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HYPERTENSIVE
DISORDER
IN PREGNANCY
PRESENTED BY :
FATIN RAIHANA BINTI MOHD AZHA
SUPERVISED BY:
DR KEMBANG AZIAH
CME
DEPARTMENT OF OBSTETRICS AND GYNECOLOGY
HOSPITAL ENCHE BESAR HAJJAH KHALSOM
Irfan Nadim Anuar
Hypertensive disorders in pregnancy remains a common cause of direct maternal death
worldwide. The mortality is related to intracranial hemorrhage from poorly controlled
hypertension. Furthermore, pre-eclampsia is frequently accompanied by FGR, which is
associated with perinatal morbidity and mortality.
In Malaysia, it is the third most common cause of death (Confidential Enquiry into Maternal
Deaths; CEMD 2019)
Goals:
o To ensure optimal treatment of preeclampsia
o To attain clinical judgemet in prolonging the pregnancy long enough for fetal
maturity while preventing complications from preeclampsia
o To effectively prevent and manage eclampsia
Source: Confidential Enquiries into
Maternal Deaths 2019
Source: CPG Management of Hypertension 5th Edition
DEFINITION
Hypertension in pregnancy SBP ≥140 mmHg and/or DBP ≥90mmHg
Proteinuria
* reflects advanced disease and is
associated with poorer prognosis
≥300mg protein in 24H urine sample, or a spot urine protein-creatinine
ratio ≥30mg/mmol, or urine dipstick ≥2+ (approximated ≥300mg/day proteinuria)
20 weeks
gestation
3 months
postpartum
Gestational Hypertension
Chronic Hypertension
Preeclampsia
+ proteinuria
de novo
superimposed
on chronic HPT
Eclampsia
+ fits
Source: International Society for the Study of
Hypertension in Pregnancy (ISSHP)
CLASSIFICATION OF HPT IN PREGNANCY
Gestational HPT
HPT detected after 20wks gestation
25% can progress into PE, more so if present before 34 weeks
Chronic HPT
• HPT diagnosed prior to 20wks gestation
• HPT during preconception
• De novo HPT in late gestation that fails to resolve 3 months
postpartum
Isolated office
hypertension
Elevated BP of 140/90 mmHg only in the clinic with normal BP
demonstrated by ambulatory BP monitoring (ABPM) either awake or
during sleep
Women in this group should not be considered low risk as they may progress to
gestational hypertension (50%) or PE (8%)
Source: International Society for the Study of
Hypertension in Pregnancy (ISSHP)
CLASSIFICATION OF HPT IN PREGNANCY
Preeclampsia (PE) ≥1 of the following:
De Novo
• Significant proteinuria
• Renal insufficiency: Cr≥90 or oliguria
• Liver disease: raised AST/ALT +/- severe RUQ pain/epigastric pain
• CNS problems: convulsions (eclampsia), hyperreflexia with clonus or
severe headaches, persistant visual disturbances (scotoma)
• Haematological problems: thrombocytopenia, coagulopathy,
haemolysis
• Fetal growth restriction
* followed by normalisation of BP by 3 months postpartum
Superimposed on Chronic
HPT
• De novo proteinuria after 20 weeks
• Worsening proteinuria in pre-existing proteinuria
• A sudden increase in the severity of HPT
• Appearance of features of PE
In cases of PIH/
Pre-eclampsia
In normal pregnancies
PATHOPHYSIOLOGY OF PREECLAMPSIA
• Maternal blood flow to placenta increases
from 50ml/min in the 1st trimester to 500-
750ml/min at term
• Achieved by anatomical convesion of the
maternal spiral arteries by trophoblast
• Trophoblast cells invade the spiral arteries
within 12 weeks of pregnancy and replace
the smooth muscle of the wall, converting
them to wide bore, low resistance, large
capacitance vessels.
