAGC-containing element without direct DNA association.

Author

Yan J, Wang K, Dong L, Liu H, Chen W, Xi W, Ding Q, Kieffer N, Caen JP, Chen S, Chen Z, and Xi X

Subjects

Base Sequence, Cell Line, Tumor, Coagulation Protein Disorders etiology, DNA metabolism, Humans, Promoter Regions, Genetic, Transcription Factor AP-1 metabolism, Coagulation Protein Disorders genetics, Gene Expression Regulation, Leukemic, Leukemia, Promyelocytic, Acute complications, Oncogene Proteins, Fusion pharmacology, Thromboplastin genetics, Transcriptional Activation

Abstract

A severe coagulopathy is a life-threatening complication of acute promyelocytic leukemia (APL) and is ascribable mainly to the excessive levels of tissue factor (TF) in APL cells regulated in response to the promyelocytic leukemia/retinoic acid receptor alpha (PML/RARalpha) fusion protein. The underlying molecular mechanisms for this regulation remain ill-defined. With U937-PR9 cell lines stably expressing luciferase reporter gene under the control of different mutants of the TF promoter, both luciferase and ChIP data allowed the localization of the PML/RARalpha-responsive sequence in a previously undefined region of the TF promoter at position -230 to -242 devoid of known mammalian transcription factor binding sites. Within this sequence a GAGC motif (-235 to -238) was shown to be crucial because deletion or mutation of these nucleotides impaired both PML/RARalpha interaction and promoter transactivation. However, EMSA results showed that PML/RARalpha did not bind to DNA probes encompassing the -230 to -242 sequences, precluding a direct DNA association. Mutational experiments further suggest that the activator protein 1 (AP-1) sites of the TF promoter are dispensable for PML/RARalpha regulation. This study shows that PML/RARalpha transactivates the TF promoter through an indirect interaction with an element composed of a GAGC motif and the flanking nucleotides, independent of AP-1 binding.

Published

2010

21. Genes influencing coagulation and the risk of aneurysmal subarachnoid hemorrhage, and subsequent complications of secondary cerebral ischemia and rebleeding.

Author

Ruigrok YM, Slooter AJ, Rinkel GJ, Wijmenga C, and Rosendaal FR

Subjects

Adult, Aged, Amino Acid Sequence, Amino Acid Substitution genetics, Blood Proteins genetics, Brain Ischemia physiopathology, Coagulation Protein Disorders metabolism, Coagulation Protein Disorders physiopathology, DNA Mutational Analysis, Factor XIII genetics, Female, Gene Frequency genetics, Genetic Markers genetics, Genetic Testing, Genetic Variation genetics, Genotype, Humans, Male, Middle Aged, Polymorphism, Genetic genetics, Risk Factors, Secondary Prevention, Subarachnoid Hemorrhage physiopathology, Brain Ischemia genetics, Coagulation Protein Disorders genetics, Gene Expression genetics, Genetic Predisposition to Disease genetics, Subarachnoid Hemorrhage complications, Subarachnoid Hemorrhage genetics

Abstract

Background: We investigated whether genes influencing coagulation are associated with the occurrence of aneurysmal subarachnoid hemorrhage (SAH) and with secondary cerebral ischemia and rebleeding in patients with aneurysmal SAH., Method: Genotyping for factor V Leiden (G1691A), prothrombin G20210A, methylenetetetrahydrofolate reductase (MTHFR) C677T, factor XIII subunit A Val34Leu, Tyr204Phe and Pro564Leu, and factor XIII subunit B His95Arg was performed in 208 patients with aneurysmal SAH and in 925 controls. Secondary cerebral ischemia occurred in 49 (24%) patients and rebleeding in 28 (14%) during their clinical course of 3 months after the aneurysmal SAH. The risk of aneurysmal SAH was assessed as odds ratio (OR) with 95% confidence interval (95% CI). The risk of secondary cerebral ischemia and rebleeding was assessed as hazard ratio (HR) with 95% CI using Cox regression., Findings: Carriers of the subunit B His95Arg factor XIII polymorphism had an increased risk of aneurysmal SAH with 23% of the patients homozygous or heterozygous for the variant allele compared to 17% of control subjects (OR 1.5, 95% CI 1.0-2.2). For the remaining genetic variants no effect on the risk of aneurysmal SAH could be demonstrated. A clear relation with the risk of secondary cerebral ischemia and of rebleeding could not be established for any of the genetic variants., Conclusions: We found that aneurysmal SAH patients are more often carriers of the subunit B His95Arg factor XIII polymorphism compared to controls. This suggests that carriers of the subunit B His95Arg factor XIII polymorphism have an increased risk of aneurysmal SAH. Larger studies should confirm our results. As aneurysmal SAH patients who died soon after admission could not be included in the present study, our results only apply to a population of patients who survived the initial hours after the hemorrhage. For the other studied genetic factors involved in coagulation, no association with the occurrence of aneurysmal SAH or with the occurrence of secondary cerebral ischemia or rebleeding after aneurysmal SAH could be demonstrated.

Published

2010

22. Two cases of congenital dysfibrinogenemia associated with thrombosis - Fibrinogen Praha III and Fibrinogen Plzen.

Author

Kotlín R, Reicheltová Z, Malý M, Suttnar J, Sobotková A, Salaj P, Hirmerová J, Riedel T, and Dyr JE

Subjects

Adult, Blood Coagulation, Coagulation Protein Disorders complications, Coagulation Protein Disorders genetics, Female, Fibrin chemistry, Fibrinogen genetics, Humans, Male, Microscopy, Electron, Scanning, Middle Aged, Mutation, Platelet Aggregation, Pulmonary Embolism genetics, Thrombosis complications, Thrombosis genetics, Coagulation Protein Disorders congenital, Coagulation Protein Disorders diagnosis, Fibrinogens, Abnormal genetics, Thrombosis diagnosis

Abstract

Congenital dysfibrinogenemia is a rare disease characterised by inherited abnormality in the fibrinogen molecule, resulting in functional defects. Two patients, a 26-year-old woman and a 61-year-old man, both with history of thrombotic events, had abnormal coagulation test results. DNA sequencing showed the heterozygous gamma Y363N mutation (Fibrinogen Praha III) and the heterozygous Aalpha N106D mutation (Fibrinogen Plzen), respectively. Fibrin polymerisation, after addition of either thrombin or reptilase, showed remarkably delayed polymerisation in both cases. Fibrinolysis experiments showed slower tPA initiated lysis of clots. SDS-PAGE did not show any difference between normal and Praha III and Plzen fibrinogens. Both mutations had a significant effect on platelet aggregation. In the presence of either ADP or TRAP, both mutations caused the decrease of platelet aggregation. SEM revealed abnormal clot morphology, with a large number of free ends and narrower fibres of both fibrin Praha III and Plzen. Praha III mutation was situated in the polymerisation pocket "a". The replacement of the bulky aromatic side chain of tyrosine by the polar uncharged small side chain of asparagine may lead to a conformational change, possibly altering the conformation of the polymerisation pocket. The Plzen mutation is situated in the coiled-coil connector and this replacement of polar uncharged asparagine residue by polar acidic aspartate changes the alpha-helical conformation of the coiled-coil connector; and may destabilise hydrogen bonds in its neighborhood. Although both mutations are situated in different regions of the molecule, both mutations have a very similar effect on fibrinogen functions and both are connected with thromboses.

