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HELLP Syndrome as a
separate entity
Dr. Mohammed Abdalla
EGYPT, Domiat G. Hospital
HELLP Syndrome
may it be a separate
entity?
yes
HELLP, a syndrome characterized by
hemolysis, elevated liver enzyme
levels and a low platelet count, is an
obstetric complication that is frequently
misdiagnosed at initial presentation. Many
investigators consider the syndrome to be
a variant of preeclampsia,
but it may be a separate entity.
In some cases , HELLP symptoms are
the first warning of preeclampsia and
the condition is misdiagnosed as
hepatitis, idiopathic thrombocytopenic
purpura, gallbladder disease, or thrombotic
thrombocytopenic purpura.
Epidemiology and Risk Factors
 HELLP syndrome 0.2 to 0.6 % of all pregnancies.
 Preeclampsia 5 to 7 % of all pregnancies.
Superimposed HELLP syndrome develops in 4 to 12
percent of women with preeclampsia or eclampsia.
Wolf JL. Liver disease in pregnancy. Med Clin North Am 1996.
Maternal mortality has been estimated to be as high as 2-
24%
Perinatal mortality is equally high, ranging from 9 –39 %.
 The hemolysis in HELLP syndrome is a
microangiopathic hemolytic anemia. Red
blood cells become fragmented as they pass
through small blood vessels with endothelial
damage and fibrin deposits.
 The peripheral smear may reveal spherocytes,
schistocytes, triangular cells and burr cells.
 increase in Bilirubin and lactic
dehydrogenase levels.
Etiology and Pathogenesis
 The elevated liver enzyme levels in
the syndrome are thought to be
secondary to obstruction of hepatic
blood flow by fibrin deposits in the
sinusoids. This obstruction leads to
periportal necrosis and, in severe cases,
intrahepatic hemorrhage, subcapsular
hematoma formation or hepatic rupture.
Etiology and Pathogenesis
 The thrombocytopenia has been
attributed to increased consumption
and/or destruction of platelets.
With platelet activation, thromboxane A and
serotonin are released, causing vasospasm,
platelet agglutination and aggregation, and further
endothelial damage.
Etiology and Pathogenesis
Clinical Presentation
 90%of patients present with generalized
malaise,
 65 % with epigastric pain,
 30 % with nausea and vomiting,
 31 percent with headache.
All are nonspecific symptoms
Because of the variable nature
of the clinical presentation,
the diagnosis of HELLP
syndrome is generally delayed
for an average of eight days.
Usually presented by complications
In one retrospective chart
review of patients with
HELLP syndrome, only
two of 14 patients entered
the hospital with the
correct diagnosis.
Because early diagnosis of this
syndrome is critical, any
pregnant woman who presents
with malaise or a viral-type
illness in the third trimester
should be evaluated with a
complete blood cell count and
liver function tests.
Clinical Presentation
The physical examination may be normal in patients
with HELLP syndrome.
1- right upper quadrant tenderness 90 %
2- Edema is not a useful marker
3- Hypertension and proteinuria may be
absent or mild.
90
65
30 31
0
10
20
30
40
50
60
70
80
90
symptoms
general malase
epigastric pain
vomiting
haedache
Clinical Presentation
SYMPTOMS
90
30 30
0
10
20
30
40
50
60
70
80
90
signs
Rt.hypochond.pain
edema
hypertention + proteinuria
signs
Clinical Presentation
Diagnosis
Martin JN Jr, Rinehart BK, May WL, Magann EF, Terrone DA,
Blake PG.
 There is agreement among most of the
authors that, the diagnosis requires the
concurrence of hemolysis, elevated liver
enzymes, and low platelet count. However,
there is obviously still a lack of consensus
on the laboratory parameters and their cutoff
values used to diagnose
Laboratory Diagnostic Criteria for
HELLP syndrome
Haemolysis
Abnormal peripheral smear : spherocytes, schistocytes,
triangular cells and burr cells
Total Bilirubin level > 1.2 mg/dL
Lactate dehydrogenase level > 600U/L
Elevated liver function test result
Serum aspartate amino transferase level > 70U/L
Lactate dehydrogenase level >600 U/L
Low platelet count
Platelet count < 150 000/mm3
Platelet count
appears to be the
most reliable
indicator of the
presence of HELLP
syndrome
Clinical utility of strict diagnostic
criteria for the HELLP
the use of strict diagnostic criteria in
the definition of the HELLP
syndrome allows for greater
prediction of complication rates.
