Epistaxis Clinical Trial
Official title:
A Retro-prospective Pediatric Data Collection Study of the Correlation Between PT and the Level of Coagulant Factor VII
The purpose of our study:
Given the large number of coagulability tests done before a number of surgeries, specially
otolaryngology procedures, such as tonsillectomy and adenoidectomy, as well as a part of
epistaxis workup, prothrombin time (PT) and partial thromboplastin time (PTT) were checked,
and it was found that in some people there is an isolated elongated PT, a low level of factor
VII was found in these people.
The purpose of the current study is to find a correlation between the value of PT\INR and the
level of factor VII, we tried to do so by a retro-prospective study on patients known to have
a factor VII deficiency at Laniado hospital, such a correlation could make both the diagnosis
and the management of people with factor VII deficiency easier and more accessible.
The study levels:
1. Data collection : On the children's population who are known for their lack of Factor
VII, we will check PT levels, we will concentrate the data in the table, along with
personal information such as age and gender
2. Data Processing : We will try to conduct a statistical relationship between the PT
values and Factor VII levels, to look for statistical significance, we will try to find
a model for predicting the level of factor VII based on PT
Number of participants:
60 participants
Ages of participants:
0-18 years old
Gender of participants:
Both sexes
Inclusion criteria:
1. A participant who is 0-18 years old
2. A participant who is, except for bleeding tendency, healthy in general
3. A participant who has elongated PT
4. A participant who has normal PTT
Exclusion criteria:
1. Background disease
2. Use of medications
3. Use of anti coagulation drugs
The duration of the study :
The study is of a retrospective type, we already have a number of subjects, we need more as
to reach statistical significance, so the expectation is two to three months
Factor VII is one of the main components of the coagulation process. It belongs to the serine
proteases and it dependents on vitamin K in order to function. Its primary function is to
initiate the clotting process itself, along with tissue factor: Following a vascular
endothelial injury, there is a response of vasoconstriction, the blood flow in contact with
the subendothelial matrix, at that time, TF, a protein in the same matrix, binds to and
activates the VII coagulation factor, then, FVIIa-TF complex begins the coagulation cascade,
at the end of that cascade, fibrin is formed.
The factor VII gene is located on the long arm of chromosome 13, sized 12 kD, contains 12
axons that encode a protein composed of 406 amino acids, it`s located at a distance of 2.8 kD
from the gene of factor X.
More than 120 mutations have been found in factor VII gene to date, the association between
genotype and phenotypes is unclear in most cases however. Seligsohn and his colleagues
described one of the mutations in Factor VII, 5-Ser339Phe, which was found in three Tunisian
families and caused a tendency to bleed through a mechanism of reduced factor X activation.
When it comes to Factor VII deficiency, the missing is never hermetic as such condition is
not compatible with life as seen from work on knockout mice. Partially missing factor VII is
the most common of all rare coagulation problems. Clinically, these are usually epistaxis,
easy bruising, gum bleeding, muscle hematoma, hamarhtrosis, hematuria, postoperative
bleeding, although there may also be conditions of life threatening blood in the nervous
system and in the gastrointestinal tract. Except for increased menstruation that occurs in
about 70% of the women with factor VII deficiency, there is no gender difference in symptoms.
Suspicion of Factor VII deficiency is usually done in the course of screening in family
members with a known deficiency or on tests following an episode of bleeding, such as
epistaxis or surgery in areas with a tendency to bleed (nose, throat or teeth) .
An abnormal PT test indicates a lack of factor VII. An elongated PTT test can suggest
hemophilia A and B (missing factors VIII and IX, respectively), lack of factor XI, incomplete
factor XII or von disease willebrand / VWF . The extension of PT also implies a deficiency in
the factors X, V, II and fibrinogen, and the result is represented by a percentage relative
to normal people.
The diagnosis of Factor VII deficiency is laboratory. The initial laboratory tests are PT,
aPTT and platelet count, followed by a FVII coagulant activity test for prolonged PT states.
In order to confirm the result, the FVII assay is performed again
Prothrombin time is typically analyzed by a laboratory technologist on an automated
instrument at 37 °C. Blood is drawn into a test tube containing liquid sodium citrate, which
acts as an anticoagulant by binding the calcium in a sample. The blood is mixed, then
centrifuged to separate blood cells from plasma (as prothrombin time is most commonly
measured using blood plasma). A sample of the plasma is extracted from the test tube and
placed into a measuring test tube Next an excess of calcium is added to the test tube,
thereby reversing the effects of citrate and enabling the blood to clot again. Finally, in
order to activate the extrinsic / tissue factor clotting cascade pathway, tissue factor is
added and the time the sample takes to clot is measured optically. The prothrombin ratio
(INR) is the prothrombin time for a patient sample divided by the result for control plasma.
There are two types of Factor VII deficiency. The first is a quantitative with both a lack of
FVII coagulant activity and with a low level of FVII antigen, the second one is qualitative
with a low FVII coagulant activity but a normal level of FVII antigen. In fact, the
examination of the antigen distinguishes between these two missing types, but does not
predict the tendency to bleed, and it is not recommended to diagnose Factor VII deficiency on
the basis of the antigen test. However, for known patients receiving a recombinant factor it
can be useful.
There are no clear guidelines for the treatment of hereditary deficiency VII. Recombinant
factor VII is a choice in many cases for both children and adults, but there are other
treatment options as discussed in our study.
The purpose of the current study is to find a correlation between the value of PT\INR and the
level of factor VII, we tried to do so by a retro-prospective study on patients known to have
a factor VII deficiency at Laniado hospital, such a correlation could make both the diagnosis
and the management of people with factor VII deficiency easier and more accessible.
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