Published

2009

23. Why dysfibrinogenaemias still matter.

Author

Weisel JW

Subjects

Blood Platelets metabolism, Crystallography, X-Ray, Dimerization, Fibrin chemistry, Fibrinogen chemistry, Fibrinogen genetics, Fibrinogens, Abnormal chemistry, Fibrinogens, Abnormal genetics, Heterozygote, Humans, Models, Genetic, Mutation, Phosphorylation, Platelet Aggregation, Platelet Glycoprotein GPIIb-IIIa Complex metabolism, Protein Binding, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders genetics

Published

2009

24. Superficial venous thrombosis: role of inherited deficiency of natural anticoagulants in extension to deep veins.

Author

Milio G, Siragusa S, Malato A, Grimaudo S, and Pinto A

Subjects

Adult, Antithrombin III Deficiency epidemiology, Chi-Square Distribution, Coagulation Protein Disorders genetics, Disease Progression, Female, Humans, Italy epidemiology, Male, Middle Aged, Prevalence, Prospective Studies, Protein C Deficiency epidemiology, Protein S Deficiency epidemiology, Risk Assessment, Risk Factors, Ultrasonography, Doppler, Duplex, Varicose Veins diagnostic imaging, Venous Thrombosis diagnostic imaging, Young Adult, Coagulation Protein Disorders epidemiology, Varicose Veins epidemiology, Venous Thrombosis epidemiology

Abstract

Aim: Superficial venous thrombosis (SVT) has been considered for a long time a limited clinical condition of low importance, but this approach has changed in recent years, when several studies demonstrated that extension to deep veins occurs in 7.3 to 44% of patients, with high prevalence of pulmonary embolism. The aim of this study was to evaluate the prevalence of inherited deficiency of natural coagulation inhibitors in patients suffering from SVT in both normal and varicose veins, and to understand their role in extension to deep veins., Methods: The study included 83 patients with SVT, without clinically obvious risk factors. Ultrasound examination was performed, and deficiencies of Protein C, Protein S and Antithrombin (AT) were investigated., Results: In the patients where SVT occurred in normal veins, coagulation inhibitor deficiencies were 6.45% in the absence of extension and 62.5% in patients with extension to deep veins. In the patients with varicose vein SVT, the presence of these factors was less evident, but their prevalence was considerably higher in those with extension to deep veins (36.3%) than in non-extension (6.06%)., Conclusions: Present data confirm the role of inherited thrombophilic states related to inhibitor deficiency, considering them as risk factors for SVT in normal veins. Furthermore, an association has been found between their presence and the progression of SVT to deep veins.

Published

2009

25. Novel splice site mutations in the gamma glutamyl carboxylase gene in a child with congenital combined deficiency of the vitamin K-dependent coagulation factors (VKCFD).

Author

Titapiwatanakun R, Rodriguez V, Middha S, Dukek BA, and Pruthi RK

Subjects

Blood Coagulation Factors genetics, Child, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders drug therapy, Diagnosis, Differential, Humans, Male, Mixed Function Oxygenases genetics, Munchausen Syndrome diagnosis, Polymorphism, Single Nucleotide, Vitamin K Deficiency diagnosis, Vitamin K Deficiency drug therapy, Vitamin K Epoxide Reductases, Carbon-Carbon Ligases deficiency, Carbon-Carbon Ligases genetics, Coagulation Protein Disorders congenital, Coagulation Protein Disorders genetics, Mutation, Vitamin K administration & dosage, Vitamin K Deficiency congenital

Abstract

Congenital combined deficiency of the vitamin K-dependent coagulation factors is a rare bleeding disorder caused by either a defect in the gamma-glutamyl carboxylase or the vitamin K epoxide reductase enzyme complex. The diagnosis should be considered when vitamin-K dependent factor activities are decreased and liver dysfunction, vitamin K deficiency, and factitious coumarin ingestion have been excluded. We report a case of VKCFD in a child resulting from compound heterozygosity for two novel splice site mutations of the gamma-glutamyl carboxylase gene. Oral vitamin K supplementation resulted in partial resolution of proteins and complete resolution of bleeding., (Copyright 2009 Wiley-Liss, Inc.)

Published

2009

26. Selective testing for thrombophilia in patients with first venous thrombosis: results from a retrospective family cohort study on absolute thrombotic risk for currently known thrombophilic defects in 2479 relatives.

Author

Lijfering WM, Brouwer JL, Veeger NJ, Bank I, Coppens M, Middeldorp S, Hamulyák K, Prins MH, Büller HR, and van der Meer J

Subjects

Adult, Blood Coagulation Factor Inhibitors genetics, Blood Coagulation Factors genetics, Coagulation Protein Disorders genetics, Cohort Studies, Family Health, Genetic Predisposition to Disease, Humans, Incidence, Netherlands epidemiology, Retrospective Studies, Risk, Thrombophilia epidemiology, Thrombophilia genetics, Venous Thrombosis blood, Thrombophilia diagnosis, Venous Thrombosis epidemiology, Venous Thrombosis etiology

Abstract

Thrombophilia screening is controversial. In a retrospective family cohort, where probands had thrombosis and a thrombophilic defect, 2479 relatives were tested for thrombophilia. In antithrombin-, protein C-, and protein S-deficient relatives, annual incidences of venous thrombosis were 1.77% (95% CI, 1.14-2.60), 1.52% (95% CI, 1.06-2.11), and 1.90% (95% CI, 1.32-2.64), respectively, at a median age of 29 years and a positive family history of more than 20% symptomatic relatives. In relatives with factor V (FV) Leiden, prothrombin 20210G>A, or high FVIII levels, these were 0.49% (95% CI, 0.39-0.60), 0.34% (95% CI, 0.22-0.49), and 0.49% (95% CI, 0.41-0.51), respectively. High FIX, FXI, and TAFI, and hyperhomocysteinemia were not independent risk factors. Annual incidence of major bleeding in antithrombin-, protein C-, or protein S-deficient relatives on anticoagulants was 0.29% (95% CI, 0.03-1.04). Cumulative recurrence rates in relatives with antithrombin, protein C, or protein S deficiency were 19% at 2 years, 40% at 5 years, and 55% at 10 years. In relatives with FV Leiden, prothrombin 20210G>A, or high levels FVIII, these were 7%, 11%, and 25%, respectively. Considering its clinical implications, thrombophilia testing should address hereditary deficiencies of antithrombin, protein C, and protein S in patients with first venous thrombosis at young age and/or a strong family history of venous thrombosis.

