Maternal medical conditions

Question 1

xFprola

General principles

Answer 1

Condition
- diagnosis, sequelae, last flare, treatments, MDT carers

Impact of condition on pregnancy
- risks
- antenatal care
- fetus and neonate
- delivery consideration
- postpartum care

Impact of pregnancy on condition
- risks of flare
- additional investigations
- delivery consideration
- post partum care

Question 2

Pre-pregnancy counselling

Answer 2

• PMHx - counsel re impacts of condition on pregnancy and impacts of pregancy on condition. Optimise.
• Meds - stop teratogens, counsel re relative safety/benefits of others if appropriate
• FHx - also note congential abnormalities
• Social Hx - smoking cessation, avoid alcohol and other substances. Review occupational hazards. Supports. DV screen.
• Document height, weight, BMI. Address gestational weight gain
• Cervical smear if due
• Antenatal bloods
• Vaccinations - MMR, Varicella, DTaP, COVID-19, HPV, Hep B
• Folic acid (appropriate dose), iodine
• Genetic carrier screening - CF, SMA, Fragile X
• Discuss travel, CMV avoidance if applicable, food safety
• CONTRACEPTION if not ready

Question 3

Obesity

Risks
Management

Pregnancy care

Answer 3

Risks:
- Maternal - Infertility, GDM, PIH and PET, labour dystocia and CS birth, shoulder dystocia, PPH, perineal trauma, maternal death, VTE, higher procedural complexity, anesthetic complications, postnatal depression, breastfeeding difficulty
- Fetal - miscarriage, fetal anomaly (NTD), preterm birth, growth restriction, macrosomia, stillbirth, NICU admission, childhood obesity

Antenatal:
- MDT = high risk obs, anaesthetics, dieticians, social work
- Limit gestational weight gain 5-9kg
- High dose folate, vitamin D
- Detailed fetal anatomy
- Early OGTT (BSLs if bariatric surgery)
- Growth USS surveillance
- Consider VTE prophylaxis

Intrapartum:
- Tertiary centre with bariatric equipment available
- IOL 39weeks if BMI >50
- IV line (may need USS guidance)
- USS for presentation on arrival
- Consider early epidural and CSE
- CTG (FSE if poor pick up)
- Active 3rd stage (deltoid IM)
- If CS: Senior staff, pannus retraction, Alexis-O, consider suprapannus incision, higher dose cefazolin, PDS for sheath

Postnatal:
- Early mobilisation
- Weight adjusted clexane for VTE prophylaxis
- Breastfeeding support
- Contraception
- PND screen
- Weightloss support - refer for bariatric surgery

Question 4

Rheumatoid arthritis

Periconceptual
Antenatal
Intrapartum
Postnatal

Risks, management

Answer 4

Periconceptual:
- Counsel risks: >50% improve in pregnancy, 90% flare PP. Atlanto-axial subluxation if GA (rare), PTB, IUGR, impacts of medications, GDM if on steroids, neonatal SLE if anti-Ro/La,
- Review meds: Azathioprine, hydroxycholorquinine, sulfasalazine okay. Biologics okay but avoid in late 3rd trimester (neonatal suppression effect). NSAIDs okay in 2nd trimester. Stop MTX and defer for 3months
- Anti Ro/La screen

Antenatal:
- MDT: High risk obs, rheumatology, obs physcians, anaesthetists
- Review joints
- BSL monitoring if on prednisone
- Monitor Hb and supplement

Intrapartum:
- Aim vaginal birth
- Sress dose monitoring if on prednisone
- Mindful of maternal positioning (hips)
- Alert anaesthetics (risk of axial/atlantosubluxation)

Postpartum:
- Re-establish medications
- Monitor for flare
- Breastfeeding support (meds dependent)
- VTE prophylaxis
- Contraception

Question 5

How do you manage a pregnancy concieved on MTX?

Answer 5

• Review reason for MTX
• e.g. RA, dose, timing
• Assess disease control
• Counsel: embryotoxic - risk miscarriage, fetal anomly in particular NTD. May also be healthy.
• Offer TOP
• Stop MTX - refer MDT and review other meds as alternatives
• Refer to MFM
• High dose folic acid
• Early anatomy USS

Postpartum: Consider switch back if needing for disease control, avoid breastfeeding, LARC and stop 3months prior to future pregnancy

Question 6

Differential diagnosis for worsening SOB in pregnancy

Answer 6

• Physiological
• Anaemia
• Anxiety
• Multiple pregnancy
• Polyhydramnios (including TTTS)
• PE
• Pulmonary oedema (with PET)
• Cardiomyopathy
• Aortic dissection
• Arrythmia
• Infective (pneumonia, influenza, COVID-19, varicella)
• Asthma flare
• Pneumothorax
• Thyroid disease

Question 7

VTE

Risk factors

Pre-existing, antenatal

Answer 7

Pre-existing:
* Previous VTE
* Known thrombophilia - heritable or acquired
* Medical comorbidities - malignancy, heart failure, active SLE, IBD, nephrotic syndrome, T1DM with nephropathy, sickle cell, current IVDU
* Age >35
* BMI >30
* Parity >/=3
* Smoking
* Gross varicose veins
* Paraplegia or other reason for immobilisation

Antenatal:
* OHSS
* Multiple pregnancy
* PET
* Hospitalisation, immobilisation
* Prolonged labour
* PPH >1000mL
* Caesarean birth
* Surgery in pregnancy or peurperium
* Stillbirth

Question 8

Suspected PE in pregnancy

Investigations and management

Answer 8

Investigation:
* FBC, coags
* Thrombophilia screen: Protein C and S, antithrombin III, prothrombin gene mutation, factor V leiden, APL antibodies (Repeat outside of pregnancy)
* ECG
* CXR
* ABG
* CT-PA if unstable, VQ not available or CXR abnormal
* Otherwise VQ scan
* USS lower limbs only if symptoms

Management:
* ABCs
* Apply oxygen - high flow
* Transfer to appropriate location
* MDT - high risk obs, haematology, ICU, anaesthetics
* Anticoagulation - LMWH vs UFH if unstable
* Consider: thrombolysis or thoracotomy and clot retrieval if massive

Question 9

PE in pregnancy

Intrapartum, postpartum

Answer 9

Intrapartum:
- Deliver tertiary centre
- Consider IOL to time anticoagulants
- Stop LMWH 24h prior
- Consider switch to UFH if higher risk
- Anaesthesia: avoid regional if <24h after LMWH. Utilise PCA. May need GA.
- IV line, up to date CBC and G&H (2units X-matched), check APTT
- Remain hydrated, utilise TEDS and SCDs
- Active 3rd stage, prepare for PPH
- Surgical considerations: drains, interrupted subcut suturing, staples
- Protamine sulphate on hand