and define the cases that are
Eligible to conservative management
Classification
full HELLP
syndrome
partial HELLP
syndrome
based on the number of
abnormalities
Audibert F, Friedman SA, Frangieh AY, Sibai BM. Am J Obstet Gynecol 1996;
175:460-4.
considered
for delivery
within 48
hours
candidates
for more
conservative
management
Classification
on the basis of platelet
count
class I, less than 50,000 per mm3
class II, 50,000 to less than 100,000 per mm3
class III, 100,000 to 150,000 per mm3
Management
Corticosteroids
Magnesium sulphate
Hypotensive drugs
Blood products
Delivery
The treatment approach should be based on the
estimated gestational age and the condition of
the mother and fetus.
Prolongation of pregnancy, in theory, may be
favourable for the foetus whereas it remains
controversial whether maternal condition is
further deteriorated by expectant management
Visser W, Wallenburg HC. Temporising management
of severe pre-eclampsia with and without the HELLP
syndrome. Br J Obstet Gynaecol 1995;102:111-7
hypertension is controlled at less than
160/110 mm hg,
Oliguria responds to fluid management .
Elevated liver function values are not
associated with right upper quadrant or
epigastric pain.
Class II –III .(platelet count).>50000
Eligibility to conservative
management
The Cochrane Library holds two
protocols which when complete
may summarize evidence to date on
the use of corticosteroids for
HELLP syndrome . and
interventionist versus expectant
management of severe pre-
eclampsia before term.
The antenatal administration of dexamethasone (Decadron) in a
high dosage of 10 mg intravenously every 12 hours has been
shown to markedly improve the laboratory abnormalities associated
with HELLP syndrome.
Steroids given antenatally do not prevent the typical
worsening of laboratory abnormalities after delivery.
However, laboratory abnormalities resolve more
quickly in patients who continue to receive steroids
postpartum.
Magann EF, Bass D, Chauhan SP, Sullivan DL, Martin RW, Martin JN Jr. Am
J Obstet Gynecol 1994;171:1148-53.
 Corticosteroid therapy should be
instituted in patients with HELLP
syndrome who have a platelet count of
less than 100,000 per mm3 .And should
be continued until liver function
abnormalities are resolving and the
platelet count is greater than 100,000 per
mm3
Magann EF, Perry KG Jr, Meydrech EF, Harris RL, Chauhan
SP, Martin JN Jr. Am J Obstet Gynecol 1994;171:1154-8.
Intravenously administered
dexamethasone appears to be more
effective than intramuscularly
adminstered betamethasone for the
antepartum treatment of mothers with
HELLP syndrome.
(Am J Obstet Gynecol 2001;184:1332-9.).
Administration of glucocorticoids increases
the use of regional anesthesia in women
with antepartum HELLP syndrome who
have thrombocytopenia.
(Am J Obstet Gynecol 2002;186:475-9.).
Patients treated with
dexamethasone exhibit longer time
to delivery; This facilitates maternal
transfer to a tertiary care center and
postnatal maturity of fetal lungs
(Am J Obstet Gynecol 2002;186:475-9.).
Patients with HELLP
syndrome should be
treated prophylactically
with magnesium sulfate
to prevent seizures,
whether hypertension is
present or not.
Antihypertensive therapy
should be initiated if blood pressure
is consistently greater than 160/110
mm hg despite the use of
magnesium sulfate. The goal is to
maintain diastolic blood pressure
between 90 and 100 mm hg.
The most commonly used
antihypertensive agent has been
hydralazine
Labetolol
Nifedipine
Between 38 -93 % of patients with
HELLP syndrome receive some
form of blood product.
 Patients with a platelet count
greater than 40,000 per mm3 are
unlikely to bleed.
Patients who undergo cesarean section
should be transfused if their platelet count
is less than 50,000 per mm3 ,
Prophylactic transfusion of platelets at
delivery does not reduce the incidence of
postpartum hemorrhage or hasten
normalization of the platelet count. .
Patients with DIC should be given fresh
frozen plasma and packed red blood cells.
Pain relief with intravenous narcotics
and local anesthesia is acceptable but
certainly not optimal for pain control.
Epidural anesthesia has been
controversial but it is the technique of
choice when it can be accomplished
safely. Insertion of an epidural catheter is
generally safe in patients with a platelet
count greater than 100,000 per mm3.
 General anesthesia can be used when
regional anesthesia is considered unsafe.