Published

2009

27. Co-existent pseudoxanthoma elasticum and vitamin K-dependent coagulation factor deficiency: compound heterozygosity for mutations in the GGCX gene.

Author

Li Q, Schurgers LJ, Smith AC, Tsokos M, Uitto J, and Cowen EW

Subjects

Amino Acid Sequence, Base Sequence, Blood Coagulation Factors, Carbon-Carbon Ligases, DNA Mutational Analysis, Female, Heterozygote, Humans, Immunohistochemistry, Male, Microscopy, Electron, Transmission, Middle Aged, Mixed Function Oxygenases genetics, Molecular Sequence Data, Multidrug Resistance-Associated Proteins genetics, Pedigree, Polymerase Chain Reaction, Pseudoxanthoma Elasticum pathology, Sequence Homology, Amino Acid, Vitamin K Epoxide Reductases, Coagulation Protein Disorders complications, Coagulation Protein Disorders genetics, Pseudoxanthoma Elasticum complications, Pseudoxanthoma Elasticum genetics, Vitamin K

Abstract

Pseudoxanthoma elasticum (PXE) is a multisystem disorder characterized by ectopic mineralization of connective tissues with primary manifestations in the skin, eyes, and cardiovascular system. The classic forms of PXE are due to mutations in the ABCC6 gene that encodes the ABCC6 protein, a putative transmembrane transporter expressed primarily in the liver and the kidneys. PXE-like clinical findings have been encountered in association with vitamin K-dependent coagulation factor deficiency, an autosomal recessive disorder that is due to mutations in either the GGCX or VKORC1 genes. In this study, we investigated a family with two siblings with characteristic features of PXE and vitamin K-dependent coagulation factor deficiency. Mutation analysis identified two GGCX mutations in the affected individuals (p. R83W and p.Q374X); however, no mutations in either ABCC6 or VKORC1 could be found. GGCX encodes a gamma-glutamyl carboxylase necessary for activation of both coagulation factors in the liver and matrix gla protein, which, in fully carboxylated form, is able to prevent ectopic mineralization. Analysis of skin by specific antibodies demonstrated that matrix gla protein was found predominantly in undercarboxylated form and was associated with the mineralized areas in the patients' lesional skin. These observations pathomechanistically suggest that, in our patients, reduced carboxylase activity results in a reduction of matrix gla protein carboxylation, thus allowing peripheral mineralization to occur. Our findings also confirm GGCX as the second gene locus causing PXE.

Published

2009

28. Familial multiple coagulation factor deficiencies - chance associations and distinct clinical disorders.

Author

Robson PJ and Mumford AD

Subjects

Blood Coagulation Disorders, Inherited classification, Blood Coagulation Disorders, Inherited history, Coagulation Protein Disorders classification, Coagulation Protein Disorders history, Hemorrhagic Disorders classification, Hemorrhagic Disorders genetics, Hemorrhagic Disorders history, History, 20th Century, Humans, Syndrome, Blood Coagulation Disorders, Inherited genetics, Coagulation Protein Disorders genetics

Abstract

The familial multiple coagulation factor deficiencies (FMCFDs) are a group of rare haemostatic disorders of genetic origin in which there is reduced plasma activity of more than one coagulation factor. FMCFDs may arise from co-incidental inheritance of separate coagulation factor deficiencies or from a single genetic or cytogenetic defect. All the FMCFDs present significant challenges in diagnosis and management yet there is little systematic evidence with which to guide clinical practice. This review summarizes the historical literature that describes the FMCFDs and introduces a refined classification of these disorders. The clinical and laboratory characteristics of the most common FMCFDs are considered in detail.

Published

2009

29. Thrombophilic dimension of recurrent fetal loss in Indian patients.

Author

Vora S, Shetty S, and Ghosh K

Subjects

Abortion, Habitual blood, Adolescent, Adult, Annexin A5 immunology, Antibodies, Anticardiolipin blood, Antibody Specificity, Antiphospholipid Syndrome blood, Antiphospholipid Syndrome complications, Autoantibodies immunology, Autoantigens immunology, Blood Coagulation Disorders, Inherited blood, Coagulation Protein Disorders blood, Coagulation Protein Disorders genetics, Female, Humans, India, Lupus Coagulation Inhibitor blood, Pregnancy, Pregnancy Complications, Hematologic genetics, Pregnancy Trimesters, Risk Factors, Thrombophilia blood, Thrombophilia genetics, beta 2-Glycoprotein I immunology, Abortion, Habitual etiology, Autoantibodies blood, Blood Coagulation Disorders, Inherited complications, Coagulation Protein Disorders complications, Pregnancy Complications, Hematologic blood, Thrombophilia complications

Abstract

We studied the prevalence of acquired and genetic thrombophilia in 198 women with recurrent fetal loss who were having three or more than three abortions. Seventy-nine women had only early pregnancy losses, that is, first trimester abortions, 30 women had only late pregnancy losses, that is, second and third trimester abortions whereas 89 had both early and late pregnancy losses. The control group included 100 age-matched fertile parous women who did not have any obstetric complications and had at least one normal healthy child. Several genetic and acquired thrombophilia markers were studied. The strongest association was observed with anticardiolipin (odds ratio 22.6, confidence interval 5.7-89, P = 0) followed by lupus anticoagulant, anti-beta2 glycoprotein-1, antiannexin. Association of antiphospholipid antibody syndromes was detected with the time of pregnancy loss in anticardiolipin, lupus anticoagulants, which was significantly associated with early pregnancy loss as compared with second and third trimester loss. In case of beta2 glycoprotein-1, antiannexin it was less significantly associated with early pregnancy loss as compared with second and third trimester loss. The risk of fetal loss with protein S deficiency was the highest risk observed for any heritable thrombophilia, followed by protein C, factor V Leiden, endothelial protein C receptor, antithrombin III deficiency and beta448 fibrinogen polymorphism. Modest risks were also observed with 5,10-methylenetetrahydrofolate reductase, plasminogen activator inhibitor 4G/4G polymorphisms and beta448 fibrinogen polymorphism. A combination of two or more than two genetic risk factors were observed in 55 (27.7%), whereas the genetic and acquired risk factors were observed in 107 (54%) of the cases. Thrombophilia is an important contributing factor for both early and late pregnancy losses; approximately two-thirds of our cases of unexplained fetal losses could be explained by acquired or heritable thrombophilia or both, which is in line with other western studies.

