sle&pregnancy prs2

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SLE and Pregnancy Syed Atiqul Haq Professor of Medicine-Rheumatology BSM Medical University, Dhaka, & APLAR-COPCORD Coordinator

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Page 1: Sle&pregnancy prs2

SLE and Pregnancy

Syed Atiqul HaqProfessor of Medicine-RheumatologyBSM Medical University, Dhaka, &

APLAR-COPCORD Coordinator

Page 2: Sle&pregnancy prs2

Basic Layout

Background

Management

Page 3: Sle&pregnancy prs2
Page 4: Sle&pregnancy prs2

Background

Effects on fertility

Effects of SLE on pregnancy

Effects of pregnancy on SLE

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Effects On Fertility

• Fertility of SLE patients usually unaltered

• Factors lowering fertility– Renal failure– Cyclophosphamide– Very active disease– Anti-phospholipid antibodies (aPLs) in high titers

– High dose steroid

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On Fetal Outcome

On Maternal Outcome

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Fetal Outcome

Effects Risk Factors

Abortions (6%-35%)

Stillbirths (4%-22%)

•Active lupus nephritis•Previous history of fetal death•The presence of the aPLs

IUGR (9-35%) Hypertension, pre-eclampsia, steroid

Prematurity (40-50%) Hypertension, pre-eclamsia

PROM Steroid treatment

NLE syndrome (5%)

CHB (1.7%)

Anti-Ro, anti-La

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Maternal Outcome

Effects Risk Factors

Toxemias DiabetesLN (30%)HypertensionToxemia in previous pregnancyThrombocytopeniaaPLs

HypertensionDiabetesInfections, UTI

Steroid treatment

Maternal death (1%, in ’60s 20%)

LN

Pulmonary hypertension

Cardiomyopathy

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Effects of Pregnancy on SLE

• Flare of disease activity during

– Any trimester of pregnancy (≈ 60%)

– Postpartum

– Commonly mild

– Severe renal flare if LN active during conception

• Permanent loss of renal function in a small proportion

• No change in the long term course

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Management

Family planning & contraception

Patient in remission

Active disease & flares

Delivery

Puerperium and Lactation

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Family Planning

• The best time for conception: after a 6-

12 months of cytotoxic-free remission

• Incidence of a flare with conception

after remission is 10% or less

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Contraception

• Mechanical barrier methods are safe

and effective, albeit less so than OCPs

• Intrauterine devices controversial

– Infections: endometritis, PID

– Perforation

– Menorrhagia

• Low estrogen contraceptive pills

Page 18: Sle&pregnancy prs2

Oral Contraceptives• Contraindications:

– aPL, other thromboembolic diseases

– Highly active disease

– Migraine

– Raynaud’s phenomenon

– FH of breast cancer

• Specific indication:

– Cyclophosphamide therapy

• Mitigates against gonadotoxicity

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Evaluation

Treatment

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Follow-up Schedule

• Monthly up to 28 weeks

• Fortnightly 28 to 32 weeks

• Weekly afterwards

• More often in patients with active disease

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Evaluation at First Visit

Initial visit: Thorough evaluation of disease activity-

• A full history and examination, BP

• Routine urinalysis

• CBC and platelet count

• Serum creatinine

• A 24 hour urinary total protein, CCr

• Anti-ds-DNA, anti-Ro and –La, aPLs

• Fasting blood glucose if at high risk

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Evaluation at Subsequent Visits

• History and examination: detect flares, BP

• Routine urinalyses

• Blood counts incl. platelet, Hb%, ESR

• From 28 weeks biophysical profile (BPP) scoring

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Additional Tests at End of Each Trimester

Urine culture

Urine protein:creatinine ratio

Serum creatinine

Anti-ds-DNA

aCL

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Anti-Ro/La Positive Mother

• FHR at each visit from 20 weeks

• Fetal echocardiography:

– Weekly 16 – 24 weeks

– Fortnightly 24 – 32 weeks

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Sheet Anchor• Patient and family education & counseling

• Drugs:– Folic acid 400 µg/d during first trimester

– HCQ: 4 to 6 mg/kg/d throughout pregnancy

– Aspirin: 75 mg/d up to 38 weeks

• History in a previous pregnancy of

– Fetal loss after the 1st trimester

– IUGR

– Early onset pre-eclampsia requiring delivery before 32 weeks

• Nephritis

• aPLs

• (Aspirin may be continued throughout pregnancy and delivery if there is

H/O MI/stroke.)

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Anti-phospholipid Ab Syndrome

• Low dose aspirin

• LMWH or UFH– Women with prior pregnancy complications but no

thrombosis

• LMWH (0.5mg/kg twice daily) or UFH (10,000 IU twice daily)

– Women with previous history of thrombosis

• LMWH (1mg/kg twice daily) or UFH (Adjusted dose to prolong

the APTT to twice control)

• Calcium supplement (1.5 gm daily)

• Axial exercise

• Prednisolone has no added benefit

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Classification of Flares

Mild

Moderate

Severe

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Mild Flares

• Maximizing dose of HCQ to 6 to 6.5 mg/kg

• Prednisone/prednisolone: 0.1 – 0.3 mg/kg/day

– Tapered off if full remission achieved quickly

– Avoided or used in low dose in 1st trimester

• Mildest flares: may be treated initially with

– Sunscreen

– topical steroid

– paracetamol

– NSAIDs (late first and second trimesters)