• This process is normally complete by 20 wks
• Complete or partial failure of
throphoblastic invasion
• Retain pre-pregnancy characteristics:
relatively narrow bore, high resistance and
low capacitance
• Results in impaired perfusion of the
fetoplacental unit
• Hypoperfused placenta releases circulating
factor(s) wich causes vascular endothelial
cell activation, affecting multiple organ
systems
a) The maternal surface shows an ill-
defined area (arrows) which coincided
with the infarction hematoma.
b) Cut sections of the placenta show a
large round hemorrhagic lesion
surrounded by infarcted placental
tissues.
These lesions are significantly
associated with intrauterine fetal
death and growth restriction
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
1. Preconception counseling and adjustment of treatment in women with chronic hypertension
Change in anti-hypertensives. Drugs of choice are Methyldopa and Labetolol.
Anti-HPT drugs contraindicated in pregancy:
• Atenolol → FGR
• ARBs, ACEIs and thiazide diuretics → Foetal anomaly
Women in reproductive age on the abovementioned drugs must be on effective contraception
The treatment of HPT in pregnancy is solely for maternal safety particularly the prevention of ICB.
It does NOT reduce the risk of development of preeclampsia or perinatal mortality, nor improve fetal growth.
Contraindicated
in asthma
Source: CPG Management of Hypertension 5th Edition
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
2. Recognition of women risk of preeclampsia for commencement of prophylaxis
Moderate Risk High Risk
•Primigravida
•Age >40 years
•Pregnancy interval >10 years
•BMI of >35kg/m2 at first visit
•Family history of PE
•Multiple pregnancy
•Hypertensive disease during previous
pregnancy
•Chronic kidney disease
•Autoimmune disease such as Systemic Lupus
Erythematosus (SLE) or anti- phospholipid
syndrome(APS)
•Type 1 or type 2 diabetes mellitus, and
chronic hypertension.
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
Risk factors based on PREDO study:
Cluster analysis to estimate the risk of preeclampsia in the high-risk Prediction and Prevention of
Preeclampsia and Intrauterine Growth Restriction (PREDO) study
The risk of preeclampsia increases exponentially with respect to the number of risk factors.
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
3. Prophylactic therapy
a. Aspirin
Women with ≥2 moderate or >1 high risk factor should be started on low dose aspirin from 12 weeks up to
16 weeks of gestation until delivery. Dosage should be 100-150mg and taken ON in order to significantly
reduce the incidence of PE
b. Calcium
Low dose calcium supplement (generally 500-1000mg daily) commenced before 20 weeks gestation
reduces the r isk of PE
There is no proven role of vitamin D, nor other supplememnts in reducing the risk of PE. Combined
vitamin C and E should be avoided because they significantly increase the incidence of low birth weight
without anu prevention effect against PE.
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
Studies on Aspirin:
CLASP trial: a randomised trial of low-dose aspirin for the prevention and treatment of pre-
eclampsia among 9364 pregnant women CLASP (Collaborative Low-dose Aspirin Study in
Pregnancy) Collaborative, published in March 1994
Overall, the use of low dose aspirin (60mg daily) was associated with a reduction of only 12% in the
incidence of proteinuric preeclampsia, which was not significant. Nor was there any significant effect on
the incidence of IUGR or of stillbirth and neonatal death. Aspirin did, however, significantly reduce the
likelihood of preterm delivery (19.7% aspirin vs 22.2% control; absolute reduction of 2.5 [SD 0.9] per
100 women treated; 2p = 0.003). There was a significant trend (p = 0.004) towards progressively
greater reductions in proteinuric pre‐ eclampsia the more preterm the delivery.
ASPRE trial: performance of screening for preterm pre-eclampsia, published July 2017
The ASPRE trial demonstrated that, in women with singleton pregnancy who were identified by means
of first-trimester combined screening as being at high risk for preterm PE, the administration of aspirin
at a dose of 150 mg per day from 11–14 weeks until 36 weeks' gestation reduces the incidence of
preterm PE by > 60%
ROLE OF PRIMARY CARE
Source: CPG Management of Hypertension 5th Edition
4. Fetal anomaly screening
Women with chronic HPT have about 20-30% increased risk for fetal congenital cardiac anomaly. They
should be referred to Maternal-Fetal Medicine (MFM) specialist in the tertiary centre for nuchal
translucency (NT) scan at 12-14wks followed by detailed scan at 22-24wks of gestation. If a cardiac
abnomaliy is detected, cardiology referral is recommended.
