Factor VII Activity and Antigen in Hemophilia B Variants

In 23 patients with Hemophilia B (variants: II B-, 5 BR and 7 B+) factor VII Activity (VII:C) and Antigen (VII:Ag), in correlation with Thrombotest were measured. Thrombotest was found prolonged in 14 patients (in 8 > x+3SD and in 6 >x+2SD). Factor VII:C was found reduced in 1/11 B-, in 2/5 BR and in 4/7 B+ variants. Factor VII:Ag was normal in all but one patient (a 5 years old boy). The ratio VII:C/VII:Ag was abnormal in 8 patients. In these patients factors II and X activities were always within the normal range. The discrepances between VII:C and VII:Ag may be due to: 1) very minor vitamin K deficiency (presence of small amounts of PIVKA-II), 2) an inhibition of factor VII activation by a factor IX “abnormal” molecule, and 3) the synthesis of an abnormal molecule of factor VII.

Factor VII Activity and Antigen in Haemophilia B Variants

10.1055/s-0038-1650001 ◽

1980 ◽

Vol 43 (01) ◽

pp. 016-019 ◽

Cited By ~ 5

Author(s):

M G Mazzucconi ◽

R M Bertina ◽

D Romoli ◽

M Orlando ◽

G Avvisati ◽

...

Keyword(s):

Prothrombin Time ◽

Vitamin K ◽

Normal Values ◽

Factor Ix ◽

Factor Vii ◽

Confidence Limits ◽

Vitamin K Deficiency ◽

Haemophilia B ◽

K Deficiency ◽

Mild Deficiency

SummaryTwenty three patients belonging to 18 different pedigrees of Haemophilia B were studied with regard to ox-brain prothrombin time and its correlation to factor VII.Eleven among them were B-negative (no detectable factor IX antigen), five were B-reduced (factor IX antigen detectable but below the normal values) and seven were B-positive (normal levels of factor IX antigen).Ox-brain prothrombin time was found prolonged (≥ x̄ + 2.5 SD:99% confidence limits) in nine patients. Factor VII Activity (VII: C) was found reduced in 1/11 B-negative, in 2/5 B-reduced and in 4/7 B-positive patients. Factor VII Antigen (VII: Ag) was found normal in all but one patient.The ratio VII:C/VII:Ag was abnormal in eight patients independently from the variant of Haemophilia B. The underlying defect which causes the prolongation of Ox-brain prothrombin time due to factor VII: C mild deficiency is heterogeneous. Age, a mild Vitamin K deficiency, the presence of an inhibitor of Factor VII activation and other unknown causes, may be responsible for this pattern.

Acquired Vitamin K Deficiency as Unusual Cause of Bleeding Tendency in Adults: A Case Report of a Nonhospitalized Student Presenting with Severe Menorrhagia

Case Reports in Obstetrics and Gynecology ◽

10.1155/2017/4239148 ◽

2017 ◽

Vol 2017 ◽

pp. 1-3 ◽

Cited By ~ 1

Author(s):

Omid Reza Zekavat ◽

Gholamreza Fathpour ◽

Sezaneh Haghpanah ◽

Seyed Javad Dehghani ◽

Maryam Zekavat ◽

...

Keyword(s):

Vitamin K ◽

Coagulation Factor ◽

Energy Drinks ◽

High Energy ◽

Factor Ix ◽

Factor Vii ◽

Bleeding Tendency ◽

Factor X ◽

Vitamin K Deficiency ◽

We report a rare case of acquired vitamin K deficiency presenting with severe menorrhagia and without any gynecological problem. Partial thromboplastin time (59.2 seconds) and prothrombin time (33.1 seconds, INR: 5.97) were considerably prolonged in laboratory evaluations. A complete coagulation factor assay test was performed for the patient: factor IX, 24%; factor II, 41%; factor VII, 3%; and factor X, 52%. She had been taking many high-energy drinks and she had inadequate dietary intake for the past 6 months. Given that she had vitamin K deficiency (VKD), a course of vitamin K therapy was started for her in the hospital. This case showed the potential for menorrhagia due to VKD with use of high-energy drinks and the value of a complete and detailed history in early diagnosis.