Postpartum:
- Caution re epidural removal
- Re-start anticoagulation at least 6weeks duration (MDT discussion with anaesthetics, haematology)
- Repeat thrombophilia screen if applicable
- Breastfeeding support
- Contraception (avoid COCP)
- Consider future pregnancy

Question 10

Counsel a patient about risks and benefits of CTPA

Answer 10

Risks:
* Significantly more radiation exposure to breast tissue than VQ scan - lifetime risk of breast cancer increased by 14%
* Theoretical risk neonatal hypothyroidism if given iodine (recent studies suggest maybe not)

Benefits:
* Low radiation dose to fetus
* Quick and readily available
* Utility if abnormal CXR: can diagnose other abnormalities e.g. pneumonia, pulmonary oedema, aortic dissection
* Can breastfeed

Question 11

Counsel a patient about risks and benefits of VQ scan

Answer 11

Risks:
* Slightly increased risk of childhood cancer
* Unable to breastfeed for 12 hours after scan.
* Less accurate if CXR abnormal

Benefits:
* Substantially less radiation to breast tissue
* Negligable radiation exposure
* Good at diagnosing peripheral PE
* Lower rate of non-diagnosis as less prone to suboptimal image quality/artefacts

Question 12

A patient is diagnosed with Cushing syndrome from adrenal source and is treated. How do you counsel her in pregnancy?

Answer 12

Risks:
PTB
IUGR
Stillbirth
GDM
HTN and PET
Excessive weight gain
Neonatal adrenal insufficiency
CS infection

Management:
BP surveillance
OGTT
Dietician
Growth USS
Aim VB
Treatment - adrenalectomy > medication

Question 13

Type 1 DM

Periconceptual
Antenatal
Delivery
Postnatal

Answer 13

Periconceptual
* Counsel risks: higher if poorly controlled - infertility, miscarriage, fetal anomaly (cardiac, NTD, sacral agenesis), PTB, HTN, PET, stillbirth, IUGR, LGA, shoulder dystocia, CS, progression of pre-existing disease, neonatal hypoglycaemia
* Optimise HbA1c - aim <48
* High dose folic acid
* Screen retinopathy, nephropathy - baseline urine ACR, CBC, Renal
* Ascertain if hypo awareness

Antenatal
* MDT - high risk obs, endocrine/diabetes/obs physicians, dietician, anaesthetics
* Aspirin from 12weeks
* Detailed fetal anatomy scan + echo, uterin artery doppler
* PET screen
* Growth surveillance - USS 28, 32, 36weeks
* Monitor BSL and insulin requirements - expect to rise, but risk of hypo in T1. Notify if falling
* Sick day advice
* HbA1c each trimester
* Screen re mental health

Delivery
* Aim VB. CS if LGA >4.5kg
* IOL 38weeks
* Insulin/glucose infusion
* CTG
* Active 3rd stage

Postnatal
* BSL monitor, alter insulin
* Neonatal BSL checks
* Breastfeeding support
* VTE prophylaxis
* Contraception
* Diabetes team follow up

Question 14

How do you manage DKA in pregnancy?

Answer 14

• Admit to HDU
• MDT
• Screen for cause/trigger and treat
• Insulin infusion +/- dextrose
• Aggressive rehydration
• Correct electrolytes, especially K+
• Hourly BSLs, ketones
• 2 hourly VBGs
• Fluid balance - monitor UO
• Fetal monitoring - CTG (may be abnormal until maternal stabilisation)
• If need to deliver, stabilise maternal status prior
• Follow up - sick day education, BSL and ketone monitoring, MDT

Question 15

SLE

Periconceptual
Antenatal
Delivery
Postnatal

Answer 15

Periconceptual
* Counsel risks - higher if untreated or flare <6months. Miscarriage, early onset FGR, PTB, HTN, PET, VTE, Stillbirth, neonatal lupus.
* Review medications usually benefit > risk but NOT for methotrexate. Continue hydroxychloroquinine.
* Baseline c3/c4, anti ds DNA, CBC, Renal, LFTs, urine ACR
* Anti Ro/La screen (30% have - if present 5% risk cutaneous lupus and 2% risk CHB)

Antenatal
* MDT - high risk obs, rheum, anaesthetics
* Aspirin (LMWH if APLs or prev VTE)
* Fetal heart auscultation if Anti Ro/La weekly from 16weeks
* FAS + uterine artery doppler
* Growth surveillance from 24weeks
* BP, PET surveillance
* Screen for flares

Delivery
* Aim VB
* IOL 38+
* CTG
* Active 3rd stage
* Hydrocortisone if high dose/long term steroids

Postnatal
* Neonatal review
* Breastfeeding support
* VTE prophylaxis
* Contraception

Question 16

A patient has had a history of IHD and is in early pregnancy. How do you counsel?

Answer 16

History - timing of event, context, diagnosis, intervention, ongoing management, current exercise tolerance
Counsel re risks - recurrence, progression of CHD in pregnancy, maternal mortality, impact of medications, PTB, IUGR
Review medications
Baseline echo
Modify RFs

Pregnancy - MDT, echo if concerns, growth surveillance, aim VB but if poor exercise tolerance or repeat event late 3rd trimester CS recommended

Postpartum - HDU monitoring, VTE prophylaxis, contracetion, breastfeeding support

Question 17

How can you differentiate an SLE flare from PET in pregnancy?

Answer 17

Active <6m prior to conception - more likley SLE
Concurrent SLE symptoms - more likely SLE
Timing <20weeks - more likley SLE
Casts on urine microscopy - more likely SLE
Thrombocytopaenia - can happen for both
Urate low - less likely PET
Anti ds DNA rising from baseline - more likely SLE
Falling complement levels from baseline - more likley SLE
Seizure - may happen in both
Renal biopsy is definitive but not done in pregnancy

Question 18

An alpha thalassaemia trait is diagnosed in a preconceptual work-up. How do you proceed?