5. Prevention of eclampsia and other complications of PE
Education on the signs and symptoms of preeclampsia for early diagnosis and referral for further
management may prevent progression into eclampsia
SEVERE PRECLAMPSIA
Source: CPG Management of Hypertension 5th Edition
Definition: (acc to the American College of Obstetricians and Gynaecologists)
a. SBP ≥160/ DBP ≥110 mmHg on two occasons at least 4 hrs apart while resting
b. Thrombocytopenia - Plt count <100
c. Abnormal liver enzymes (elevated AST/ALT), severe persistant RUQ/epigastric pain
unresponsive to treament
d. Pulmonary oedema
e. New onset of cerebral or visual disturbances
Principle of management include:
1) Control of BP (mangement of acute hypertensive crisis:
• IV Hydralazine, IV Labetolol or oral Nifedipine may be used to lower the BP.
• BP should be reduced within 30-60 minutes to reduce the risk of maternal stroke
• Diuretics are generally contraindicated as it reduces plasma volume → IUGR and may
increase perinatal mortality. Only used in the treatment of acute pulmonary oedema
2) Monitoring of maternal or fetal complications
3) Seizure prophylaxis
4) Timely delivery
IV Labetolol Protocol
IV Labetolol 10mg STAT (2cc-PURE) over 1
minute and repeat at 5 minute intervals
(max dose: 200mg (40cc)
Infusion syringe pump:
200mg IV Labetolol (40cc) in 50cc syringe and
start at 4cc/hr, and increase by 4cc at 30 minutes.
Stop infusion if rate exceeds 150mg/hr (30cc/hr)
and inform specialist
1 vial = 5cc = 25mg
Effective dose: 20-150mg/hr (4-30cc/hr)
IV Hydralazine Protocol
Loading dose:
• Start at 4cc/hr for 5 mins
• To check BP after 5 mins
• Then cont with maintenance dose
Maintenance dose:
• 1cc/hr
• check BP after 15 min
• icrease by 1cc/hr every 30 mins to titrate till DBP
100mmHg
• Maintain IV Hydralazine once DBP 90-100mmHg
• Titrate down once DBP <90mmHg
1 vial = 5cc = 20mg
Maximum dose: 10cc/hr
Dilution: 5cc Hydralazine + 20cc NS
Antidote: IV Atropine 600mcg (bolus)
IV MgSO4 is the drug of choice for prevention of eclampsia and to abort an eclamptic fit.
It also provides fetal neuroprotection following the preterm birth with a significant reduction in the
incidence of cerebral palsy.
Alternative is IV Diazepam but it is inferior in
efficacy.
1. Start MgSO4, and continue for 24 hrs
following delivery or initiation
(whichever comes later).
2. Consider delivery once decision for
MgSO4 has been made.