Published

2008

30. Spectrum of changes in endogenous thrombin potential due to heritable disorders of coagulation.

Author

Ghosh K, Mota L, Shetty S, and Kulkarni B

Subjects

Area Under Curve, Coagulation Protein Disorders genetics, Factor V metabolism, Factor Xa metabolism, Hemorrhage etiology, Humans, Time Factors, Blood Coagulation Disorders, Inherited blood, Coagulation Protein Disorders blood, Thrombin biosynthesis

Abstract

The modern thrombin generation tests describe different phases of generation of thrombin that is initiation, amplification and inhibition of thrombin generation as well as the integral amount of generated thrombin. We investigated 55 patients with congenital deficiencies of different coagulation factors and analysed the relationship between the nature and the concentration of clotting factors, with different parameters of thrombin generation curve that is lag time, peak, time to peak and the area under curve or endogenous thrombin potential. The endogenous thrombin potential was unaffected by severe deficiency of factors XI and XII, and reduced in factor IX, VII and factor V and VIII deficiencies. The lag time was significantly prolonged in cases of severe factor VII, X and V deficiencies, and was almost normal in cases of factors VIII, IX, combined factors V and VIII, factor XI, XII and XIII deficiencies. The peak height was severely affected in cases of severe factor X, V, VIII and IX deficiency and combined deficiency of multiple vitamin K dependant coagulation factors, and significantly reduced in factor VIII, V, X, XIII and combined vitamin K deficiency.In all the patients with less than 40% thrombin generation, the clinical symptoms were severe. Bleeding symptoms were restricted to epistaxis and ecchymosis when thrombin generation was more than 90% of the normal. In the cases of combined deficiency of factors V and VIII all the values were intermediate as they exhibit mild deficiencies of both factors V and VIII and correlated well with the clinical symptoms. Endogenous thrombin potential of inherited isolated deficiencies of coagulation factors may thus provide an interesting insight about involvement of the deficient factor(s) at different phases of thrombin generation.

Published

2008

31. [Pseudoxanthoma elasticum with cutis laxa and multiple coagulation factor deficiency: a single genetic entity].

Author

Dereure O

Subjects

Genetic Heterogeneity, Humans, Multidrug Resistance-Associated Proteins genetics, Mutation genetics, Syndrome, Coagulation Protein Disorders genetics, Cutis Laxa genetics, Pseudoxanthoma Elasticum genetics

Published

2008

32. Coagulation disorders and inhibitors of coagulation in children from Mansoura, Egypt.

Author

Abdelrazik N, Rashad H, Selim T, and Tharwat L

Subjects

Adult, Blood Coagulation Disorders blood, Blood Coagulation Disorders congenital, Blood Coagulation Disorders etiology, Blood Coagulation Disorders, Inherited blood, Blood Coagulation Disorders, Inherited epidemiology, Blood Coagulation Disorders, Inherited genetics, Blood Coagulation Factors immunology, Child, Preschool, Coagulation Protein Disorders blood, Coagulation Protein Disorders epidemiology, Coagulation Protein Disorders genetics, Egypt epidemiology, Female, Hemorrhage etiology, Heterozygote, Hospitals, Pediatric statistics & numerical data, Hospitals, University statistics & numerical data, Humans, Infant, Infant, Newborn, Isoantibodies blood, Liver Diseases blood, Liver Diseases complications, Male, Prevalence, Severity of Illness Index, Vitamin K Deficiency Bleeding blood, Vitamin K Deficiency Bleeding epidemiology, Blood Coagulation Disorders epidemiology, Blood Coagulation Factors antagonists & inhibitors

Abstract

Disorders of coagulation in children often prove challenging to the medical care team. The aims of this study were to assess the spectrum and prevalence of coagulation disorders among children attending Mansoura University Children Hospital (MUCH), Mansoura, Egypt. A total of 105 pediatric patients were referred to MUCH. They were divided into two groups: congenital coagulation disorders (75 cases, age 45.36 +/- 48.59 months), and acquired coagulation disorders (30 cases, age 56.13 +/- 61.61 months). All patients were subjected to thorough history taking including the nature of bleeding, family, past history, mode of inheritance, and detailed physical findings. Hemostatic tests included: platelet count, bleeding time (BT), prothrombin time (PT), activated partial thromboplastin time (APTT), thrombin time (TT). Specific tests in the congenital group include assay of coagulation factors according to each disorder, Von Willebrand factor assay, ristocetin aggregation test, APTT mixing study for detection of inhibitors in complicated hemophilia cases, F VIII C to VWAg ratio with cut off 0.7 for detection of carriers in some hemophilia A families. Congenital disorders constituted 71.4% of the studied cases vs. 28.6% for acquired disorders. Hemophilia A (42.85%), hemophilia B (14.28%) and liver diseases (14.28%) represented the majority of the studied cases. Mild and moderate cases of hemophilia A and B are more frequent than severe cases in both types. Male sex is more frequent than female in the congenital group (94.7 vs. 5.3%, P < 0.001). Direct correlation existed between factor level assay and severity of hemophilia (r = 0.73, P = 0.006). Three mothers and one sister were identified as carrier out of four families. Anti-clotting factors inhibitor was detected in 18.2% of patients with hemophilia A and in 9.1% with hemophilia B. In conclusion, our study found that hemophilias are the most prevalent congenital coagulation disorders among children. Attention must be given for detection of hemophilia carriers and inhibitors of clotting factors.

Published

2007

33. Compound heterozygosity of novel missense mutations in the gamma-glutamyl-carboxylase gene causes hereditary combined vitamin K-dependent coagulation factor deficiency.

