Intraventricular Hemorrhage Clinical Trial
Official title:
Research a New Predictive Marker of Intraventricular Hemorrhage in Very Preterm Infants: HEMO PREMA Study
The most frequent complications in premature infants are neurological complications:
intracranial hemorrhages and white matter lesions. In Epipage 2 study the incidence of
severe intraventricular hemorrhages remains stable. Severe hemorrhages are associated with
neurological sequelae.
A recent study in humans and in animals shows the role of the complex formed by plasminogen
activator (t-PA) and its inhibitor (PAI-1) in the induction of vascular fragility via
stromelysin (MMP-3). FIBRINAT study in Rouen University Hospital showed a rate of complex
t-PA-PAI1 probably very high in preterm infants. An other factor maturation PDGF-C induced
by t-PA is associated with the vascular embrittlement. Among the few genetic factors
associated with cerebral palsy include 2 SNP of PAI-1 gene and one SNP in the gene of
endothelial NO synthase.
The hypothesis is that a high rate of the complex t-PA-PAI-1 in cord blood could be a high
risk of intracranial hemorrhage in preterm infants and provide predictive of their
occurrence. The rates of MMP-3, PDGF-C and PAI-1 free in cord blood, and the polymorphism of
PAI-1 gene and eNOS could separately or associated with the main criterion to identify
predictive of hemorrhages.
The main objective is to search a rate difference of the complex t-PA-PAI-1 in cord blood of
preterm infants (before 30 weeks of gestation) that would predict intracranial hemorrhage
coming in the first days of life.
The secondary objectives are
- Evaluate potential marker risk of high levels of MMP-3, PAI-1 free, and PDGF-CC
- Search in both groups the presence of alleles -675G4 / G5 and 11053 (G / T) of the
PAI-1 gene and -922 (A / G) of the eNOS gene.
120 preterm infants will be included before 30 weeks of gestation with precise
inclusion and exclusion criteria during a period of 3 years.
Patients will be divided into two groups according to whether they will or not showed
intracranial hemorrhage (detected by ultrasound J5-J7).
The complex rate tPA-PAI-1, PAI-1 free, MMP-3 and PDGF-C will be measured. The comparison
between the two groups will be carried out using statistical tests. Comparison of the
presence of the alleles -675 4G and 11053T the PAI-1 gene or -922G eNOS gene between the two
groups will be performed.
The demonstration of this hypothesis would permit to identify children from birth in whom
the immediate implementation of preventive treatment of bleeding is desirable.
n/a
Allocation: Non-Randomized, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Prevention
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