Anticonvulsants in PE and Eclampsia
Source: Handbook of Obstetric Emergencies
by Dr Gunasegaran Rajan
IV MgSO4 Protocol
1) The Loading Dose
IV MgSO4 4g Slow Bolus
Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan
8cc MgSO4 + 12cc NS in 20cc syringe
run on IV infusion pump 80cc/hr to infuse
20cc in 15 mins
In case of eclampsia;
If fit persist >15minutes, add 2g MgSO4
4cc MgSO4 + 16cc NS in 20cc syringe
(infused at 80cc/hr)
Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan
IV MgSO4 Protocol
2) The Maintainence Dose
IV MgSO4 1g/hr
2cc MgSO4 + 48cc NS in 50cc syringe
run on IV infusion pump 50cc/hr for 24 hrs after the last fit or 24 hrs after delivery, whichever
comes later
MgSO4 Toxicity
1. Monitoring toxicity (hourly)
• ECG - prolonged PR interval, wide QRS complex
• Deep tendon reflexes must be present
• Urine output >30ml/hr (0.5cc/kg/hr)
• RR between 12 to 16/minute
• SPO2 >95%
• GCS E4V5M6
Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan
2. Antidote
1g Calcium Gluconate (10cc of 10% solution) given slow IV bolus over 10 minutes
Source: NICE guidelines 2020 hypertension in pregnancy and management
Fetal assessment
• Offer fetal heart auscultation at every antenatal appointment
• Carry out USG assessment of the fetus at diagnosis and, if normal, repeat every 2 weekly
• Carry out CTG at diagnosis and then only if clinically indicated; reduced FM/ PV bleed/
abdominal pain/ deterioration of maternal indication
Example of Umilical Artery Doppler Wave Forms
A) Normal umbilical artery Doppler flow waveform
B) Absent
C) Reversed end-diastolic Doppler flow in umbilical artery
USG assessment 2 weekly for non-PE women with previous:
• Severe PE
• PE requiring delivery <34 wks
• PE with SGA (<10th centile)
• IUD
• Placental abruptio
Source: NICE guidelines 2020 hypertension in pregnancy and management
Timing of birth
Weeks of
pregnancy
Timing of birth
<34 wks
Continue surveillance unless there are indications for planned early birth. Offer IV
MgSO4 and IV Dexamethasone as per guidelines on preterm labour and birth
34-36 wks
Continue surveillance unless there are indications for planned early birth.
When considering the option for planned early brith, take into account the woman/s
and baby’s condition, risk factors and availability of neonatal unit beds. Consider IV
Dexamethasone as per guidelines on preterm labour and birth
>37 wks Initiate birth within 24-48 hrs
Indications for planned early birth:
• Inability to control maternal BP, despite using ≥3 antiHPT in appropriate doses
• Maternal SPO2 <90%
• Progressive deterioration in liver function, rel function, hemolysis or platelet count
• Ongoing neurological features; intractable headache, repeated visual scotoma, eclampsia
• Placental abruptio
• Reversed end-diastolic flow in the umbilical artery doppler velocimetry, a non-reassuring
CTG, or stillbirth
ECLAMPSIA OBSTETRIC
EMERGENCY
ACTIVATE RED ALERT
Place patient in left lateral position (recovery position)
Secure airway
Administer oxygen
• Give MgSO4 as per protocol
• IV access x2
• Commence antiHPT as per protocol
• Cont IV MgSO4 infusion as per protocol
• Auscultate heart and lungs
• Palpate abdomen, reflexes, assess fetal
condition
• VE and catheterize after BP stablised
• Decide mode of delivery
• Refer to anaethesia for ICU management
Blood Ix: FBC, LFT, RP, uric acid, coag profile, GXM
7 Principles of Managing Eclampsia
POSTPARTUM CARE
Source: CPG Management of Hypertension 5th Edition
• Postpartum, BP should be regularly checked at local clinics
• The dose of antihypertensives should be tailed down gradually
• On average, anti-HPT agents are required for longer in womwith PE (~2wks) than those with
gestational hypertension (~1wk)
• Chronic HPT is diagnosed when HPT persists after 3 months postpartum.
LONG TERM FOLLOW-UP
• Evidence suggests 13% of women with PE will have underlying essential HPT that was not suspected
antenatally.
• There is increased risk of ischaemic heart disease, thrmboembolism and stroke following PE
• Long-term follow-up ot pts with a history of hypertension in pregnancy is advisable
Thank
you!