Author

Darghouth D, Hallgren KW, Shtofman RL, Mrad A, Gharbi Y, Maherzi A, Kastally R, LeRicousse S, Berkner KL, and Rosa JP

Subjects

Alleles, Amino Acid Sequence, Amino Acid Substitution, Base Sequence, Blood Coagulation Disorders, Inherited enzymology, Blood Coagulation Disorders, Inherited genetics, Child, Conserved Sequence, DNA Mutational Analysis, DNA Primers genetics, Evolution, Molecular, Female, Heterozygote, Humans, Infant, Male, Mixed Function Oxygenases genetics, Molecular Sequence Data, Mutation, Missense, Pedigree, Polymerase Chain Reaction, Sequence Homology, Amino Acid, Vitamin K Epoxide Reductases, Carbon-Carbon Ligases deficiency, Carbon-Carbon Ligases genetics, Coagulation Protein Disorders enzymology, Coagulation Protein Disorders genetics, Vitamin K metabolism

Abstract

Hereditary combined vitamin K-dependent (VKD) coagulation factor deficiency is an autosomal recessive bleeding disorder associated with defects in either the gamma-carboxylase, which carboxylates VKD proteins to render them active, or the vitamin K epoxide reductase (VKORC1), which supplies the reduced vitamin K cofactor required for carboxylation. Such deficiencies are rare, and we report the fourth case resulting from mutations in the carboxylase gene, identified in a Tunisian girl who exhibited impaired function in hemostatic VKD factors that was not restored by vitamin K administration. Sequence analysis of the proposita did not identify any mutations in the VKORC1 gene but, remarkably, revealed 3 heterozygous mutations in the carboxylase gene that caused the substitutions Asp31Asn, Trp157Arg, and Thr591Lys. None of these mutations have previously been reported. Family analysis showed that Asp31Asn and Thr591Lys were coallelic and maternally transmitted while Trp157Arg was transmitted by the father, and a genomic screen of 100 healthy individuals ruled out frequent polymorphisms. Mutational analysis indicated wild-type activity for the Asp31Asn carboxylase. In contrast, the respective Trp157Arg and Thr591Lys activities were 8% and 0% that of wild-type carboxylase, and their compound heterozygosity can therefore account for functional VKD factor deficiency. The implications for carboxylase mechanism are discussed.

Published

2006

34. The fibrinogen Aalpha R16C mutation results in fibrinolytic resistance.

Author

Flood VH, Al-Mondhiry HA, and Farrell DH

Subjects

Child, Preschool, Coagulation Protein Disorders blood, Fibrin metabolism, Heterozygote, Humans, Male, Coagulation Protein Disorders genetics, Fibrinogen genetics, Fibrinogens, Abnormal genetics, Fibrinolysis genetics, Mutation

Abstract

The fibrinogen Aalpha R16C mutation is a common cause of dysfibrinogenaemia and has been previously associated with both bleeding and thrombosis. However, the mechanism underlying the thrombotic phenotype has not yet been elucidated. This report characterises the defect in fibrinolysis seen as a result of the Aalpha R16C mutation. A young patient with dysfibrinogenaemia (fibrinogen Hershey III) was found to be heterozygous for the Aalpha R16C mutation. Functional assays were performed on the purified fibrinogen to characterise clot formation and lysis with plasmin and trypsin. Consistent with previous results, clot formation was diminished. Unexpectedly, fibrinolysis was also delayed. Plasminogen activation was normal, ruling out decreased plasmin generation as the mechanism behind the fibrinolytic resistance. Western blot analysis showed no difference in the amount of bound alpha2-antiplasmin or albumin. When clot lysis was assayed with trypsin substituted for plasminogen, a significant delay was also observed, indicating that defective binding to plasminogen could not explain the fibrinolytic resistance. These results suggest that the defective fibrinolysis is due to increased proteolytic resistance, most likely reflecting changes in clot structure.

Published

2006

35. Functional characterization of fibrinogen Bicêtre II: a gamma 308 Asn-->Lys mutation located near the fibrin D:D interaction sites.

Author

Marchi RC, Carvajal Z, Boyer-Neumann C, Anglés-Cano E, and Weisel JW

Subjects

Adult, Asparagine genetics, Coagulation Protein Disorders etiology, Factor XIII metabolism, Fibrin chemistry, Fibrin genetics, Fibrin ultrastructure, Fibrinogens, Abnormal physiology, Fibrinolysis genetics, Humans, Lysine genetics, Male, Microscopy, Electron, Scanning, Models, Molecular, Reference Values, Blood Coagulation genetics, Coagulation Protein Disorders genetics, Fibrin Fibrinogen Degradation Products genetics, Fibrinogens, Abnormal genetics, Fibrinogens, Abnormal metabolism, Mutation, Missense genetics

Abstract

The effects of the gamma-308 Asn-->Lys substitution of fibrinogen Bicêtre II on clot formation, structure and properties were determined to elucidate the role of this part of the molecule in fibrin polymerization. This process was followed by measurement of turbidity, and the structure and biophysical characteristics of the clots were studied by permeation, scanning electron microscopy, and rheological techniques. Turbidity studies revealed an increased lag period and greater final turbidity for fibrin BII clots, indicating impaired oligomer formation. By permeation it was found that BII clots had greater network porosity, four times more than that of the control. The clot architecture visualized by scanning electron microscopy was similar to that of control clots with pore size and fiber diameter slightly increased. BII clots had a stiffness decreased by more than half, and an increased loss tangent, a measure of the inelastic deformation of the clot. All these results suggest a disruption of the proper alignment of fibrin monomers during oligomer formation. Consistent with these results, fibrin cross-linking by adding the physiological concentration of factor XIII to the purified protein showed that gamma and alpha chain cross-linking was impaired in BII clots. This amino acid substitution defines distinctive effects on the surface of the D:D interaction sites that are reflected in the clot structure and functional properties.

