Overview management of postpartum haemorrhage
amomtan
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Jul 05, 2011
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Antepartum &
Postpartum
Hemorrhage (APH &PPH)
Al-Momtan
Postpartum
Hemorrhage (APH &PPH)
Al-Momtan
Antepartum & Postpartum Hemorrhage
•Obstetrics is "bloody business."
•Death from hemorrhage still remains a leading
cause of maternal mortality.
•Hemorrhage was a direct cause of more than
18 percent of 3201 pregnancy-related
maternal deaths.
•Obstetrics is "bloody business."
•Death from hemorrhage still remains a leading
cause of maternal mortality.
•Hemorrhage was a direct cause of more than
18 percent of 3201 pregnancy-related
maternal deaths.
Postpartum Hemorrhage
•In spite of marked improvements in management, PPH
remains a significant contributor to maternal morbidity and
mortality both in developing and developed countries.
•One of the most challenging complications a clinician will face.
•Prevention, early recognition and prompt appropriate
intervention are the keys to minimizing its impact.
•In spite of marked improvements in management, PPH
remains a significant contributor to maternal morbidity and
mortality both in developing and developed countries.
•One of the most challenging complications a clinician will face.
•Prevention, early recognition and prompt appropriate
intervention are the keys to minimizing its impact.
DEFINITION:
The loss of >500ml of blood from the genital tract in
the first 24 hrs after delivery
(or)
< 500 ml with haemodynamic changes in the mother.
(or)
>1000 ml –cesarean section within 24 hrs.
(or)
> 1400 ml –Elective cesarean hysterectomy
(or)
> 3000 ml –Emergency cesarean hysterectomy
The loss of >500ml of blood from the genital tract in
the first 24 hrs after delivery
(or)
< 500 ml with haemodynamic changes in the mother.
(or)
>1000 ml –cesarean section within 24 hrs.
(or)
> 1400 ml –Elective cesarean hysterectomy
(or)
> 3000 ml –Emergency cesarean hysterectomy
-In a recent ACOG study PPH is defined as Haematocrit change of 10% or the
need for red cell transfusion.
Severe PPH - > 1500ml blood loss
or
Drop in Hb concentration 40g/l.
or
4 units of blood transfusion.
Secondary PPH -Blood loss between 24 hrs and 6 weeks
Post-delivery.
In general, early PPH involves heavier bleeding and greater morbidity.
need for red cell transfusion.
Severe PPH - > 1500ml blood loss
or
Drop in Hb concentration 40g/l.
or
4 units of blood transfusion.
Secondary PPH -Blood loss between 24 hrs and 6 weeks
Post-delivery.
In general, early PPH involves heavier bleeding and greater morbidity.
Incidence:
Subjective : 2 –11%
Objective : 20%
Classification of primary PPH
Atonic PPH –80%
Traumatic PPH –15%
Retained placenta, membranes,
coagulation failure –5%
Subjective : 2 –11%
Objective : 20%
Classification of primary PPH
Atonic PPH –80%
Traumatic PPH –15%
Retained placenta, membranes,
coagulation failure –5%
Haematological Changes in Pregnancy
•40% expansion of blood volume by 30 weeks
•600 ml/min of blood flows through intervillous space
•Appreciable increase in concentration of Factors I (fibrinogen),
VII, VIII, IX, X
•Plasminogen appreciably increased
•Plasmin activity decreased
•Decreased colloid oncotic pressure secondary to 25%
reduction in serum albumin
•40% expansion of blood volume by 30 weeks
•600 ml/min of blood flows through intervillous space
•Appreciable increase in concentration of Factors I (fibrinogen),
VII, VIII, IX, X
•Plasminogen appreciably increased
•Plasmin activity decreased
•Decreased colloid oncotic pressure secondary to 25%
reduction in serum albumin
Reduced Maternal Blood Volume
•Small stature
•Severe preeclampsia/eclampsia
•Early gestational age
•Small stature
•Severe preeclampsia/eclampsia
•Early gestational age
PPH
PPH
•The etiologies of early PPH are most easily understood as abnormalities of
one or more of four basic processes.
•The four “T” processes.
•Previous PPH!!
•The etiologies of early PPH are most easily understood as abnormalities of
one or more of four basic processes.
•The four “T” processes.
•Previous PPH!!
The Four “T”
Tone
Tissue
Trauma
Thrombin
Tone
Tissue
Trauma
Thrombin
PPH Risk Factors
•Many factors affect a woman’s risk of PPH.
•Each of these risk factors can be understood
as predisposing her to one or more of the four
“T” processes.
•Many factors affect a woman’s risk of PPH.
•Each of these risk factors can be understood
as predisposing her to one or more of the four
“T” processes.
PPH Risk Factors
PPH Risk Factors
PPH Risk Factors
PPH Risk Factors
PREVENTION OF PPH
•Although any woman can experience a PPH, the
presence of risk factors makes it more likely.