Answer 18

• Ascertain mutation
• Ascertain partner’s status
• Consider PIGD or donor gamete with screening prior
• In pregnancy: NIPT for fetal genotype, amniocentesis to confirm if will change management
• Screen Hb, only supplement Fe if low

Question 19

Beta thalassaemia

Periconceptual
Antenatal
Delivery
Postnatal

Answer 19

Periconceptual:
* Counsel risks - inheritance, worsening anaemia, IUGR, PTB, CS for CPD
* Test partner, consider PIGD or gamete donation
* Aggressive Fe chelation, stop 3m prior to pregnancy
* Screen re Fe overload - TFT, echo, ECG, cardiac MRI, LFTs, liver USS, DEXA scan, fructossamine,
* RBC antibody and hepatitis screen
* High dose folate

Antenatal:
* MDT - high risk obs, MFM, haematology, anaesthetics, paediatrics, genetics
* High dose folate
* Fe only if low
* Aspirin if splenectomy and plt count >600
* Fetal genotype if at risk - NIPT or CVS/amniocentesis
* Growth surveillance
* Fructossamine or BSL monitoring - HbA1c less reliable if transfusion dependent
* Consider chelation after 20weeks

Delivery:
* Aim VB
* CTG
* Active 3rd stage
* IV desferrioxamine

Postnatal:
* Breastfeeding support
* VTE prophylaxis
* Contraception

Question 21

Essential HTN

Periconceptual
Antenatal
Delivery
Postnatal

Answer 21

Periconceptual:
* Counsel risks - progression of HTN, renal disease, cardiomyopathy, ACS, stroke, CS delivery, PET, miscarriage, stillbirth, PTB, IUGR
* Review if underlying cause or not
* Baseline urine PCR, renal, LFTs, CBC, HbA1c, lipids
* Adjust meds

Antenatal:
* MDT - obs phys, high risk obs, anaesthetics
* Aspirin/Ca from 12weeks
* UtA doppler with FAS
* Serial BP checks, PET screens
* Treat BP to remain <140/90
* Growth USS 4weekly from 28weeks

Delivery
* Aim VB
* IOL 39weeks
* CTG
* Analgesia - epidural to optimise
* Active 3rd stage - avoid syntometrine

Postnatal
* BP monitoring
* Adjust meds
* Breastfeeding support
* VTE prophylaxis
* Contraception

Question 21

Myasthenia Gravis

Periconceptual
Antenatal
Delivery
Postnatal

Answer 21

Periconceptual:
* Counsel risks - course unpredictable (40% relapse, 30% improve, 30% no change), early pregnancy changes may reduce medication efficacy, risk fetal arthyrogyroposis, transient neonatal MG
* Optimise pre pregnancy, consider thymectomy
* Review meds, stop teratogens

Antenatal:
* MDT - high risk obs, anaesthetics, neurology, paeds
* Continue pyridostigmine, alter dose frequency
* Clear documentation of medications to avoid incl aminoglycosides, Bblockers, MgSo4 (may cause a crisis!) anaesthetic drugs
* Monitor TFTs
* Detailed USS if reduced FMs, polyhydramnios

Delivery:
* Aim VB
* Early epidural
* May need AVB if exhausted
* Give meds IV, stress dose hydrocortisone if long term steroids

Postnatal:
* Observe neonate for 48hrs
* Breastfeeding support
* Re-adjust meds if needed
* Thymectomy if not had prior
* Monitor for PP relapse

Question 22

Rheumatic heart disesase with mitral stenosis

Periconceptual
Antenatal
Intrapartum
Postnatal

Answer 22

Periconceptual:
* Counsel risks - cardiac failure, pulmonary oedema, arrythmia, atrial thrombus, maternal mortality up to 3%, IUGR, PTB, IUFD
* Review function, symptoms, treatment, last echo
* Review meds
* Baseline echo, ECG, CXR
* Contraception and defer if valve <1cm2- vavotomy

Antenatal
* MDT - high risk obs, cardiology, anaesthetics
* Consider TOP if severe
* Echo each trimester
* Avoid high HR to enable LA filling - Bblock, restrict exercise, rhthym control
* Balloon valvotomy if severe
* Growth USS
* Optimise Fe
* VTE prophylaxis

Intrapartum:
* Aim VB
* IOL/schedulled timing to allow for MDT
* Optimise analgesia (avoid high HR)
* Passive 2nd stage
* Telemetry
* Fluid balance
* Avoid supine or lithotomy
* Active 3rd stage (caution re syntometrine and carboprost)

Postnatal:
* Care in CCU/HDU
* Strict fluid balance +/- frusemide
* Telemetry
* VTE prophylaxis
* Breastfeeding suport
* Contraception
* MH screen
* Cardiology follow up

Question 23

You see a patient with increasing SOB in pregnancy and suspect cardiomyopathy. How do you manage?

Answer 23

Assess:
* History
* Examination - obs, weight, JVP, auscultation ?oedema/effusion, murmur, peripheral oedema
* Investigation - CXR, BNP, ECG, echocardiogram

Management:
* MDT - high risk obs, cardiology, anaesthetics
* HDU/ICU
* Serial echo
* Treat HF - Bblockers, rhythm conrol (digoxin), diuretics (frusemide), vasoidlators (hydralazine, GTN)
* BP treatment
* VTE prophylaxis
* Avoid aortocaval compression
* Delivery - elective, mode depends on tolerance. If VB early epidural, shorten 2nd stage
* Ecbolics - slow oxytocin, avoid syntometrine and carboprost
* Postnatal - strict fluid balance as highest time of deterioration, telemetry, may need inotropes, VTE prophylaxis, contraception, breastfeeding support, 33% recurrence risk, debrief

Question 24

How do you manage fast AF in a patient with a background of RHD, intrapartum?

Answer 24

ABCs
O2s
IV access
Telemtery
Bblock, digoxin, frusemide
CTG
Consider delivery to reduce preload

Question 25

Sickle cell anaemia

Periconceptual
Antenatal
Intrapartum
Postnatal

Answer 25

Periconceptual:
* Counsel risks - up to 50% crisis, maternal infection, perinatal and maternal mortality, VTE, acute chest syndrome, miscarriage, PTB, IUGR, PET, abruption, RBC antibodies and high Fe if transfusions, autosomal recessive
* Test partner, consider PIGD
* Echo
* Medication review
* High dose folate
* Consider Fe chleation, check for RBC antibody
* Review medications - stop hydroxyurea
* Get vaccines up to date

Antenatal:
* MDT - haematology, high risk obs, anaesthetics, paeds
* High dose folate, aspirin
* Crisis prevention
* ABx prophylaxis
* Hb monitoring
* Serial growth USS
* Screen for PET
* VTE prophylaxis

Intrapartum:
* Aim VB
* IV access, valid G&H
* Analgesia
* Crisis prevention - avoid dehydration, long labour, low temp
* CTG

Postnatal:
* VTE prophylaxis
* Breastfeeding suport
* Contraception
* MH screen
* Test neonate

Autosomal recessive

Question 26

How do you manage a sickle cell crisis?