Published

2006

36. Inherited thrombophilia.

Author

Franchini M, Veneri D, Salvagno GL, Manzato F, and Lippi G

Subjects

Afibrinogenemia, Blood Coagulation Factors analysis, Blood Coagulation Factors genetics, Child, Preschool, Coagulation Protein Disorders blood, Coagulation Protein Disorders therapy, Female, Fibrinolysis, Heparin Cofactor II deficiency, Humans, Male, Pregnancy, Risk Factors, Thrombophilia blood, Thrombophilia therapy, Thromboplastin deficiency, Blood Coagulation Factor Inhibitors deficiency, Coagulation Protein Disorders genetics, Coagulation Protein Disorders physiopathology, Genetic Predisposition to Disease genetics, Thrombophilia genetics, Thrombophilia physiopathology

Abstract

Inherited thrombophilia can be defined as a genetically determined predisposition to the development of thromboembolic complications. Since the discovery of activated protein C resistance in 1993, several additional disorders have been described and, at present, it is possible to identify an inherited predisposition in about 60 to 70% of patients with such complications. These inherited prothrombotic risk factors include qualitative or quantitative defects of coagulation factor inhibitors, increased levels or function of coagulation factors, defects of the fibrinolytic system, altered platelet function, and hyperhomocysteinemia. In this review, the main inherited prothrombotic risk factors are analyzed from epidemiological, laboratory, clinical, and therapeutic points of view. Finally, we discuss the synergism between genetic and acquired prothrombotic risk factors in particular conditions such as childhood and pregnancy.

Published

2006

37. A novel fibrinogen gamma chain mutation (gamma 239 Gln-->His) is the cause of dysfibrinogenemia Vicenza.

Author

Castaman G, Ghiotto R, Duga S, and Rodeghiero F

Subjects

Coagulation Protein Disorders genetics, Fibrinogen chemistry, Fibrinogens, Abnormal genetics, Humans, Blood Coagulation Disorders, Inherited genetics, Fibrinogen genetics, Mutation, Missense

Published

2005

38. Familial hypodysfibrinogenaemia associated with second occurrence of gamma326 Cys-->Tyr mutation.

Author

Dear A, Brennan SO, and George PM

Subjects

Adult, DNA Mutational Analysis, Family Health, Fibrinogens, Abnormal chemistry, Humans, Male, Point Mutation, Polymers, Thrombin Time, Coagulation Protein Disorders genetics, Fibrinogens, Abnormal genetics, Mutation, Missense, Venous Thrombosis genetics

Published

2005

39. Congenital bleeding disorders.

Author

Brown DL

Subjects

Blood Coagulation Disorders, Inherited physiopathology, Blood Coagulation Disorders, Inherited therapy, Blood Platelet Disorders genetics, Blood Platelet Disorders physiopathology, Child, Coagulation Protein Disorders diagnosis, Coagulation Protein Disorders genetics, Coagulation Protein Disorders physiopathology, Hemophilia A diagnosis, Hemophilia A physiopathology, Hemophilia A therapy, Humans, von Willebrand Diseases diagnosis, von Willebrand Diseases physiopathology, von Willebrand Diseases therapy, Blood Coagulation Disorders, Inherited diagnosis

Published

2005

40. Familial multiple coagulation factor deficiencies: new biologic insight from rare genetic bleeding disorders.

Author

Zhang B and Ginsburg D

Subjects

Carbon-Carbon Ligases metabolism, Coagulation Protein Disorders blood, Coagulation Protein Disorders complications, Factor V genetics, Factor V metabolism, Factor V Deficiency blood, Factor V Deficiency complications, Factor V Deficiency genetics, Factor VIII genetics, Factor VIII metabolism, Female, Hemophilia A blood, Hemophilia A complications, Hemophilia A genetics, Humans, Male, Mannose-Binding Lectins genetics, Membrane Proteins genetics, Models, Biological, Mutation, Vitamin K metabolism, Coagulation Protein Disorders genetics

Abstract

Combined deficiency of factor (F)V and FVIII (F5F8D) and combined deficiency of vitamin K-dependent clotting factors (VKCFD) comprise the vast majority of reported cases of familial multiple coagulation factor deficiencies. Recently, significant progress has been made in understanding the molecular mechanisms underlying these disorders. F5F8D is caused by mutations in two different genes (LMAN1 and MCFD2) that encode components of a stable protein complex. This complex is localized to the secretory pathway of the cell and likely functions in transporting newly synthesized FV and FVIII, and perhaps other proteins, from the ER to the Golgi. VKCFD is either caused by mutations in the gamma-carboxylase gene or in a recently identified gene encoding the vitamin K epoxide reductase. These two proteins are essential components of the vitamin K dependent carboxylation reaction. Deficiency in either protein leads to under-carboxylation and reduced activities of all the vitamin K-dependent coagulation factors, as well as several other proteins. The multiple coagulation factor deficiencies provide a notable example of important basic biological insight gained through the study of rare human diseases.

Published

2004

41. Compound heterozygous mutations in the gamma-glutamyl carboxylase gene cause combined deficiency of all vitamin K-dependent blood coagulation factors.

Author

Rost S, Fregin A, Koch D, Compes M, Müller CR, and Oldenburg J

Subjects

Amino Acid Sequence, Animals, Heterozygote, Humans, Infant, Male, Molecular Sequence Data, Mutation, Missense, Point Mutation, Polymorphism, Restriction Fragment Length, Sequence Alignment, Carbon-Carbon Ligases genetics, Coagulation Protein Disorders genetics, Mutation, Vitamin K physiology

Abstract

Hereditary combined deficiency of the vitamin K-dependent coagulation factors II, VII, IX, X, protein C, S and protein Z (VKCFD) is a very rare autosomal recessive inherited bleeding disorder. The phenotype may result from functional deficiency of either the gamma-glutamyl carboxylase (GGCX) or the vitamin K epoxide reductase (VKOR) complex. We report on the third case of VKCFD1 with mutations in the gamma-glutamyl carboxylase gene, which is remarkable because of compound heterozygosity. Two mutations were identified: a splice site mutation of exon 3 and a point mutation in exon 11, resulting in the replacement of arginine 485 by proline. Screening of 100 unrelated normal chromosomes by restriction fragment length polymorphism and denaturing high-performance liquid chromatography analysis excluded either mutation as a frequent polymorphism. Substitution of vitamin K could only partially normalize the levels of coagulation factors. It is suggested that the missense mutation affects either the propeptide binding site or the vitamin K binding site of GGCX.

Published

2004

42. Biophysical characterization of fibrinogen Caracas I with an Aalpha-chain truncation at Aalpha-466 Ser: identification of the mutation and biophysical characterization of properties of clots from plasma and purified fibrinogen.