Factor VII Antibody-neutralizing Material in Hereditary and Acquired Factor VII Deficiency

Blood ◽

10.1182/blood.v38.1.1.1 ◽

1971 ◽

Vol 38 (1) ◽

pp. 1-8 ◽

Cited By ~ 59

Author(s):

SCOTT H. GOODNIGHT ◽

DONALD I. FEINSTEIN ◽

BJARNE ØSTERUD ◽

SAMUEL I. RAPAPORT

Keyword(s):

Liver Disease ◽

Vitamin K ◽

Factor Vii ◽

Vitamin K Deficiency ◽

Present Evidence ◽

Hereditary Factor ◽

Factor Vii Deficiency ◽

Coagulant Activity ◽

Abstract Evidence is provided for the existence of at least two types of hereditary factor VII deficiency. In one type there is synthesis of a protein which neutralizes a factor VII antibody but lacks coagulant activity. In the second type, no factor VII antibody neutralizing material is present. Evidence is also provided for the existence of two types of acquired factor VII deficiency. Apparently, low factor VII activity in liver disease results from decreased synthesis of factor VII protein. In contrast, warfarin administration or vitamin K deficiency leads to the synthesis of factor VII protein that lacks clotting activity.

THROMBO-HEMORRHAGIC SKIN NECROSIS DUE TO RAPID DEVELOPMENT OF SEVERE VITAMIN K DEFICIENCY ASSOCIATED WITH CHOLESTASIS

10.1055/s-0038-1644311 ◽

1987 ◽

Cited By ~ 1

Author(s):

J J Michiels ◽

R M Bertina

Keyword(s):

Vitamin K ◽

Skin Necrosis ◽

Protein C ◽

Degradation Products ◽

Rapid Development ◽

Factor Vii ◽

Vitamin K Deficiency ◽

Antigen Concentration ◽

Severe Vitamin ◽

A female patient is presented, who developed thrombotic and hemorrhagic skin necrosis of the feet and toes during an acute episode of severe vitamin K deficiency due to cholestasis in the absence of coumarin treatment. Painful blue toes and feet progressed to erythematous swelling and bluish discoloration with blister formations and immanent gangrene. The histo-pathology of skin excisions from the erythematous skin lesions showed extravasation of erythrocytes and extensive fibrin thrombus formations in capillaries and venules as has been described in patients with coumarin skin necrosis. At the time of painful acrocyanosis the results of coagulation investigations (platelets 109 × 109/1, APTT 56/35 sec., PT 61/15 sec., ThrombotestR (TT) less than 3%, NormotestR (NT) less than 10%, fibrinogen 1,6 g/l, absence of fibrin monomers and degradation products, factor V 1.00 u/ml, antithrombin lil 1.03 u/ml and alfa2 antiplasmin 0.97 u/ml were consistent with severe vitamin K deficiency. Measurements of vitamin K dependent factors revealed very low levels for procoagulant factor VII (16%) and protein C (22%) antigen concentration and normal levels for procoagulant factor II (97%) and procoagulant factor X (87%) antigen concentration. After substitution of 5 mg vitamin K1 both the TT and NT normalized.These data confirm the hypothesis that an imbalance within procoagulant and anticoagulant vitamin K dependent factors (severe protein C and factor VII deficiency as compared to the procoagulant factors IX, X and II due to rapid development of vitamin K deficiency) contributes to the pathogenesis of thrombo-hemorrhagic skin necrosis and that the so-called coumarin necrosis is not due to drug toxicity.

Cancer Procoagulant: A Novel Vitamin K-Dependent Activity?

10.1055/s-0038-1652047 ◽

1981 ◽

Author(s):

M B Donati ◽

F Delaini ◽

M Colucci ◽

G De Beilis Vitti ◽

D Locati ◽

...

Keyword(s):