Answer 26

Admit
ABCs
MDT
IV access, Hb, G&H
O2
Warm IVFs
Transfuse if needed
Analgesia
Antiemetics
Antibiotics
VTE prophylaxis

Question 27

APLS

Periconceptual
Antenatal
Delivery
Postnatal

Answer 27

Periconceptual
* Screen for disease sequalae
* Counsel risks - miscarriage, early onset FGR, PTB, HTN, PET, abruption, VTE, stillbirth, neonatal lupus.
* Review medications
* Baseline CBC, Renal, LFTs, urine ACR
* Anti Ro/La screen (30% have - if present 5% risk cutaneous lupus and 2% risk CHB)

Antenatal
* MDT - high risk obs, haem, anaesthetics
* Aspirin + LMWH (prophylactic, intermediate if prev VTE and therapeutic if on treatment prior)
* Fetal heart auscultation if Anti Ro/La weekly from 16weeks
* FAS + uterine artery doppler
* Growth surveillance from 24weeks
* BP, PET surveillance
* Pscyhological support (especially if recurrent losses)

Delivery
* Aim VB
* IOL 38+
* Bridge clexane to UFH if treatment - time neuroaxial anaesthesia if needed
* CTG
* Active 3rd stage

Postnatal
* Neonatal review
* Breastfeeding support
* VTE prophylaxis
* Contraception - avoid COCP

Question 28

Marfan Syndrome
Periconceptual
Antenatal
Delivery
Postnatal

Answer 28

Periconceptual:
* Counsel risks - aortic dissection (highest if aortic root >40mm), PET, mortality, PTB (cervical incompetence), inheritance as autosomal dominant, IUGR, stillbirth
* Consider PIGD, egg donor and surrogacy,
* Echo
* Contraception and aortic root repair if >45mm

Antenatal:
* MDT - MFM, cardiology, anaesthetics
* Echo each trimester (monthly if >40mm)
* Bblocker
* Cervical length USS
* Serial growth

Delivery:
* Tertiary unit
* VB unless aortic root >45mm or hx of dissection
* Instrumental, shorten second stage
* Analgesia - early epidural
* Telemetry

Postnatal:
* Cardiac monitoring
* VTE prophylaxis
* Breastfeeding support
* Contraception
* Cardiology follow up, echo at 6months
* Monitor re symtpoms as risk of rupture persist 6-8weeks

Question 29

You see a patient at 34weeks with a history of itchy palms and no rash, you suspect obstetric cholestasis. How do you proceed?

Answer 29

Assess:
* LFTs
* Bile salts
* Screen for other causes

Manage:
* Counsel re risks - maternal symptoms, poor sleep, PTB, stillbirth, meconium, CS delivery, no long term maternal or neonatal harm
* LFT and bile salt weekly
* FM monitoring - no role for routine CTG unless concerns
* Topical emolients
* Antihistamines (sedating at night)
* Ursodeoxycholic acid - consider, not routine
* Screen for psychological wellbeing
* IOL timing according to bile salts
- <40 deliver at term
- 40-100 deliver 38weeks
- >100 deliver accordingly, may do 36weeks
* CTG in labour
* Postnatal - repeat LFTs 6weeks (resolution confirms diagnosis), future pregnancy recurrence risk, avoid COCP

Question 30

List a differential diagnosis list for obstetric cholestasis and investigations to exclude other causes

Answer 30

• HELLP syndrome/PET
• Viral hepatitis
• Biliary: AFLP, pancreatitis, primary biliary cirrhosis
• Autoimmune hepatitis
• Dermatoses: eczema, PEP, atopic eruption of pregnancy, pemphigoid gestationis

Investigations:

• Bile salts
• FBC, LFTs, Cr, coagulation study
• Blood gas: glucose, lactate, ammonia
• Viral hepatitis panel: Hep A/B/C, CMW, EBV
• Liver autoantibodies: anti-Sm, anti-mitochondrial, ANA
• Liver/upper GI USS
• Urine PCR

Question 31

What is a differential diagnosis for thrombocytopaenia in pregnancy and how do you investigate?

Answer 31

• Gestational - >100, all screens normal
• PET/HELLP - BP, urine PCR, CBC, Renal, LFTs, haemolysis screen
• AFLP - LFTs, BSL, coags
• ITP - platelet surface antibodies (diagnosis of exclusion)
• DIC - sepsis screen, coags
• Bone marrow failure - blood film
• TTP/HUS - ADAMST13 test, haemolysis screen
• Infection - HIV, viral
• Drugs - e.g. heparin
• SLE/APLS - antibodies, hx and exam

Question 32

Cystic Fibrosis
Periconceptual
Antenatal
Delivery
Postnatal

Answer 32

Periconceptual:
* Counsel risks - lung function deterioration, CHF, maternal mortality (depends on FEV and nutrition), PTB, IUGR
* Test partner genotype, PIGD as autosomal recessive
* Pulmonary function test, consider echo
* Sputum culture - treat and defer if Burkholderia
* Vaccinations
* Optimise nutrition

Antenatal:
* MDM - MFM, high risk obs, genetics, dietician, respiratory, chest physio
* Continue meds incl dornase alfa
* Screen spirometry and sputum regularly
* GDM screen (often have pancreatic insufficiency)
* Serial growth USS
* Admit for bedrest if hypoxia

Delivery:
* Aim VB
* Consider instrumental for shortened second stage if maternal exhaustion, risk of pneumothorax
* Analgesia - epidural
* Pulse oximetry monitoring
* If OT - avoid GA if possible

Postnatal:
* Pulse oximetry monitoring - consdier in HDU
* VTE prophylaxis
* Breastfeeding support
* Contraception
* MMH screen
* MDT follow up

Question 33

Explain to patients with positive CF carrier status what CF is and what is their risk of having a child with CF and what their fertility options are.

Answer 33

CF is a genetic condition where a faulty gene results in impaired movement of salt and water in and out of cells. This causes a build up of thick sticky mucus in various organs leading to dysfunction. Can affect lungs, pancreas.
It is a condition that reduces life expectancy; 50% of people will live past 40 years old.

If both parents are carriers:
* 50% chance child will be a carrier
* 25% chance child will have CF
* 25% chance child will not have CF or be a carrier.