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Moderate Flare

• Maximizing dose of HCQ

• Prednisone/Prednisolone: 0.3 – 0.5 mg/kg

– Attempt at gradual taper after full remission

• AZT or Cys A

– Flare recurrence with prednisone <7.5 mg/d

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Severe Flare

• Prednisone/Prednisolone: 1 mg/kg/day

– May be preceded by pulse MP

• Azathioprine: 1.5 to 2 mg/kg/day or

cyclosporin A 3 -- 4 mg/kg/day

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Steroid Maintenance Till Term

• Patients requiring maintenance

steroid before conception

• Recurrent mild flares

• Moderate to severe flares

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Cyclophosphamide

• Indications:

– Acute anuric renal failure

– Alveolar heamorrage

– Refractory class IV nephritis

• Amniocentesis and karyotyping

• High risk of spontaneous abortion

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Delivery Setting

• In a hospital with neonatal ICU

• Vaginal route preferred

• Routine caesarian delivery not recommended

• Indications for caesarian section

– As for women without lupus

– High incidence of non-reassuring BPP score leading to

caesarian delivery

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Steroid Stress Coverage: Indication

• Treatment with systemic steroid within 2

years of the anticipated delivery

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Steroid Stress Coverage: Protocol

• Day of delivery: Hydrocortisone 100 mg I/V just prior to onset of delivery and 8 hourly

• 2nd day: 50 mg 8 hourly

• Day 3 onwards:– No steroid if not on steroid before delivery

– Restart oral dose used before delivery

• If on more than 75 mg of prednisone daily– appropriate hydrocortisone equivalent for days 2 and 3

– then resume previous oral dose

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Post-partum Flare

• Risk groups:– Active disease at conception

– Significant end-organ damage

• Detection:– Focused history & examination

– Lab tests:• Urinalysis

• blood counts

• Serum creatinine

• Urine protein/creatinine ratio

• Anti-dsDNA

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Lactation• Safe drugs:

– short acting NSAIDs (not aspirin)

– prednisolone <15 mg/d

• Higher dose: after morning feed and next feed after 4 hrs

– HCQ

– Warfarin

– Heparin

• Drugs to be avoided

– AZT

– CysA

– MTX

– Cylophosphamide

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Conclusion

Safe motherhood possible with

• Increased awareness of the potential problems for mother and fetus

• Meticulous multidisciplinary follow up

• Effective disease control

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Page 46: Sle&pregnancy prs2

Neonatal Lupus Syndrome (NLE)

• Congenital heart block (CHB) – 1.7%

– CCHB carries 15 to 30% mortality

• Transient cutaneous lupus lesions

• Cytopenias

• Hepatic, and other systemic manifestations

Page 47: Sle&pregnancy prs2

Causes of Maternal Death

Pulmonary hypertension

Pulmonary embolus

HELLP syndrome

Cardiomyopathy

Severe renal flare

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Flare During Pregnancy

• Usually mild with arthritis and rash

• Major organ flares may occur

– Kidneys 40%: in LN patients

• 50-60% if active during conception

• 7-10% if quiescent during conception

– Central nervous system 5%

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Counselling

• Target: patient and family• Issues

• Chances of flare• Fetal loss• Prematurity• IUGR• Hypertension• Preeclampsia• Need for rigorous follow-up

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Indications for Elective Abortion

Severe compromise of function of

• Kidneys

• Myocardium

• Lungs

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Mild Moderate

Muco-cutaneous Butterfly rash

Photosensitivity

Maculopapular

Mild oral ulcer

Mild DLE

Severe oral ulcer

Severe DLE

Diffuse SCLE

Lupus profundus

Skin vasculitis

Articular Arthralgia, mild polyartritis

Disabling polyarthritis

Therapeutic Classification

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Mild Moderate Severe

Renal Class I, IIa Class IIb, LN Class III, IV LN

Neuro-psychiatric

Lupus headache

ChoreaPeripheral neuropathy

Delirium

Encephalitis

Psychosis

Coma

Myelopathy

Therapeutic Classification (contd.)

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Mild Moderate Severe

Hematological Platelet30 to 100,000

Platelet

15 to 30,000 (preg: 30 to 100,000)

Hemolytic anemia

Lupus adenitis

Platelet <15,000

(preg: <30,000)

Cardiopulmonary Pleurisy Pleural effusion

Pneumonitis

Pericarditis

Mild myocarditis

Severe pneumonitis

Pulmonary hemorrhage

Cardiac tamponade

Severe myocarditis

Therapeutic Classification (contd.)

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Mild Moderate Severe

Gastro-intestinal

Mild hepatitis

Pancreatitis

Peritonitis

Severe hepatitis

Colitis

Protein-losing enteropathy

Mesenteric vasculitis

Miscellaneous Responsive fever

Fatigue

Myalgia

Refractory/high fever

Therapeutic Classification (contd.)

Page 55: Sle&pregnancy prs2

Pre-eclampsia vs. Renal Flare

Feature Pre-eclampsia Lupus flare

Arthritis, rash -- +

Active sediment in urine

C3, C4 ↓ ↑

Anti-dsDNA = ↑

Uric acid, liver enzymes ↑ =

Urinary calcium ↓ =

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Treatment of Heart Block

• Dexamethasone 4 mg/day– Partial:

• If reverts or doesn’t progress: till delivery• If progresses to complete: taper

– Complete:• If reverts to partial: till delivery• If doesn’t revert after 6 weeks: taper