Drinking Water ◽

Vitamin K ◽

Coagulation Factor ◽

Factor Vii ◽

Similar Degree ◽

Vitamin K Deficiency ◽

Tumor Implantation ◽

Dependent Activity ◽

K Deficiency ◽

Cancer Procoagulant

Cells from some experimental tumors have been found to possess a peculiar procoagulant activity, which directly activates coagulation factor X, independently of both the intrinsic and extrinsic clotting pathways. We report here that, in the Lewis Lung Carcinoma (3LL) model, such a cell procoagulant is inhibited by vitamin K-deficiency (either dietary or pharmacologically induced).Warfarin was given chronically to mice in drinking water from day 7 after i.m. tumor implantation at a schedule which maintained the prothrombin complex activity (thrombotest) at less than 5% of control values. Vitamin K-deficiency was also induced by feeding the mice with an appropriate diet at a schedule which gave a similar degree of plasma anticoagulation. At day 18 after tumor implantation macrophage- free 3LL cell suspensions obtained by spilling of necrosis- free tumor fragments were tested for their specific clot- promoting capacity by a one-stage recalcification time of factor VII-deficient plasma. 3LL cells from either group of vitamin K-deficient animals gave significantly longer clotting times than controls (84 ± 4 and 82 ± 3 sec versus 42 ± 2 sec, p< 0.001, n = 15 for each of the 3 groups) corresponding to 18-25% of the activity of controls.This effect was completely reversed by adding vit. K to drinking water of vitamin K-deficient animals. Administration of autologous prothrombin complex concentrate, sufficient to completely correct the thrombotest values for several hours before tumor cell harvest, did not modify the effect induced by vitamin K-deficiency on 3LL cells. This data suggests that cancer procoagulant may represent a new vitamin K-dependent activity; vitamin K-deficiency would thus display not only a plasmatic but also a “cellular” anticoagulant effect. The latter could be relevant to the reported antimetastatic effect of vitamin K-deficiency.

Des-Gamma-Carboxyprothrombin (PIVKA II) and Plasma Vitamin K1 in Newborns and Their Mothers

10.1055/s-0038-1646281 ◽

1992 ◽

Vol 68 (04) ◽

pp. 383-387 ◽

Cited By ~ 13

Author(s):

R von Kries ◽

M J Shearer ◽

J Widdershoven ◽

K Motohara ◽

G Umbach ◽

...

Keyword(s):

Vitamin K ◽

Plasma Vitamin ◽

Vitamin K1 ◽

Normal Range ◽

Vitamin K Deficiency ◽

Detection Rates ◽

Crossed Immunoelectrophoresis ◽

Normal Ranges ◽

Age Related ◽

SummaryAssessments of the vitamin K status in newborns and their mothers by means of des-γ-carboxy-prothrombin (PIVKA II) measurement have given equivocal results. Part of the variability could be attributed to differences in sensitivity (i.e. the ability to detect small concentrations) and validity (i.e. ability to detect vitamin K deficiency) of the methods applied. None of these methods have yet been validated with respect to plasma vitamin K1. In 22 healthy mother/infant pairs PIVKA II was determined using three different assays including ratio Xa/ecarin (Xa/ec), crossed immunoelectrophoresis (CIE), and an ELISA with a monoclonal antibody (MAB). The results were compared with conventional clotting tests and plasma vitamin K1. The following results were obtained:Cord blood: Clotting tests within age-related normal ranges; PIVKA II detection rates: 0/22 (Xa/ec), 1/22 (CIE), 4/22 (MAB); plasma vitamin K1: undetectable in 20/22.Mothers: Clotting tests all within normal range; PIVKA II detection rates: 1/22 (Xa/ec), 0/22 (CIE), 5/22 (MAB); plasma vitamin K1 (pg/ml) for all mothers (median; range): 186; 55–833; for PIVKA II positive mothers: 213; 59–699.PIVKA II detectability in newborns and mothers was not correlated. The results show an increase in sensitivity for PIVKA II detection in the order of MAB ≫CIE >Xa/ec. Due to the very low plasma vitamin K1 at birth, no correlation was possible between cord PIVKA II detectability and plasma vitamin K1. However, in mothers at term PIVKA II MAB appears to be unrelated to the vitamin K status.

Placental Transfer of Vitamin K1 and Its Implications in Fetal Hemostasis

10.1055/s-0038-1647631 ◽

1988 ◽

Vol 60 (01) ◽

pp. 039-043 ◽

Cited By ~ 52

Author(s):

L Mandelbrot ◽

M Guillaumont ◽

M Leclercq ◽

J J Lefrère ◽

D Gozin ◽

...