If one parent has CF and one parent is a carrier:
* 50% chance child will have CF
* 50% chance child will be a carrier

Fertility options:
* Await birth of child to determine status, with chances as above (Guthrie card or sweat test)
* Antenatal screen with NIPT -
* Antenatal diagnosis with CVS or amnio - need to know miscarriage risk, may have TOP if +ve
* Pre-implantation genetic diagnosis with IVF (risk OHSS, multiples, still recommmend invasive test in pregnancy to confirm)
* Gamete donor
* Adoption

Question 34

Outline your management for a woman with a new diagnosis of GDM at 28 weeks gestation:

Counsel, manage, delivery, postnatal

Answer 34

Counsel:
* Explain - during pregnancy your body doesn’t regulate glucose as well which predisposes women to developing GDM which is where your blood glucose level is abnormally high.
* Risks - LGA, IUGR, stillbirth, PET, CS delivery, shoulder dystocia, neonatal hypoglycaemia and jaundice, 30% recurrent GDM, up to 50% T2DM, childhood obesity

Manage:
* MDT - high risk obs, endocrine/diabetes team, dietician, anaesthetics
* BSL testing QID - aim fasting </= 5 and post meals </= 6.7
* Exercise, limit GWG
* Treatment with diet, metformin, insulin
* PET surveillance
* Growth USS 4weekly

Delivery:
- Aim VB
- IOL 38-40 weeks
- Delivery in hospital
- IVL, FBC, G&H
- BSL monitoring in labour +/-insulin infusion
- CEFM in labour
- Prepare for shoulder dystocia, active 3rd stage

Postnatal:
- Stop GDM meds.
- Check BSLs
- Breastfeeding and ASAP
- BSL monitoring for baby +/- paeds review
- Contraception
- T2DM screening: OGTT or fasting glucose or HbA1c 3 months PP.

Question 35

IBD
Periconceptual
Antenatal
Delivery
Postnatal

Answer 35

Periconceptual:
* Counsel - low if well controlled, risk of flare 1/3, highest PP if UC, if poorly controlled miscarriage, PTB, IUGR, perineal trauma if vulval involvement. Stoma may crack or bleed
* Review meds

Antenatal:
* MDT - high risk obs, gastroenterology, dietician, anaesthetics
* Continue meds, stop TNF-alpha in 3rd trimester
* High dose folate if anti-folate
* Screen for B12 and Fe deficiency
* GDM screen and repeat if on steroids
* Growth USS surveillance

Delivery:
* Aim VB
* ElCS if perianal disease, J pouch, fistula
* If stoma - have surgeon present at delivery
* Lower threshold for episiotomy
* Stress dose hydrocortisone if on steroids

Postnatal:
* Breastfeeding support
* VTE prophylaxis
* Contraception
* Symptom review for flare
* Avoid live vaccines for infant for 6m if taking TNF alpha e.g.infliximab
* MDT follow up

Question 36

von Willebrand’s disease
Periconceptual
Antenatal
Delivery
Postnatal

Answer 36

Periconceptual:
* Assess type, bleeding history, response to DDAVP
* Counsel risks -
Type 1 - levels rise, higher bleeding 1st trim as not happened yet
Type 2/3 - minimal change so higher risk bleeding with APH, PPH (and scondary PPH), perineal haematoma, RBC transfusion, fetal ICH and cephalhaematoma
* Baseline vwF and factor VIII assays
* RBC antibody screen

Antenatal:
* MDT - high risk obs, haematology, anaesthetics, paeds
* Document haemostasis plan
* Avoid aspirin
* Optimise Hb and Fe
* vWF level at booking, third trim and pre procedure
* DDAVP

Delivery:
* Deliver in hospital
* Aim VB
* If T2 or 3: Avoid ECV, FBS, FSE, ventouse, midcavity forceps
* Regional anaesthesia depends on type and vWF levels
* IV access, 4units Xmatched
* Assess vWF levels and repeat if long labour
* DDAVP 0.3mck/kg if levels <0.5 (care to fluid restrict and avoid in PET)
* IV TXA
* Active 3rd stage (give IV not IM)
* Weigh losses

Postnatal:
* Cord bloods to check if neonate affected
* Continue TXA and DDAVP
* Monitor lochia - levels fall again so higher risk bleeding
* Neonate - PO vitamin K if type 2 or 3, head USS if type 3
* VTE prophylaxis - caution re LMWH
* Breastfeeding support
* Contraception and menstrual control

1 - less of vWF (AD)
2 - present, but not functioning (AD)
3 - severe reduction/absent (AR)

Question 37

Asthma
Periconceptual
Antenatal
Delivery
Postnatal

Answer 37

Periconceptual:
* Counsel risks - 1/3 improve, 1/3 worsen, 1/3 remain the same. No adverse effect if well controlled. If poor control - miscarriage, stillbirth, PTB, IUGR. Corticosteroid effects if systemic.
* Review meds - usually benefits > risks to obtain control and emphasise safety

Antenatal:
* MDT - high risk obs, respiratory, anaesthetics, NICU
* Avoid triggers
* Continue meds
* Treat flare as usual - prednisolone okay
* BSL test if on steroids

Delivery:
* Aim VB
* Meds as usual (less risk flare >36weeks)
* Stress dose hydrocotrisone if long term steroids
* Avoid carboprost if PPH (miso okay)

Postnatal:
* Avoid NSAIDs
* Breastfeeding support
* VTE prophylaxis
* Contraception
* PN follow up with GP or respiratory

Question 38

How do you manage an asthma attack in pregnancy?

Answer 38

DRSABCs
Admit
MDT - high risk obs, respiratory, anaesthetics
Oxygen - hudson mask, high flow, aim O2 sats >/= 95% and uptitrate as required
IV lines x2
Electrolytes check, ABG
Nebulise - Beta agonists, trial ipratropium bromide
Steroids - IV hydrocort or PO prednisone (whichever available)
Consdier IV Magneiusm sulphate or aminophylline
Rehydration if needed
Fetal monitoring via CTG
CXR to check for pneumonia and pneumothorax
Consider ICU if deteriorating PEFR, persisting hypoxia, hypercapnia, acidosis, feeble respiration, drowsiness, confusion, coma, respiratory arrest
Consider differentials, especially if not improving - PET with pulmonary oedema, PE, cardiomyopathy, sepsis,
Consider delivery if resp arrest, not improving or fetal distress

Question 39

Thrombocytopaenia in pregnancy
Differential diagnosis and investigations

Answer 39

• Gestational - usually above 80, normal pre pregnancy and resolves post, investigations normal
• PET/HELLP - Hb, renal, LFT, uPCR, haemolysis screen (LDH, haptoglobin, reticulocytes, unconjugated bilirubin), HTN
• AFLP - BSL, LFTs, coags
• ITP - antiplaatelet antibodies
• TTP/HUS - ADAMST13 test, haemolysis screen
• SLE - PMHx review, APLS screen, anti ds DNA, C3/C4
• DIC - coags, sepsis screen
• Bone marrow suppression - blood film
• Drug induced e.g. heparin
• Viral
• Spurious result

Clinical assessment - purpura, petechiae, lymphafenopathy, splenomegaly

Question 40

Thrombophilias in order of risk for thrombosis

Answer 40

• Antithrombin III deficiency - HIGHEST, monitor anti-Xa levels
• Protein C deficiency
• Protein S deficiency
• Factor V leiden - compound heterozygote > homozygote > heterozygote
• Prothrombin mutation