Portis R, Jacobs MA, Skerman JH, Skerman EB. HELLP syndrome (hemolysis, elevated
liver enzymes, and low platelets) pathophysiology and anesthetic considerations. AANA
J 1997;65:37-47.
Complications
Complications
The mortality rate for women with HELLP
syndrome is approximately 1.1 %
 From 1 to 25 % of affected women develop
serious complications such as DIC, placental
abruption, adult respiratory distress syndrome,
hepatorenal failure, pulmonary edema,
subcapsular hematoma and hepatic rupture.
 A significant percentage of patients receive
blood products.
Sibai BM, Ramadan MK, Usta I, Salama M, Mercer BM, Friedman SA. Maternal
morbidity and mortality in 442 pregnancies with hemolysis, elevated liver enzymes,
and low platelets (HELLP syndrome). Am J Obstet Gynecol 1993;169:1000-6.
Infant morbidity and mortality rates range
from 10 to 60 %, depending on the severity of
maternal disease.
 Infants affected by HELLP syndrome are
more likely to experience intrauterine growth
retardation and respiratory distress
syndrome.
Dotsch J, Hohmann M, Kuhl PG. Neonatal morbidity and mortality
associated with maternal haemolysis, elevated liver enzymes and low
platelets syndrome. Eur J Pediatr 1997;156:389-91.
Complications
1.10%
25%
60%
0.00%
10.00%
20.00%
30.00%
40.00%
50.00%
60.00%
matern.mort. maternal
complication
fetal
complication
Complications
take home
Once the diagnosis of HELLP
syndrome has been established, the
best markers to follow are the
maternal lactate dehydrogenase
level and
the maternal platelet count
The laboratory abnormalities in
HELLP syndrome typically
worsen after delivery and then
begin to resolve by three to four
days postpartum.
Martin JN Jr, Blake PG, Perry KG Jr, McCaul JF, Hess LW, Martin RW.
The natural history of HELLP syndrome: patterns of disease progression
and regression. Am J Obstet Gynecol 1991;164(6 pt 1):1500-9.
take home
The incidence of hemorrhagic
complications is higher when
platelet counts are < 40,000
per mm3
take home
Patients with HELLP syndrome who
complain of severe right upper
quadrant pain, neck pain or shoulder
pain should be considered for hepatic
imaging regardless of the severity of
the laboratory abnormalities, to assess
for subcapsular haematoma or rupture
take home
Patients with HELLP
syndrome should be
routinely treated with
corticosteroids.
take home
HELLP syndrome

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HELLP syndrome

  • 1. HELLP Syndrome as a separate entity Dr. Mohammed Abdalla EGYPT, Domiat G. Hospital
  • 2. HELLP Syndrome may it be a separate entity? yes
  • 3. HELLP, a syndrome characterized by hemolysis, elevated liver enzyme levels and a low platelet count, is an obstetric complication that is frequently misdiagnosed at initial presentation. Many investigators consider the syndrome to be a variant of preeclampsia, but it may be a separate entity.
  • 4. In some cases , HELLP symptoms are the first warning of preeclampsia and the condition is misdiagnosed as hepatitis, idiopathic thrombocytopenic purpura, gallbladder disease, or thrombotic thrombocytopenic purpura.
  • 5. Epidemiology and Risk Factors  HELLP syndrome 0.2 to 0.6 % of all pregnancies.  Preeclampsia 5 to 7 % of all pregnancies. Superimposed HELLP syndrome develops in 4 to 12 percent of women with preeclampsia or eclampsia. Wolf JL. Liver disease in pregnancy. Med Clin North Am 1996. Maternal mortality has been estimated to be as high as 2- 24% Perinatal mortality is equally high, ranging from 9 –39 %.
  • 6.  The hemolysis in HELLP syndrome is a microangiopathic hemolytic anemia. Red blood cells become fragmented as they pass through small blood vessels with endothelial damage and fibrin deposits.  The peripheral smear may reveal spherocytes, schistocytes, triangular cells and burr cells.  increase in Bilirubin and lactic dehydrogenase levels. Etiology and Pathogenesis
  • 7.  The elevated liver enzyme levels in the syndrome are thought to be secondary to obstruction of hepatic blood flow by fibrin deposits in the sinusoids. This obstruction leads to periportal necrosis and, in severe cases, intrahepatic hemorrhage, subcapsular hematoma formation or hepatic rupture. Etiology and Pathogenesis
  • 8.  The thrombocytopenia has been attributed to increased consumption and/or destruction of platelets. With platelet activation, thromboxane A and serotonin are released, causing vasospasm, platelet agglutination and aggregation, and further endothelial damage. Etiology and Pathogenesis
  • 9. Clinical Presentation  90%of patients present with generalized malaise,  65 % with epigastric pain,  30 % with nausea and vomiting,  31 percent with headache. All are nonspecific symptoms
  • 10. Because of the variable nature of the clinical presentation, the diagnosis of HELLP syndrome is generally delayed for an average of eight days. Usually presented by complications
  • 11. In one retrospective chart review of patients with HELLP syndrome, only two of 14 patients entered the hospital with the correct diagnosis.