REFERENCES :
1. Clinical Practice Guidelines - Management of Hypertension (5th
Edition) 2018 MOH/P/PAK/391.18 (GU)
2. ISSHP guidelines in hypertension disorder in pregnancy
3. Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan,
Muniswaran Ganeshan, Tang Boon Nee, Thaneemalai
Jeganathan
4. Obstetrics by Ten Teachers 19th Edition
CME
DEPARTMENT OF OBSTETRICS AND GYNECOLOGY/ HEBHK

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CME Hypertension in Pregnancy.pdf

  • 1. HYPERTENSIVE DISORDER IN PREGNANCY PRESENTED BY : FATIN RAIHANA BINTI MOHD AZHA SUPERVISED BY: DR KEMBANG AZIAH CME DEPARTMENT OF OBSTETRICS AND GYNECOLOGY HOSPITAL ENCHE BESAR HAJJAH KHALSOM Irfan Nadim Anuar
  • 2. Hypertensive disorders in pregnancy remains a common cause of direct maternal death worldwide. The mortality is related to intracranial hemorrhage from poorly controlled hypertension. Furthermore, pre-eclampsia is frequently accompanied by FGR, which is associated with perinatal morbidity and mortality. In Malaysia, it is the third most common cause of death (Confidential Enquiry into Maternal Deaths; CEMD 2019) Goals: o To ensure optimal treatment of preeclampsia o To attain clinical judgemet in prolonging the pregnancy long enough for fetal maturity while preventing complications from preeclampsia o To effectively prevent and manage eclampsia
  • 3. Source: Confidential Enquiries into Maternal Deaths 2019
  • 4. Source: CPG Management of Hypertension 5th Edition DEFINITION Hypertension in pregnancy SBP ≥140 mmHg and/or DBP ≥90mmHg Proteinuria * reflects advanced disease and is associated with poorer prognosis ≥300mg protein in 24H urine sample, or a spot urine protein-creatinine ratio ≥30mg/mmol, or urine dipstick ≥2+ (approximated ≥300mg/day proteinuria) 20 weeks gestation 3 months postpartum Gestational Hypertension Chronic Hypertension Preeclampsia + proteinuria de novo superimposed on chronic HPT Eclampsia + fits
  • 5. Source: International Society for the Study of Hypertension in Pregnancy (ISSHP) CLASSIFICATION OF HPT IN PREGNANCY Gestational HPT HPT detected after 20wks gestation 25% can progress into PE, more so if present before 34 weeks Chronic HPT • HPT diagnosed prior to 20wks gestation • HPT during preconception • De novo HPT in late gestation that fails to resolve 3 months postpartum Isolated office hypertension Elevated BP of 140/90 mmHg only in the clinic with normal BP demonstrated by ambulatory BP monitoring (ABPM) either awake or during sleep Women in this group should not be considered low risk as they may progress to gestational hypertension (50%) or PE (8%)
  • 6. Source: International Society for the Study of Hypertension in Pregnancy (ISSHP) CLASSIFICATION OF HPT IN PREGNANCY Preeclampsia (PE) ≥1 of the following: De Novo • Significant proteinuria • Renal insufficiency: Cr≥90 or oliguria • Liver disease: raised AST/ALT +/- severe RUQ pain/epigastric pain • CNS problems: convulsions (eclampsia), hyperreflexia with clonus or severe headaches, persistant visual disturbances (scotoma) • Haematological problems: thrombocytopenia, coagulopathy, haemolysis • Fetal growth restriction * followed by normalisation of BP by 3 months postpartum Superimposed on Chronic HPT • De novo proteinuria after 20 weeks • Worsening proteinuria in pre-existing proteinuria • A sudden increase in the severity of HPT • Appearance of features of PE
  • 7. In cases of PIH/ Pre-eclampsia In normal pregnancies PATHOPHYSIOLOGY OF PREECLAMPSIA • Maternal blood flow to placenta increases from 50ml/min in the 1st trimester to 500- 750ml/min at term • Achieved by anatomical convesion of the maternal spiral arteries by trophoblast • Trophoblast cells invade the spiral arteries within 12 weeks of pregnancy and replace the smooth muscle of the wall, converting them to wide bore, low resistance, large capacitance vessels. • This process is normally complete by 20 wks • Complete or partial failure of throphoblastic invasion • Retain pre-pregnancy characteristics: relatively narrow bore, high resistance and low capacitance • Results in impaired perfusion of the fetoplacental unit • Hypoperfused placenta releases circulating factor(s) wich causes vascular endothelial cell activation, affecting multiple organ systems
  • 8. a) The maternal surface shows an ill- defined area (arrows) which coincided with the infarction hematoma. b) Cut sections of the placenta show a large round hemorrhagic lesion surrounded by infarcted placental tissues. These lesions are significantly associated with intrauterine fetal death and growth restriction
  • 9.