Keyword(s):

Vitamin K ◽

High Performance ◽

Ultrasound Guidance ◽

Placental Transfer ◽

Vitamin K1 ◽

Vitamin K Deficiency ◽

Prothrombin Activity ◽

Oral Supplementation ◽

K Deficiency ◽

The Mean

SummaryVitamin K status was evaluated using coagulation studies and/ or vitamin IQ assays in a total of 53 normal fetuses and 47 neonates. Second trimester fetal blood samples were obtained for prenatal diagnosis under ultrasound guidance. Endogenous vitamin K1 concentrations (determined by high performance liquid chromatography) were substantially lower than maternal levels. The mean maternal-fetal gradient was 14-fold at mid trimester and 18-fold at birth. Despite low vitamin K levels, descarboxy prothrombin, detected by a staphylocoagulase assay, was elevated in only a single fetus and a single neonate.After maternal oral supplementation with vitamin K1, cord vitamin K1 levels were boosted 30-fold at mid trimester and 60 fold at term, demonstrating placental transfer. However, these levels were substantially lower than corresponding supplemented maternal levels. Despite elevated vitamin K1 concentrations, supplemented fetuses and neonates showed no increase in total or coagulant prothrombin activity. These results suggest that the low prothrombin levels found during intrauterine life are not due to vitamin K deficiency.

Kinetic Aspects of the Interaction of Blood-Clotting Enzymes

10.1055/s-0038-1651250 ◽

1968 ◽

Vol 20 (01/02) ◽

pp. 078-087 ◽

Cited By ~ 34

Author(s):

H. C Hemker ◽

A. D Muller

Keyword(s):

Vitamin K ◽

Blood Clotting ◽

Experimental Results ◽

Factor X ◽

Clotting Factors ◽

Vitamin K Deficiency ◽

SummaryPIVKA, the circulating anticoagulant protein found in vitamin K deficiency can, on kinetical grounds, be recognized as an analogue of factor X. The existence of analogues of other vitamin K-dependent clotting factors cannot be ruled out, but need not be assumed to explain the experimental results.

Extravascular Administration of Factor IX: Potential for Replacement Therapy of Canine and Human Hemophilia B

10.1055/s-0038-1656082 ◽

1997 ◽

Vol 77 (05) ◽

pp. 0944-0948 ◽

Cited By ~ 20

Author(s):

Darla Liles ◽

Charles N Landen ◽

Dougald M Monroe ◽

Celeste M Lindley ◽

Marjorie s Read ◽

...

Keyword(s):

Gene Therapy ◽

Vitamin K ◽

Absorption Rate ◽

Venous Access ◽

Factor Ix ◽

Hemophilia B ◽

Current Therapy ◽

Home Therapy ◽

Routes Of Administration ◽

Plasma Compartment

SummaryCurrent therapy for hemophilia B requires large intravenous doses of factor IX (F.IX) given in the clinic or at home. Although home therapy is possible for many patients, it is often complicated by factors such as the lack of good venous access. Very little is known about extravascular routes for administering proteins like F.IX (57 kD) or other vitamin K-dependent procoagulant factors into the circulation. Questions about the absorption rate from extravascular administration as well as plasma recovery and bioavailability have arisen recently with the growing availibility of highly purified procoagulant proteins and increased interest in gene therapy of hemophilia B. Therefore, a group of studies were undertaken to determine the absorption rate, plasma recovery, and bioavailability of high purity, human plasma-derived F.IX concentrates administered via extravascular routes in hemophilia B dogs and in one human hemophilia B subject. Five hemophilia B dogs were given human F.IX via either a subcutaneous (SC), intramuscular (IM), intra- peritoneal (IP) or intravenous (IV) route. In a subsequent study, a single SC administration of human F.IX was compared to an identical IV dose of F.IX in the human hemophilia B subject. All extravascular routes of F.IX administration in both the canine and human gave lower levels of circulating plasma F.IX than the IV route, however all routes resulted in measurable F.IX activity. Of the extravascular routes, the IM injection in the canine resulted in a bioavailibility of 82.8%, while the SC injection resulted in a bioavailability of 63.5%. F.IX reached the plasma compartment by all extravascular routes used, confirming that F.IX can be absorbed extravascularly. The duration of measurable F.IX activity following extravascular administration is prolonged beyond that typically seen with IV administration. These data show that significant levels of F.IX may be obtained via SC injection in canine and ‘ human hemophilia B subjects and further highlight the potential of extravascular routes of administration for future experimental and clinical uses of F.IX and other procoagulant proteins.

Behavioral changes and osteocalcin in an experimental model of subclinical vitamin K deficiency in rats

10.26226/morressier.5785edc6d462b80296c99447 ◽

2016 ◽

Author(s):

Silvia Gancheva Marinova

Keyword(s):

Experimental Model ◽

Vitamin K ◽

Behavioral Changes ◽

Vitamin K Deficiency ◽

K Deficiency ◽

Subclinical Vitamin