  • 12. Because early diagnosis of this syndrome is critical, any pregnant woman who presents with malaise or a viral-type illness in the third trimester should be evaluated with a complete blood cell count and liver function tests.
  • 13. Clinical Presentation The physical examination may be normal in patients with HELLP syndrome. 1- right upper quadrant tenderness 90 % 2- Edema is not a useful marker 3- Hypertension and proteinuria may be absent or mild.
  • 14. 90 65 30 31 0 10 20 30 40 50 60 70 80 90 symptoms general malase epigastric pain vomiting haedache Clinical Presentation SYMPTOMS
  • 16. Diagnosis Martin JN Jr, Rinehart BK, May WL, Magann EF, Terrone DA, Blake PG.  There is agreement among most of the authors that, the diagnosis requires the concurrence of hemolysis, elevated liver enzymes, and low platelet count. However, there is obviously still a lack of consensus on the laboratory parameters and their cutoff values used to diagnose
  • 17. Laboratory Diagnostic Criteria for HELLP syndrome Haemolysis Abnormal peripheral smear : spherocytes, schistocytes, triangular cells and burr cells Total Bilirubin level > 1.2 mg/dL Lactate dehydrogenase level > 600U/L Elevated liver function test result Serum aspartate amino transferase level > 70U/L Lactate dehydrogenase level >600 U/L Low platelet count Platelet count < 150 000/mm3
  • 18. Platelet count appears to be the most reliable indicator of the presence of HELLP syndrome
  • 19. Clinical utility of strict diagnostic criteria for the HELLP the use of strict diagnostic criteria in the definition of the HELLP syndrome allows for greater prediction of complication rates. and define the cases that are Eligible to conservative management
  • 20. Classification full HELLP syndrome partial HELLP syndrome based on the number of abnormalities Audibert F, Friedman SA, Frangieh AY, Sibai BM. Am J Obstet Gynecol 1996; 175:460-4. considered for delivery within 48 hours candidates for more conservative management
  • 21. Classification on the basis of platelet count class I, less than 50,000 per mm3 class II, 50,000 to less than 100,000 per mm3 class III, 100,000 to 150,000 per mm3
  • 23. The treatment approach should be based on the estimated gestational age and the condition of the mother and fetus. Prolongation of pregnancy, in theory, may be favourable for the foetus whereas it remains controversial whether maternal condition is further deteriorated by expectant management Visser W, Wallenburg HC. Temporising management of severe pre-eclampsia with and without the HELLP syndrome. Br J Obstet Gynaecol 1995;102:111-7
  • 24. hypertension is controlled at less than 160/110 mm hg, Oliguria responds to fluid management . Elevated liver function values are not associated with right upper quadrant or epigastric pain. Class II –III .(platelet count).>50000 Eligibility to conservative management
  • 25.
  • 26. The Cochrane Library holds two protocols which when complete may summarize evidence to date on the use of corticosteroids for HELLP syndrome . and interventionist versus expectant management of severe pre- eclampsia before term.
  • 27. The antenatal administration of dexamethasone (Decadron) in a high dosage of 10 mg intravenously every 12 hours has been shown to markedly improve the laboratory abnormalities associated with HELLP syndrome. Steroids given antenatally do not prevent the typical worsening of laboratory abnormalities after delivery. However, laboratory abnormalities resolve more quickly in patients who continue to receive steroids postpartum. Magann EF, Bass D, Chauhan SP, Sullivan DL, Martin RW, Martin JN Jr. Am J Obstet Gynecol 1994;171:1148-53.
  • 28.  Corticosteroid therapy should be instituted in patients with HELLP syndrome who have a platelet count of less than 100,000 per mm3 .And should be continued until liver function abnormalities are resolving and the platelet count is greater than 100,000 per mm3 Magann EF, Perry KG Jr, Meydrech EF, Harris RL, Chauhan SP, Martin JN Jr. Am J Obstet Gynecol 1994;171:1154-8.