Author

Marchi R, Meyer M, de Bosch N, Soria J, Arocha-Piñango CL, and Weisel JW

Subjects

Biomechanical Phenomena, Coagulation Protein Disorders genetics, DNA Mutational Analysis, Family Health, Fibrin chemistry, Fibrin metabolism, Fibrinogens, Abnormal chemistry, Fibrinogens, Abnormal physiology, Humans, Microscopy, Electron, Scanning, Porosity, Sequence Deletion, Blood Coagulation, Codon, Nonsense, Fibrinogen genetics, Fibrinogens, Abnormal genetics

Abstract

Fibrinogen Caracas I is a dysfibrinogenemia with a mild bleeding tendency; a novel nonsense mutation, in the gene coding the Aalpha-chain, identified in this study as G4731T, giving rise to a new stop codon at Aalpha-Glu 467. Fibrinogen from two family members, the mother and sister of the propositus, both heterozygous for the mutation were studied, analyzing clots made from both plasma and purified fibrinogen. Clot structure and properties were characterized by turbidity, permeation, scanning electron microscopy and rheological studies. Permeation through Caracas I plasma clots was decreased, consistent with the decreased final turbidity. As shown by scanning electron microscopy, plasma clots from the patients were composed of very thin fibers, with increased fibrin density and reduced pore size. Viscoelastic measurements revealed that fibrinogen Caracas I plasma clots were much stiffer and less subject to compaction. These results demonstrate a key role of the carboxyl-terminal alpha chains of fibrin in lateral aggregation during polymerization and reinforce the utility of studying plasma clots. It is important to point out that the biophysical studies with fibrinogen purified by two different methods yielded contradictory results, which can be accounted for by selective purification of certain molecular species as seen by two-dimensional electrophoresis.

Published

2004

43. Is there a 'Basque' profile regarding autosomal recessive deficiencies of coagulation factors?

Author

Bauduer F, Ducout L, Dutour O, and Degioanni A

Subjects

Adolescent, Adult, Age of Onset, Aged, Aged, 80 and over, Child, Child, Preschool, Chromosome Disorders ethnology, Coagulation Protein Disorders ethnology, Female, France ethnology, Homozygote, Humans, Infant, Male, Middle Aged, Chromosome Disorders genetics, Coagulation Protein Disorders genetics

Abstract

When excluding haemophilia and von Willebrand disease, coagulation factors deficiencies constitute rare autosomal recessive disorders (<1 in 500,000) of less precisely defined epidemiology. We have reported herein the distribution of these entities in the French Basque Country, a genetic isolate of very old individualization with peculiar biological specificities. The prevalence of these disorders was markedly high, especially, as already shown, factor XI deficiency. This unusual profile needs to be discussed in the view of population genetics.

Published

2004

44. Genetics of thrombophilia: impact on atherogenesis.

Author

Voetsch B and Loscalzo J

Subjects

Arteriosclerosis etiology, Blood Vessels metabolism, Coagulation Protein Disorders genetics, Fibrinolysis genetics, Fibrinolysis physiology, Humans, Arteriosclerosis genetics, Thrombophilia genetics

Abstract

Purpose of Review: The goal of this review is to present an update on basic and epidemiological findings associating variants in prothrombotic genes with atherogenesis and atherothrombotic disease., Recent Findings: The relation between atherosclerosis and thrombosis has long been recognized but only recently has it been understood that certain hemostatic factors affect not only thrombus formation, but also have a direct atherogenic role. Atherosclerosis is a complex disorder that results from the interaction of multiple genetic and environmental factors. Numerous polymorphisms and mutations in genes related to the hemostatic system and to vascular redox determinants that modulate nitric oxide bioavailability have been identified in the past decade; their role in atherogenesis and the risk of cardiovascular disease, however, remain uncertain. We will discuss the functional implications and association with disease risk of polymorphisms in coagulation factors (fibrinogen, prothrombin, and factor V); fibrinolytic factors (plasminogen activator inhibitor 1 and lipoprotein(a)); platelet surface receptors; and vascular redox determinants (methylenetetrahydrofolate reductase, endothelial nitric oxide synthase, and the antioxidant enzymes cellular glutathione peroxidase and paraoxonase)., Summary: Overall, these genetic variants have a modest effect on risk when considered individually but gain potency when acting synergistically with other genetic or environmental risk factors. We conclude that a better characterization of these interactions, in addition to the identification of potential novel genetic determinants, constitute key issues in the future understanding of the pathogenesis of atherothrombosis.

Published

2004

45. DNA-based lab tests.

Subjects

Blood Coagulation genetics, Coagulation Protein Disorders genetics, Factor V genetics, Humans, Prothrombin genetics, Coagulation Protein Disorders diagnosis, Mutation, Reagent Kits, Diagnostic, Thrombosis prevention & control

Published

2004

46. Medicine: K is for koagulation.

Author

Sadler JE

Subjects

Animals, Anticoagulants pharmacology, Chromosome Mapping, Chromosomes, Human, Pair 16 genetics, Coagulation Protein Disorders enzymology, Drug Resistance genetics, Humans, Mice, Mixed Function Oxygenases antagonists & inhibitors, Mixed Function Oxygenases chemistry, Mixed Function Oxygenases metabolism, Mutation, Missense genetics, Rats, Vitamin K metabolism, Vitamin K Epoxide Reductases, Coagulation Protein Disorders genetics, Mixed Function Oxygenases genetics

Published

2004

47. Mutations in VKORC1 cause warfarin resistance and multiple coagulation factor deficiency type 2.

Author

Rost S, Fregin A, Ivaskevicius V, Conzelmann E, Hörtnagel K, Pelz HJ, Lappegard K, Seifried E, Scharrer I, Tuddenham EG, Müller CR, Strom TM, and Oldenburg J

Subjects

Amino Acid Sequence, Animals, Base Sequence, COS Cells, Cell Line, Chromosome Mapping, Coagulation Protein Disorders enzymology, DNA Mutational Analysis, Humans, Mice, Mixed Function Oxygenases antagonists & inhibitors, Mixed Function Oxygenases chemistry, Mixed Function Oxygenases metabolism, Molecular Sequence Data, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Vitamin K Epoxide Reductases, Coagulation Protein Disorders genetics, Drug Resistance genetics, Mixed Function Oxygenases genetics, Mutation, Missense genetics, Warfarin pharmacology

Abstract

Coumarin derivatives such as warfarin represent the therapy of choice for the long-term treatment and prevention of thromboembolic events. Coumarins target blood coagulation by inhibiting the vitamin K epoxide reductase multiprotein complex (VKOR). This complex recycles vitamin K 2,3-epoxide to vitamin K hydroquinone, a cofactor that is essential for the post-translational gamma-carboxylation of several blood coagulation factors. Despite extensive efforts, the components of the VKOR complex have not been identified. The complex has been proposed to be involved in two heritable human diseases: combined deficiency of vitamin-K-dependent clotting factors type 2 (VKCFD2; Online Mendelian Inheritance in Man (OMIM) 607473), and resistance to coumarin-type anticoagulant drugs (warfarin resistance, WR; OMIM 122700). Here we identify, by using linkage information from three species, the gene vitamin K epoxide reductase complex subunit 1 (VKORC1), which encodes a small transmembrane protein of the endoplasmic reticulum. VKORC1 contains missense mutations in both human disorders and in a warfarin-resistant rat strain. Overexpression of wild-type VKORC1, but not VKORC1 carrying the VKCFD2 mutation, leads to a marked increase in VKOR activity, which is sensitive to warfarin inhibition.