  • 10.
  • 11. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition 1. Preconception counseling and adjustment of treatment in women with chronic hypertension Change in anti-hypertensives. Drugs of choice are Methyldopa and Labetolol. Anti-HPT drugs contraindicated in pregancy: • Atenolol → FGR • ARBs, ACEIs and thiazide diuretics → Foetal anomaly Women in reproductive age on the abovementioned drugs must be on effective contraception The treatment of HPT in pregnancy is solely for maternal safety particularly the prevention of ICB. It does NOT reduce the risk of development of preeclampsia or perinatal mortality, nor improve fetal growth.
  • 12. Contraindicated in asthma Source: CPG Management of Hypertension 5th Edition
  • 13. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition 2. Recognition of women risk of preeclampsia for commencement of prophylaxis Moderate Risk High Risk •Primigravida •Age >40 years •Pregnancy interval >10 years •BMI of >35kg/m2 at first visit •Family history of PE •Multiple pregnancy •Hypertensive disease during previous pregnancy •Chronic kidney disease •Autoimmune disease such as Systemic Lupus Erythematosus (SLE) or anti- phospholipid syndrome(APS) •Type 1 or type 2 diabetes mellitus, and chronic hypertension.
  • 14. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition Risk factors based on PREDO study: Cluster analysis to estimate the risk of preeclampsia in the high-risk Prediction and Prevention of Preeclampsia and Intrauterine Growth Restriction (PREDO) study The risk of preeclampsia increases exponentially with respect to the number of risk factors.
  • 15. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition 3. Prophylactic therapy a. Aspirin Women with ≥2 moderate or >1 high risk factor should be started on low dose aspirin from 12 weeks up to 16 weeks of gestation until delivery. Dosage should be 100-150mg and taken ON in order to significantly reduce the incidence of PE b. Calcium Low dose calcium supplement (generally 500-1000mg daily) commenced before 20 weeks gestation reduces the r isk of PE There is no proven role of vitamin D, nor other supplememnts in reducing the risk of PE. Combined vitamin C and E should be avoided because they significantly increase the incidence of low birth weight without anu prevention effect against PE.
  • 16. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition Studies on Aspirin: CLASP trial: a randomised trial of low-dose aspirin for the prevention and treatment of pre- eclampsia among 9364 pregnant women CLASP (Collaborative Low-dose Aspirin Study in Pregnancy) Collaborative, published in March 1994 Overall, the use of low dose aspirin (60mg daily) was associated with a reduction of only 12% in the incidence of proteinuric preeclampsia, which was not significant. Nor was there any significant effect on the incidence of IUGR or of stillbirth and neonatal death. Aspirin did, however, significantly reduce the likelihood of preterm delivery (19.7% aspirin vs 22.2% control; absolute reduction of 2.5 [SD 0.9] per 100 women treated; 2p = 0.003). There was a significant trend (p = 0.004) towards progressively greater reductions in proteinuric pre‐ eclampsia the more preterm the delivery. ASPRE trial: performance of screening for preterm pre-eclampsia, published July 2017 The ASPRE trial demonstrated that, in women with singleton pregnancy who were identified by means of first-trimester combined screening as being at high risk for preterm PE, the administration of aspirin at a dose of 150 mg per day from 11–14 weeks until 36 weeks' gestation reduces the incidence of preterm PE by > 60%