  • 29. Intravenously administered dexamethasone appears to be more effective than intramuscularly adminstered betamethasone for the antepartum treatment of mothers with HELLP syndrome. (Am J Obstet Gynecol 2001;184:1332-9.).
  • 30. Administration of glucocorticoids increases the use of regional anesthesia in women with antepartum HELLP syndrome who have thrombocytopenia. (Am J Obstet Gynecol 2002;186:475-9.).
  • 31. Patients treated with dexamethasone exhibit longer time to delivery; This facilitates maternal transfer to a tertiary care center and postnatal maturity of fetal lungs (Am J Obstet Gynecol 2002;186:475-9.).
  • 32.
  • 33. Patients with HELLP syndrome should be treated prophylactically with magnesium sulfate to prevent seizures, whether hypertension is present or not.
  • 34.
  • 35. Antihypertensive therapy should be initiated if blood pressure is consistently greater than 160/110 mm hg despite the use of magnesium sulfate. The goal is to maintain diastolic blood pressure between 90 and 100 mm hg.
  • 36. The most commonly used antihypertensive agent has been hydralazine Labetolol Nifedipine
  • 37.
  • 38. Between 38 -93 % of patients with HELLP syndrome receive some form of blood product.  Patients with a platelet count greater than 40,000 per mm3 are unlikely to bleed.
  • 39. Patients who undergo cesarean section should be transfused if their platelet count is less than 50,000 per mm3 , Prophylactic transfusion of platelets at delivery does not reduce the incidence of postpartum hemorrhage or hasten normalization of the platelet count. . Patients with DIC should be given fresh frozen plasma and packed red blood cells.
  • 40.
  • 41. Pain relief with intravenous narcotics and local anesthesia is acceptable but certainly not optimal for pain control. Epidural anesthesia has been controversial but it is the technique of choice when it can be accomplished safely. Insertion of an epidural catheter is generally safe in patients with a platelet count greater than 100,000 per mm3.  General anesthesia can be used when regional anesthesia is considered unsafe. Portis R, Jacobs MA, Skerman JH, Skerman EB. HELLP syndrome (hemolysis, elevated liver enzymes, and low platelets) pathophysiology and anesthetic considerations. AANA J 1997;65:37-47.
  • 43. Complications The mortality rate for women with HELLP syndrome is approximately 1.1 %  From 1 to 25 % of affected women develop serious complications such as DIC, placental abruption, adult respiratory distress syndrome, hepatorenal failure, pulmonary edema, subcapsular hematoma and hepatic rupture.  A significant percentage of patients receive blood products. Sibai BM, Ramadan MK, Usta I, Salama M, Mercer BM, Friedman SA. Maternal morbidity and mortality in 442 pregnancies with hemolysis, elevated liver enzymes, and low platelets (HELLP syndrome). Am J Obstet Gynecol 1993;169:1000-6.
  • 44. Infant morbidity and mortality rates range from 10 to 60 %, depending on the severity of maternal disease.  Infants affected by HELLP syndrome are more likely to experience intrauterine growth retardation and respiratory distress syndrome. Dotsch J, Hohmann M, Kuhl PG. Neonatal morbidity and mortality associated with maternal haemolysis, elevated liver enzymes and low platelets syndrome. Eur J Pediatr 1997;156:389-91. Complications
  • 46. take home Once the diagnosis of HELLP syndrome has been established, the best markers to follow are the maternal lactate dehydrogenase level and the maternal platelet count
  • 47. The laboratory abnormalities in HELLP syndrome typically worsen after delivery and then begin to resolve by three to four days postpartum. Martin JN Jr, Blake PG, Perry KG Jr, McCaul JF, Hess LW, Martin RW. The natural history of HELLP syndrome: patterns of disease progression and regression. Am J Obstet Gynecol 1991;164(6 pt 1):1500-9. take home
  • 48. The incidence of hemorrhagic complications is higher when platelet counts are < 40,000 per mm3 take home
  • 49. Patients with HELLP syndrome who complain of severe right upper quadrant pain, neck pain or shoulder pain should be considered for hepatic imaging regardless of the severity of the laboratory abnormalities, to assess for subcapsular haematoma or rupture take home
  • 50. Patients with HELLP syndrome should be routinely treated with corticosteroids. take home