•For women with such risk factors, consideration
should be given to extra precautions such as:
–IV access
–Coagulation studies
–Crossmatching of blood
–Anaesthesia backup
–Referral to a tertiary centre
•Although any woman can experience a PPH, the
presence of risk factors makes it more likely.
•For women with such risk factors, consideration
should be given to extra precautions such as:
–IV access
–Coagulation studies
–Crossmatching of blood
–Anaesthesia backup
–Referral to a tertiary centre
PREVENTION OF PPH
•UTEROTONIC DRUGS
–Routine oxytocic administration in the third stage of labour
can reduce the risk of PPH by more than 40%
–The routine prophylaxis with oxytocics results in a reduced
need to use these drugs therapeutically
–Management of the third stage of labour should therefore
include the administration of oxytocin after the delivery of
the anterior shoulder.
•UTEROTONIC DRUGS
–Routine oxytocic administration in the third stage of labour
can reduce the risk of PPH by more than 40%
–The routine prophylaxis with oxytocics results in a reduced
need to use these drugs therapeutically
–Management of the third stage of labour should therefore
include the administration of oxytocin after the delivery of
the anterior shoulder.
Intranatal:
• Hasty delivery of the baby is to be avoided.
• Adequate amount of blood should be cross matched and
available when haemorrhage is anticipated.
• Coagulation studies are done in cases of Abruptio
placenta and retained dead fetus.
• Hasty delivery of the baby is to be avoided.
• Adequate amount of blood should be cross matched and
available when haemorrhage is anticipated.
• Coagulation studies are done in cases of Abruptio
placenta and retained dead fetus.
ActiveManagementof3rdStageofLabour:
1.UterotonicAgents:
•10 units of oxytocin IM or
•Syntometrine (5 unitsofoxytocinand0.5mg
ergonovine maleate).
•Misoprostol, a prostaglandin E1analogue, 600g
orally.
2.Earlycordclamping
3.Controlledcordtraction.
1.UterotonicAgents:
•10 units of oxytocin IM or
•Syntometrine (5 unitsofoxytocinand0.5mg
ergonovine maleate).
•Misoprostol, a prostaglandin E1analogue, 600g
orally.
2.Earlycordclamping
3.Controlledcordtraction.
MANAGEMENT OF PPH
•Early recognition of PPH is a very important factor in
management.
•An established plan of action for the management of
PPH is of great value when the preventative
measures have failed.
•Lab:
-CBC / BG / Cross match of 4-6 units of blood
-KFT / Coagulation profile
-Give FFP / cryoprecipitate if coagulation test results are abnormal
-Give platelet concentrates if the platelet count is < 50 X 109/L & bleeding continues
•Early recognition of PPH is a very important factor in
management.
•An established plan of action for the management of
PPH is of great value when the preventative
measures have failed.
•Lab:
-CBC / BG / Cross match of 4-6 units of blood
-KFT / Coagulation profile
-Give FFP / cryoprecipitate if coagulation test results are abnormal
-Give platelet concentrates if the platelet count is < 50 X 109/L & bleeding continues
MANAGEMENT OF PPH
MANAGEMENT OF PPH
DRUG THERAPY FOR PPH
MANAGEMENT OF PPH
MANAGEMENT OF PPH
MANAGEMENT OF PPH
Evaluation of response
-Monitor pulse, blood pressure, blood gas status, &
acid-base status +monitoring central venous pressure.
-Measure urine output using an indwelling catheter
-Order regular FBC counts and coagulation tests to
guide blood component therapy
-Monitor pulse, blood pressure, blood gas status, &
acid-base status +monitoring central venous pressure.
-Measure urine output using an indwelling catheter
-Order regular FBC counts and coagulation tests to
guide blood component therapy
Summary: remember 4 Ts
•“TONE”
•Rule out Uterine Atony
•Palpate fundus.
•Massage uterus.
•Oxytocin
•Methergine
•Hemabate
•“TONE”
•Rule out Uterine Atony
•Palpate fundus.
•Massage uterus.
•Oxytocin
•Methergine
•Hemabate
Summary: remember 4 Ts
•“Tissue”
•R/O retained placenta
•Inspect placenta for
missing cotyledons.
•Explore uterus.
•Treat abnormal
implantation.
•“Tissue”
•R/O retained placenta
•Inspect placenta for
missing cotyledons.
•Explore uterus.
•Treat abnormal
implantation.
Summary: remember 4 Ts
•“TRAUMA”
•R/O cervical or vaginal
lacerations.
•Obtain good exposure.
•Inspect cervix and
vagina.
•Worry about slow
bleeders.
•Treat haematomas.
•“TRAUMA”
•R/O cervical or vaginal
lacerations.
•Obtain good exposure.
•Inspect cervix and
vagina.
•Worry about slow
bleeders.
•Treat haematomas.
Summary: remember 4 Ts
•“THROMBIN” •Check labs if suspicious.
•“THROMBIN” •Check labs if suspicious.
Thank you..
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