  • 17. ROLE OF PRIMARY CARE Source: CPG Management of Hypertension 5th Edition 4. Fetal anomaly screening Women with chronic HPT have about 20-30% increased risk for fetal congenital cardiac anomaly. They should be referred to Maternal-Fetal Medicine (MFM) specialist in the tertiary centre for nuchal translucency (NT) scan at 12-14wks followed by detailed scan at 22-24wks of gestation. If a cardiac abnomaliy is detected, cardiology referral is recommended. 5. Prevention of eclampsia and other complications of PE Education on the signs and symptoms of preeclampsia for early diagnosis and referral for further management may prevent progression into eclampsia
  • 18. SEVERE PRECLAMPSIA Source: CPG Management of Hypertension 5th Edition Definition: (acc to the American College of Obstetricians and Gynaecologists) a. SBP ≥160/ DBP ≥110 mmHg on two occasons at least 4 hrs apart while resting b. Thrombocytopenia - Plt count <100 c. Abnormal liver enzymes (elevated AST/ALT), severe persistant RUQ/epigastric pain unresponsive to treament d. Pulmonary oedema e. New onset of cerebral or visual disturbances Principle of management include: 1) Control of BP (mangement of acute hypertensive crisis: • IV Hydralazine, IV Labetolol or oral Nifedipine may be used to lower the BP. • BP should be reduced within 30-60 minutes to reduce the risk of maternal stroke • Diuretics are generally contraindicated as it reduces plasma volume → IUGR and may increase perinatal mortality. Only used in the treatment of acute pulmonary oedema 2) Monitoring of maternal or fetal complications 3) Seizure prophylaxis 4) Timely delivery
  • 19.
  • 20. IV Labetolol Protocol IV Labetolol 10mg STAT (2cc-PURE) over 1 minute and repeat at 5 minute intervals (max dose: 200mg (40cc) Infusion syringe pump: 200mg IV Labetolol (40cc) in 50cc syringe and start at 4cc/hr, and increase by 4cc at 30 minutes. Stop infusion if rate exceeds 150mg/hr (30cc/hr) and inform specialist 1 vial = 5cc = 25mg Effective dose: 20-150mg/hr (4-30cc/hr) IV Hydralazine Protocol Loading dose: • Start at 4cc/hr for 5 mins • To check BP after 5 mins • Then cont with maintenance dose Maintenance dose: • 1cc/hr • check BP after 15 min • icrease by 1cc/hr every 30 mins to titrate till DBP 100mmHg • Maintain IV Hydralazine once DBP 90-100mmHg • Titrate down once DBP <90mmHg 1 vial = 5cc = 20mg Maximum dose: 10cc/hr Dilution: 5cc Hydralazine + 20cc NS Antidote: IV Atropine 600mcg (bolus)
  • 21. IV MgSO4 is the drug of choice for prevention of eclampsia and to abort an eclamptic fit. It also provides fetal neuroprotection following the preterm birth with a significant reduction in the incidence of cerebral palsy. Alternative is IV Diazepam but it is inferior in efficacy. 1. Start MgSO4, and continue for 24 hrs following delivery or initiation (whichever comes later). 2. Consider delivery once decision for MgSO4 has been made. Anticonvulsants in PE and Eclampsia Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan
  • 22. IV MgSO4 Protocol 1) The Loading Dose IV MgSO4 4g Slow Bolus Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan 8cc MgSO4 + 12cc NS in 20cc syringe run on IV infusion pump 80cc/hr to infuse 20cc in 15 mins In case of eclampsia; If fit persist >15minutes, add 2g MgSO4 4cc MgSO4 + 16cc NS in 20cc syringe (infused at 80cc/hr)
  • 23. Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan IV MgSO4 Protocol 2) The Maintainence Dose IV MgSO4 1g/hr 2cc MgSO4 + 48cc NS in 50cc syringe run on IV infusion pump 50cc/hr for 24 hrs after the last fit or 24 hrs after delivery, whichever comes later