Question 41

ITP
Periconceptual
Antenatal
Delivery
Postnatal

Answer 41

Periconceptual:
* Counsel risks - falling of platelets further, spontaneous bleeding if <20, surgical bleeding if <50, PPH, neonatal bleeding e.g ICH as IgG cross placenta (poor maternal/neonatal correlation), GDM if long term steroids, limitation to regional anaesthesia if <80
* Review meds, optmise prior, splenectomy if needed
* Baseline FBC

Antenatal:
* MDT - high risk obs, haematology, anaesthetics, neonates
* Baseline FBC then monthly, fortnightly n 3rd trimester
* Plts need to be:
* >20 to prevent spontaneous haemorrhage
* >50 to prevent haemorrhage - AIM
* >80 for regional anaesthesia
* Treat if <50, symptoms, bleeding - steroids, IVIG, anti-D, other agents (thrombopoietin receptor agonists)
* Consider splenectomy in 2nd trim if severe
* No role for cordocentesis
* Clear anaesthetic plan documented
* BSL testing if long term/high dose steroids

Delivery:
* Aim VB at term
* Regional anaesthetic only if plt >80, may use PCA or GA if OT needed
* Avoid FBS, FSE, ventouse and difficult instrumental
* IV line, valid G&H
* Active 3rd stage (caution re IM)
* Platelet infusion if bleeding risk and severe

Postnatal:
* Plt follow up
* Cord bloods and neonatal sample 48hours
* Avoid IM Vit K until known
* Neonatal head USS or MRI if affected to check for ICH
* May be role for TXA
* VTE prophylaxis - NOT for clexane
* Avoid NSAIDs
* Breastfeeding support
* Contraception

Question 42

FGM
Periconceptual
Antenatal
Delivery
Postnatal

Answer 42

Periconceptual:
* Counsel risks - infertility, UTIs, difficulty with assessments, severe perineal trauma
* Counsel illegal to do, take anyone overseas to do and reinfublate
* Document type and provide diagram - better for single examination
* Specialist referrals if needed - fertility, urogynae
* Renal USS if urologicla obstruction

Antenatal:
* MDT - high risk obs, specialist centre, cultural support
* Offer deinfibulation in pregnancy or at birth - prefer in 2nd trimester as enables time to plan and have access to experienced clinician

Delivery:
* Aim VB
* If no deinfibulation prior - deinfibulation or anterior episiotomy.
* Warm compresses, higher chance of needing RML episiotomy
* Only repair to achieve haemostasis and anatomy restoration
* May need IDUC in

Postnatal:
* Reinforce illegal to perform or take child overseas to do
* Social and cultural support
* VTE prophlyaxis
* Breastfeeding support
* Contraception
* MMH screen
* Follow up for smear if not had prior

Question 43

Hypothyroidism
Periconceptual
Antenatal
Delivery
Postnatal

Answer 43

Periconceptual:
* Counsel risks - minimal if well controlled. Miscarriage, PTB, stillbirth, IUGR, abruption, PPH, neonatal neurodeveleopmental delay, cretinism if severe
* Review pathology
* Baseline TFTs, (anti TPO antibody not needed)
* Review meds, treat if TSH high,T4 low or TSH >10

Antenatal:
* MDT - high risk obs, endocrine, neonatal
* May need to uptitrate levothyroxine
* TFTs each trimester - aim TSH <2.5
* Growth USS if not well controlled
* Iodine

Delivery:
* Aim VB
* Active 3rd stage

Postnatal:
* Breastfeeding support
* VTE prophylaxis
* Contraception
* Monitor for PP thyroiditis

Question 44

Hyperthyroidism
Periconceptual
Antenatal
Delivery
Postnatal

Answer 44

Periconceptual:
* Counsel risks - exacerbation in T1, miscarriage, PTB, IUGR, fetal and neonatal thyrotoxicosis 1%, flare PP
* Baseline TFTs and TRAB
* Review meds - prefer PTU in first trimester, avoid pregnancy 4 months if radioactive iodine
* Review pathology

Antenatal:
* MDT - high risk obs, MFM, endocrine, neonatal
* TFTs and TrAB each trimester
* Refer MFM if TRAB high - risk fetal hyperthyroidism, assess growth, hydrops, fetal goitre (high mortality)
* PTU in 1st trimester then switch to carbimazole
* Stop iodine if hyperthhyroid, avoid seaweed foods
* Beta blockade
* Thyroidectomy in 2nd trimester if needed (airway compromise, suspected ca)
* Radioactive iodine contraindicated

Delivery:
* Aim VB
* Active 3rd stage
* Monitor for thyroid storm

Postnatal:
* Cord bloods for TFTs
* Neonatal observations for up to 2weeks, may need carbimazole until TRABs disappear
* Breastfeeding support
* VTE prophylaxis
* Contraception
* TFTs 2-4months
* Monitor for PP thyroiditis

Question 45

How do you manage a thyrotoxic crisis?

Answer 45

• MDT - high risk obs, endocrine, anaesthetics
• HDU/critical care
• IV access
• IVFs
• Cooling cares
• BSL control
• Beta blockade
• PTU high dose
• High dose iodide
• CTG - NB should improve with maternal improvement
• Consider DDx - sepsis, PE, AF

Question 46

PET
Antenatal
Delivery
Postnatal

Answer 46

Antenatal:
* MDT - high risk obs, anaesthetics, neonatal
* Counsel risks - HTN, stroke, eclampsia, low platelets, hepatic and renal impairment, pulmonary oedema, VTE, IUGR, abruption, NICU admission, PTB (iatrogenic), stillbirth, maternal mortality
* Bloods - FBC, Cr, LFTs twice weekly, coags if plt low or LFT impairment
* No need to repeat uPCR once positive unless suspect contaminated
* BP monitoring - twice weekly as OP if stable or as IP if new diagnosis, severe, other complicating features
* Antihypertensives to aim BP <140/90 - labetalol, methyldopa, nifedipine
* Growth USS and dopplers minimum fortnightly
* If <34weeks - corticosteroids
* Thromboprophylaxis if IP and delivery not imminent
* Monitor for symptom progression - headache, vision changes, swelling, RUQ pain
* MMH screen

Delivery:
* Delivery 37+ weeks, 34+ weeks if severe features or earlier if critical
* Aim VB - consider assisted if severe HTN in 2nd stage to limit further pressure rises with valsalva
* IV line, valid G&H, bloods within 6hours
* BP management - POs, IVs if vomiting or severe, epidural (if plts >80)
* Fluid balance and fluid restrict
* IV MgSo4 if severe
* Continuous CTG
* Active 3rd stage - concentrated oxytocin infusion, avoid syntometrine
* HDU if severe