Published

2004

48. Rare Bleeding Disorder Registry: deficiencies of factors II, V, VII, X, XIII, fibrinogen and dysfibrinogenemias.

Author

Acharya SS, Coughlin A, and Dimichele DM

Subjects

Adolescent, Adult, Afibrinogenemia epidemiology, Afibrinogenemia genetics, Aged, Child, Child, Preschool, Coagulation Protein Disorders genetics, Coagulation Protein Disorders therapy, Factor V Deficiency epidemiology, Factor V Deficiency genetics, Factor VII Deficiency epidemiology, Factor VII Deficiency genetics, Factor X Deficiency epidemiology, Factor X Deficiency genetics, Factor XIII Deficiency epidemiology, Factor XIII Deficiency genetics, Fibrinogens, Abnormal, Heterozygote, Homozygote, Humans, Hypoprothrombinemias epidemiology, Hypoprothrombinemias genetics, Infant, Infant, Newborn, Middle Aged, Registries, Retrospective Studies, Blood Coagulation Factors genetics, Coagulation Protein Disorders epidemiology

Abstract

A North American registry for rare bleeding disorders [factor (F)II, factor (F)VII, factor (F)X, factor (F)V, factor (F)XIII, fibrinogen deficiencies and dysfibrinogenemias] was established to gather information about disease prevalence, genotyping frequency, diagnostic events, clinical manifestations, treatment and prophylaxis strategies, as well as disease- and treatment-related complications. Questionnaires were sent to 225 hemophilia treatment centers in the USA and Canada. Among 26% of responding centers, 294 individuals [4.4% of the registered children (200/4583) and 2.4% of adults (94/3809)] were diagnosed with one or more of the rare bleeding disorders (RBDs) included in this survey. The ethnic distribution for each disorder paralleled that of the general US population with the exception of the disproportionately large number of Latinos with FII deficiency. Only 5.4% of affected individuals were genotyped. An abnormal preoperative bleeding screen most often led to diagnosis. The most common coagulopathy was FVII deficiency; however, 40% of homozygous patients were asymptomatic. FX and FXIII deficiencies caused the most severe bleeding manifestations. Among all RBDs, the most common sites of bleeding were skin and mucus membranes. Multiple products were used to treat hemorrhage; however, half of the bleeding episodes required no therapy. The majority of patients suffered no long-term complications from hemorrhage. Treatment-related complications included viral seroconversion, anemia, allergic reactions and venous access device-related events. This registry provides the most comprehensive information to date about North American individuals with RBDs and could serve as an important resource for both basic scientist and clinician.

Published

2004

49. Hypofibrinogenemia caused by a nonsense mutation in the fibrinogen Bbeta chain gene.

Author

Mimuro J, Hamano A, Tanaka T, Madoiwa KS, Sugo T, Matsuda M, and Sakata Y

Subjects

Aged, Coagulation Protein Disorders congenital, DNA Mutational Analysis methods, Deoxyribonucleases, Type II Site-Specific, Female, Fibrinogen analysis, Fibrinogen genetics, Humans, Point Mutation, Coagulation Protein Disorders genetics, Codon, Nonsense, Fibrinogens, Abnormal genetics

Abstract

Congenital hypofibrinogenemia, fibrinogen Tottori II, caused by a nonsense mutation in the fibrinogen Bbeta chain gene, was found in a 68-year-old Japanese female. The plasma fibrinogen level was 99.2 mg dL(-1) as determined by the thrombin time method. No overt molecular abnormalities were observed in purified patient fibrinogen by SDS-PAGE analysis. After sequencing all exons and exon-intron boundaries of three fibrinogen genes, we found a heterozygous single point mutation of T-->G at position 3356 of the patient fibrinogen Bbeta chain gene. This nucleotide mutation results in a nonsense mutation (TAT sequence for Bbeta 41Tyr to TAG sequence for a translation termination signal). The mutation was confirmed by polymerase chain reaction-restriction fragment length polymorphism analysis, since this nucleotide mutation results in a new NheI recognition sequence at this position. These data indicated that the nonsense mutation of the fibrinogen Bbeta chain gene caused a truncated fibrinogen Bbeta chain, which may not be assembled in the fibrinogen molecule.

Published

2003

50. Spontaneous intracerebral hemorrhage due to coagulation disorders.

Author

Quinones-Hinojosa A, Gulati M, Singh V, and Lawton MT

Subjects

Adolescent, Adult, Aged, Blood Coagulation Disorders physiopathology, Case Management, Cerebral Hemorrhage diagnosis, Cerebral Hemorrhage therapy, Child, Child, Preschool, Coagulation Protein Disorders complications, Coagulation Protein Disorders genetics, Coagulation Protein Disorders physiopathology, Craniotomy, Female, Fibrinolytic Agents adverse effects, Forecasting, Hemophilia A complications, Hemostasis physiology, Humans, Infant, Male, Middle Aged, Neoplasms complications, Platelet Aggregation Inhibitors adverse effects, Postoperative Complications blood, Pregnancy, Pregnancy Complications, Hematologic blood, Puerperal Disorders blood, Randomized Controlled Trials as Topic, Risk Factors, Blood Coagulation Disorders complications, Cerebral Hemorrhage etiology

Abstract

Although intracranial hemorrhage accounts for approximately 10 to 15% of all cases of stroke, it is associated with a high mortality rate. Bleeding disorders account for a small but significant risk factor associated with intracranial hemorrhage. In conditions such as hemophilia and acute leukemia associated with thrombocytopenia, massive intracranial hemorrhage is often the cause of death. The authors present a comprehensive review of both the physiology of hemostasis and the pathophysiology underlying spontaneous ICH due to coagulation disorders. These disorders are divided into acquired conditions, including iatrogenic and neoplastic coagulopathies, and congenital problems, including hemophilia and rarer diseases. The authors also discuss clinical features, diagnosis, and management of intracranial hemorrhage resulting from these bleeding disorders.

Published

2003