  • 24. MgSO4 Toxicity 1. Monitoring toxicity (hourly) • ECG - prolonged PR interval, wide QRS complex • Deep tendon reflexes must be present • Urine output >30ml/hr (0.5cc/kg/hr) • RR between 12 to 16/minute • SPO2 >95% • GCS E4V5M6 Source: Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan 2. Antidote 1g Calcium Gluconate (10cc of 10% solution) given slow IV bolus over 10 minutes
  • 25. Source: NICE guidelines 2020 hypertension in pregnancy and management Fetal assessment • Offer fetal heart auscultation at every antenatal appointment • Carry out USG assessment of the fetus at diagnosis and, if normal, repeat every 2 weekly • Carry out CTG at diagnosis and then only if clinically indicated; reduced FM/ PV bleed/ abdominal pain/ deterioration of maternal indication Example of Umilical Artery Doppler Wave Forms A) Normal umbilical artery Doppler flow waveform B) Absent C) Reversed end-diastolic Doppler flow in umbilical artery USG assessment 2 weekly for non-PE women with previous: • Severe PE • PE requiring delivery <34 wks • PE with SGA (<10th centile) • IUD • Placental abruptio
  • 26. Source: NICE guidelines 2020 hypertension in pregnancy and management Timing of birth Weeks of pregnancy Timing of birth <34 wks Continue surveillance unless there are indications for planned early birth. Offer IV MgSO4 and IV Dexamethasone as per guidelines on preterm labour and birth 34-36 wks Continue surveillance unless there are indications for planned early birth. When considering the option for planned early brith, take into account the woman/s and baby’s condition, risk factors and availability of neonatal unit beds. Consider IV Dexamethasone as per guidelines on preterm labour and birth >37 wks Initiate birth within 24-48 hrs Indications for planned early birth: • Inability to control maternal BP, despite using ≥3 antiHPT in appropriate doses • Maternal SPO2 <90% • Progressive deterioration in liver function, rel function, hemolysis or platelet count • Ongoing neurological features; intractable headache, repeated visual scotoma, eclampsia • Placental abruptio • Reversed end-diastolic flow in the umbilical artery doppler velocimetry, a non-reassuring CTG, or stillbirth
  • 27. ECLAMPSIA OBSTETRIC EMERGENCY ACTIVATE RED ALERT Place patient in left lateral position (recovery position) Secure airway Administer oxygen • Give MgSO4 as per protocol • IV access x2 • Commence antiHPT as per protocol • Cont IV MgSO4 infusion as per protocol • Auscultate heart and lungs • Palpate abdomen, reflexes, assess fetal condition • VE and catheterize after BP stablised • Decide mode of delivery • Refer to anaethesia for ICU management Blood Ix: FBC, LFT, RP, uric acid, coag profile, GXM 7 Principles of Managing Eclampsia
  • 28. POSTPARTUM CARE Source: CPG Management of Hypertension 5th Edition • Postpartum, BP should be regularly checked at local clinics • The dose of antihypertensives should be tailed down gradually • On average, anti-HPT agents are required for longer in womwith PE (~2wks) than those with gestational hypertension (~1wk) • Chronic HPT is diagnosed when HPT persists after 3 months postpartum. LONG TERM FOLLOW-UP • Evidence suggests 13% of women with PE will have underlying essential HPT that was not suspected antenatally. • There is increased risk of ischaemic heart disease, thrmboembolism and stroke following PE • Long-term follow-up ot pts with a history of hypertension in pregnancy is advisable
  • 29. Thank you! REFERENCES : 1. Clinical Practice Guidelines - Management of Hypertension (5th Edition) 2018 MOH/P/PAK/391.18 (GU) 2. ISSHP guidelines in hypertension disorder in pregnancy 3. Handbook of Obstetric Emergencies by Dr Gunasegaran Rajan, Muniswaran Ganeshan, Tang Boon Nee, Thaneemalai Jeganathan 4. Obstetrics by Ten Teachers 19th Edition CME DEPARTMENT OF OBSTETRICS AND GYNECOLOGY/ HEBHK