Postnatal:
* BP monitoring 72hours - transition to longer acting e.g. enalapril if ongoing need
* Continue fluid balance and restriction
* Continue MgSO4 for 24hours PP if running
* Avoid NSAIDs
* Breastfeeding support - NB cabergoline contraindicated
* VTE prophylaxis - clexane, TEDs
* Contraception
* MMH screen
* Investigate if early onset for APLS, adjust other modifiers if present
* Future pregnancy - recurrence 15%, aspirin from 12weeks, UtA doppler at FAS, BP monitoring, consider delivery 39weeks
* Cardiovascular assessment annually
* PN debrief if severe, early onset

Question 47

Periconceptual
Antenatal
Delivery
Postnatal

Answer 47

Periconceptual:
* Counsel risks -

Antenatal:
* MDT

Delivery:
* Aim VB
*

Postnatal:
* Breastfeeding support
* VTE prophylaxis
* Contraception

Question 48

Outline how often urine protein and preeclampsia bloods should be checked in:

Chronic HTN

Gest HTN

PET

Answer 48

• Chronic HTN
  
  • Proteinuria: every visit
  • PET bloods: if BP control worsens or new proteinurina
• Gest HTN:
  
  • Proteinuria: 1x/week
  • PET bloods: 1x/week
• PET:
  
  • Proteinuria: at diagnosis. Repeat daily if non-proteinuric.
  • PET bloods: twice weekly at least

Question 49

HELLP syndrome
Antenatal
Delivery
Postnatal

Answer 49

Antenatal:
* MDT - high risk obs, anaesthetics, neonatal
* Counsel risks - HTN, stroke, eclampsia, low platelets, hepatic and renal impairment, hepatic haematoma and rupture, pulmonary oedema, coagulopathy, VTE, IUGR, abruption, NICU admission, PTB (iatrogenic), stillbirth, maternal mortality
* Bloods - FBC, Cr, LFTs, coags, haemolysis screen, G&H
* BP monitoring - Q4H
* Antihypertensives to aim BP <140/90 - labetalol, methyldopa, nifedipine
* If <34weeks - corticosteroids
* Thromboprophylaxis - TEDs, SCDs
* Monitor for symptom progression - headache, vision changes, swelling, RUQ pain
* Liver USS if worsening pain
* Fluid balance and fluid restrict
* IV MgSo4
* Continuous CTG
* HDU
* MMH screen

Delivery:
* AT DIAGNOSIS
* Most have CS unless later gestation, multiparous, favourable
* 2x IV line, bloods every 6hours, valid G&H with 4units cross matched
* Prepare for PPH - active 3rd stage - concentrated oxytocin infusion, avoid syntometrine. Replace clotting factors accordingly, consider MTP activation
* BP management - POs, IVs if vomiting or severe, epidural (if plts >80)

Postnatal:
* HDU
* BP monitoring 72hours - transition to longer acting e.g. enalapril if ongoing need
* Bloods 6hourly
* Continue fluid balance and restriction
* Continue MgSO4 for 24hours PP if running
* Avoid NSAIDs
* Breastfeeding support - NB cabergoline contraindicated
* VTE prophylaxis - clexane if coags and platelets normal, TEDs, SCDs
* Contraception
* MMH screen
* Investigate if early onset for APLS, adjust other modifiers if present
* Future pregnancy - recurrence 20% PET and 7% HELLP, aspirin from 12weeks, UtA doppler at FAS, BP monitoring, consider delivery 39weeks
* Cardiovascular assessment annually
* PN debrief if severe, early onset

Question 50

You are looking after a patient who is now postpartum with HELLP syndrome with progressive worsening of RUQ pain. You suspect a hepatic haematoma, how do you proceed?

Answer 50

• DRSABCs
• HDU/ICU setting
• MDT - high risk obs, anaesthetic, general surgeons, OT staff, MWs
• Regular cycling observations
• Ensure 2x large bore IVs, consider arterial line and central access
• Bloods - FBC, LFTs, coags, BSL, G&H - cross match at least 4 units
• Liver USS
• Analgesia, keep NBM, IVFs (slow)
• WH clexane if taking
• Aim conservative management, consider embolisation
• If unstable - book for urgent laparotomy, packing, rarely liver resection, activate MTP, cell saver if present
• Document, debrief

Question 51

Epilepsy
Periconceptual
Antenatal
Delivery
Postnatal

Answer 51

Periconceptual:
* Counsel risks - lower seizure threshold (highest risk intrapartum and postpartum), fetal hypoxia during, volume of distribution changes in pregnancy so doses need adjusting. Impacts of medications (some teratogenic - fetal valproate and anticonvulsant syndromes - NTDs, orofacial, cardiac, dysmoprhism, hypoplastic nails/digits
* Review seizure control - types, frequencies, timing of last, precipitants
* Review meds - monotherapy at lowest dose safest but need to balance risks vs benefits. STOP valproate and await control once switched prior to concieving
* 5mg folic acid

Antenatal:
* MDT - high risk obs, neurology, anaesthetics
* Monotherapy at lowest dose possible
* 5mg folic acid
* Early anatomy USS at NT, fetal echo after anatomy
* Serial growth USS from 28weeks
* Baseline medication levels
* Lamotrigiene in particular needs increase as non protein bound and larger volume of distribution

Delivery:
* In hospital with IV line in, not safe for pool
* Aim VB
* Avoid long labour, exhaustion, maternal distress from pain - early epidural
* Keep taking meds - consider IV if poor oral intake, vomiting
* Have seizure terminating medication on standby
* Consider Ddx for a seizure if occurs e.g. eclampsia

Postnatal:
* Sleep hygiene, keep hydrated - someone may need to look after baby to enable adequate sleep
* Don’t bathe baby alone, change on the floor not high surface
* Medication review
* Breastfeeding support - okay with most meds
* VTE prophylaxis - caution re anticoagulants if freuquent seizures as risk of head trauma and ICH
* Contraception - may need to avoid COCP if enzyme inducing

Question 52

Spinal cord injury
Periconceptual
Antenatal
Delivery
Postnatal

Answer 52

Periconceptual:
* Counsel risks - impared cough reflex - aspiration pneumonia, autonomic dyssreflexia (if lesion >T6), spont PTB, precipitous and painless labour, UTIs, bowel dysfunction, abnormal lie, weight gain, pressure ulcers, VTE
* Assess circumstances leading to and level of lesion, level of functioning
* Review meds - often pain concurrent
* Fertility - not affected but may need IUI or IVF if mobility limited

