Post-Partum Hemorrhage Clinical Trial
Official title:
Hexakaprone Treatment for Post-Partum Hemorrhage Prophylactic
Post-Partum Hemorrhage (PPH) is a common obstetrical complication. It may occur after both vaginal and cesarean delivery with a reported prevalence of 4-6% of deliveries [1]. Prophylactic treatment with oxytocin after fetus extraction is a common practice. [1,2]Transexamic acid - Hexakapron is a potent antifibrinolytic, it prevents lysine adhesion to plasminogen molecules by blocking its binding site. It can lower fibrinolysis rate and by that reduce bleeding [9]. Systematic treatment of anti-fibrinolytic drugs is in surgical practice after procedures such as coronary artery bypass graft, orthopedic surgeries and liver transplantation [10-13]. Hexakapron is an FDA approved drug, it is defined as a class B drug for pregnancy and lactation [12], it is already being used in a non-routine fashion in the delivery room during PPH.In obstetrics Hexakapron given before vaginal or cesarean delivery has been presumed to decrease blood loss and PPH. 2 studies that included 453 woman reported decrease in PPH (RR 0.51, 95% CI 0.36 to 0.72) [13-15]. However specific protocols for prophylactic treatment with Hexakapron as available with oxytocin are lacking, and further research is necessary to determine such guidelines [16].
Post-Partum Hemorrhage (PPH) is a common obstetrical complication. It may occur after both
vaginal and cesarean delivery with a reported prevalence of 4-6% of deliveries [1].
Prophylactic treatment with oxytocin after fetus extraction is a common practice. [1,2] The
increase in plasma volume during pregnancy, and uterine perfusion that reaches 750ml/min
near term [3] are causes for excessive blood loss during vaginal or cesarean delivery. Blood
loss is approximately 500ml and 1000ml during vaginal and cesarean delivery respectively.
Studies have shown that blood transfusion treatment reaches to up to 6 % after cesarean
section [5-6].
During placental delivery fibrinogen and fibrin degradation and plasminogen activation
occurs. This causes fibrinolytic cascade that continues 6-10 hours post-partum [7]. Tissue
injury during cesarean section may convert the hemostatic equilibrium towards fibrinolysis
that results in excessive bleeding [8]/ Transexamic acid - Hexakapron is a potent
antifibrinolytic, it prevents lysine adhesion to plasminogen molecules by blocking its
binding site. It can lower fibrinolysis rate and by that reduce bleeding [9]. Systematic
treatment of anti-fibrinolytic drugs is in surgical practice after procedures such as
coronary artery bypass graft, orthopedic surgeries and liver transplantation [10-13].
Hexakapron is an FDA approved drug, it is defined as a class B drug for pregnancy and
lactation [12], it is already being used in a non-routine fashion in the delivery room
during PPH.
In obstetrics Hexakapron given before vaginal or cesarean delivery has been presumed to
decrease blood loss and PPH. 2 studies that included 453 woman reported decrease in PPH (RR
0.51, 95% CI 0.36 to 0.72) [13-15]. However specific protocols for prophylactic treatment
with Hexakapron as available with oxytocin are lacking, and further research is necessary to
determine such guidelines [16].
PPH jeopardize young reproductive women's health, it is specifically related to major
morbidity in the context of prior anemia which features this population in high rates [17].
PPH is the major maternal cause of death, with 100000 cases per year [6].
Thus the investigators sought to investigate the efficacy of Hexakapron, as a prophylactic
treatment after vaginal delivery and cesarean section, in reducing PPH.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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