Antenatal:
* MDT - high risk os, neurology, anaesthetics, dieticians, respiratory, neonates, care workers
* Optimise nutrition and weight gain
* Urine cultures for infection, low threshold for ABx prophylaxis if not already
* Bowel hygiene
* BP surveillance
* Serial growth USS
* VTE prophylaxis
* Give advice about feeling for FMs, uterine palpations for contractions, home uterine activity monitor
* May admit from 36weeks and weekly cervical checks
* Advice re autonomic dysreflexia - headaches, flushing, arrhythmia, respiratory distress
* MMH screen

Delivery:
* Aim VB
* Assisted vaginal delivery common for maternal effort, AD risk
* Early epidural even if no pain
* Monitor for autonomic dysreflexia - BP, HR, O2 sats monitoring
* CTG - uteroplacental vasoconstriction in autonomic dysreflexia
* IDUC

Postnatal:
* Breastfeeding support
* VTE prophylaxis
* Contraception - avoid COCP as higher VTE risk
* Social supports

Question 53

You are looking after a patient in labour who has a history of traumatic T6 spinal cord injury. After a cervical exam (where she is reported to be 5cm and stretchy) she becomes tachycardic and hypertensive. You suspect autonomic dysreflexia, how do you proceed?

Answer 53

• Declare emergency
• MDT - senior obs, senior anaesthetics
• IV access
• Site anasthetic (epidural or spinal or CSE) to level T10 to block afferent signals
• IV antihypertensives
• Can also sit up to help blood pool in legs
• Empty bladder and check bowel not impacted
• Keep CTG on
• Can still aim vaginal birth with shortened second stage
• Also do PET screen as differential for HTN

Question 54

Renal transplant
Periconceptual
Antenatal
Delivery
Postnatal

Answer 54

Periconceptual:
* Counsel risks - progression of renal disease, transplant rejection, infertility, miscarriage, stillbirth, PTB, HTN and PET, CS delivery (and injury to transplant), medication effects e.g. steroids - GDM, PTB, adrenal suppression
* Assess underlying disease ?risk ongoing
* Document location of transplant
* Review meds - emphasise relative benefits >risks and importance of adherence. Prednisone, azathiprine, ciclosporin and tacrolimus okay. Defer if mycophenalate
* Baseline renal function, PCR
* Defer pregnancy for 2-3years after transplant, if Cr >130, recent rejection

Antenatal:
* MDT - high risk obs, pbs physicians, renal team, anaesthetics, dieticians
* Continue meds - emphasise adherence, monitor levels
* Vitamin D supplementation
* Monitor Hb, Fe, may need EPO
* Aspirin from 12weeks
* Uterine artery dopplers at anatomy scan
* Serial growth USS
* OGTT, BSL testing if regular steroids
* VTE prophylaxis - clexane if in proteinuric range
* BP surveillance - PET more difficult to diganose if pre-exiting HTN and proteinuria
* Regular urine cultures - ABx prophylaxis if recurrent UTIs
* MMH screen

Delivery:
* Aim VB
* If CS needed to be done by most senior person available, vertical skin incision, liase with transplant team
* Timing of delivery - 38weeks
* May need stress dose hydrocortisone if long term steroids
* Careful fluid balance
* IV prophylaxis for any intrumentals, episiotomty

Postnatal:
* Avoid NSAIDs
* Breastfeeding support
* VTE prophylaxis
* Contraception
* Renal follow up

Question 55

You see a patient at 32weeks with severe RUQ pain. You suspect acute fatty liver of pregnancy. How do you proceed?

Answer 55

Assess:
* Bloods - CBC, renal and electrolytes, LFTs, coagulation, BSL
* USS - upper abdomen, pregnancy
* Exclude other causes - PET, hepatitis, autoimmune liver disease
* CTG

Manage:
* Admit
* MDT - high risk obs, anaestehtics
* 2x IV access
* 2units blood Xmatched
* Correct coagulopathy
* IV glucose for correction of hypoglycaemia
* Hourly observations
* Fluid balance
* Corticosteroids (if <35weeks)
* IV ABX - high risk of sepsis
* May need DDAVP if massive diuresis
* Prepare for urgent delivery once stabilised - caesarean section
* Anticipate higher bloods loss, prepare for MTP
* Post op - HDU, VTE prophylaxis, fluid balance, breastfeeding support, contraception, follow up, counsel low recurrence risk

Question 56

IVDU/Heroin addiction
Periconceptual
Antenatal
Delivery
Postnatal

Answer 56

Periconceptual:
* Counsel risks - miscarriage, PTB, stillbirth, abruption, IUGR
* Refer to CADs, commence opiate substitution or medically supervised withdrawal
* Extended STI screen
*

Antenatal:
* MDT - high risk obs, CADS, MMH team, neonates, social workers, dieticians
* OST - Methadone or buproprion - safer to be on in pregnancy, withdrawal not recommended
* Re-test syphilis 28weeks
* Growth USS

Delivery:
* Aim VB
* Analgesia as needed intrapartum - may have higher requirement

Postnatal:
* Neonatal observation
* Encourage breastfeeding
* VTE prophylaxis
* Contraception
* Ongoing follow up

Question 57

Prolactinoma (macro)
Periconceptual
Antenatal
Delivery
Postnatal

Answer 57

Periconceptual:
* Counsel risks - infertility if not treated, 15% increase in size in pregnancy
* Review medications - usually benefits > risks
* If need surgery recommend treatment prior to pregnancy
* Baseline visual field assessment

Antenatal:
* MDT - high risk obs, endocrine, neurosurgery
* Continue meds - cabergoline or bromocriptine
* No role for PRL surveillance as increased in pregnancy
* Repeat MRI if worsening symptoms
* Transphenoidal surgery in 2nd trimester

Delivery:
* Aim VB

Postnatal:
* Breastfeeding - usually not possible on dopamine agonist
* VTE prophylaxis
* Contraception - avoid oestrogen contaning

Question 58

AMA - how do you counsel?

Answer 58

Counsel - higher infertility, miscarriage, aneuploidy, GDM, HTN and PET, MI, IUGR, stillbirth

Manage - aspirin, MSS, FAS, growth USS, BP surveillance, IOL at term

Question 59

Ehlers Danlos

Answer 59

Periconceptual:
* Assess type
* PIGD as autosomal dominant
* Avoid pregnancy if vascular type
* Counsel risks - joint dislocations, spont PTB, malpresentation if fetus affected, PPH, percipitous labour, uterine rupture and aortic dissection if vascular type

Pregnancy:
* MDT
*

Intrapartum:
* Can have vaginal birth
* Careful positioning of hips in labour, otherwise offer a CS if recurrent dislocation

Postnatal:
*