Michael A Heneghan, MD, MMedSc, FRCPI. Institute of Liver...

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Autoimmune Hepatitis: Management in special Populations Michael A Heneghan, MD, MMedSc, FRCPI. Institute of Liver Studies, King’s College Hospital, London.

Transcript of Michael A Heneghan, MD, MMedSc, FRCPI. Institute of Liver...

Page 1: Michael A Heneghan, MD, MMedSc, FRCPI. Institute of Liver ...static.livemedia.gr/livemedia/documents/al18169_us63_20160321162543... · Autoimmune Hepatitis: Management in special

Autoimmune Hepatitis: Management in special

Populations

Michael A Heneghan, MD, MMedSc, FRCPI.

Institute of Liver Studies,

King’s College Hospital, London.

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Special Populations

Pregnancy

Elderly

Cirrhosis

Ethnic populations

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Amenorrhoea

• Prevalence • 60% on transplant waiting list

• 20% if cholestatic liver disease

• Problem of selection bias and reporting

Mass et al. Transplantation 1996

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Age and Presentation

Gronbaek et al. J Hepatol 2014 Van Gerven Scand J Gastro 2014;49:1245-54

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AIH may present in Pregnancy: Standard Induction Regimens

• Prednis(ol)one

• 0.5-1 mg/kg/day with reducing doses to maintainance of 5-7.5 mg/day

• Budesonide

• 9 mg/day with reducing doses to maintainance of 3 mg/day

• Restrict to patients who are non-cirrhotic

Addition of Azathioprine 1 mg/kg/day when bilirubin < 100 and following measurement of TPMP levels.

EASL Clinical Practice Guidelines: 2015

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Normal Pregnancy

• Palmar erythema

• Spider naevi (60%)

• Increased blood volume and cardiac ouput

• Small oesophageal varices present in up to 50%

• Compression of IVC and azygous flow

• Decreased gallbladder motility

• lithogenicity of bile ( cholesterol synthesis)

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Summary of biochemical changes

Parameter Alteration from non

pregnant state

Albumin/Total protein Decreased

Urea/Uric Acid/PCV Decreased

Alk phos Increase

(Bone/placenta)

Fibrinogen/Chol/Trigl Increased

Bilirubin Increased

Bile acids/AST/ALT/GGT No change

Alpha feto protein HCC/Spina bifida

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Definitions • Low birth weight was defined as <2500 g.

• Small for gestational age (SGA) birth • Birth weight <2 SD below the mean for gestational age

according to the reference curve of estimated foetal growth.

• Gestational age at birth categorized into: • very preterm (<32 weeks),

• moderately preterm (32–36 weeks)

• term (37–44 weeks).

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Swedish Patient Register (PAR) 2006-2011

Variable AIH N = 171 Non-AIH N = 576 642

Induction therapy 66 (38.6%) 3882 (0.7%)

No induction therapy 105 (61.4%) 572 760 (99.3%)

Maintenance therapy 68 (39.8%) 843 (0.1%)

No maintenance therapy 103 (60.2%) 575 799 (99.9%)

No treatment 82 (48.0%) 572 305 (99.2%)

Treatment 89 (52.0%) 4337 (0.8%)

Stokkeland et al Liver International 2015 In press

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Swedish Patient Register (PAR) 2006-2011

Variable AIH N = 171 Non-AIH N = 576 642

Prednisolone 61 (35.7%) 3762 (0.7%)

Budesonide 8 (4.7%) 181 (0.0%)

Azathioprine 52 (30.4%) 641 (0.1%)

No azathioprine 119 (69.6%) 576 001 (99.9%)

Mercaptopurine 2 (1.2%) 52 (0.0%)

Tacrolimus 12 (7.0%) 37 (0.0%)

Cyclosporine 3 (1.8%) 84 (0.0%)

Mycophenolate 0 (0.0%) 10 (0.0%)

Methotrexate 0 (0.0%) 67 (0.0%)

Stokkeland et al Liver International 2015 In press

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Pregnancy and birth outcomes for all women with AIH and population controls in Sweden

AIH N = 171 (%)

Non-AIH N = 576 642 (%)

Crude RR Adjusted RRa

Gestational diabetes

8 (4.7%) 6475 (1.1%) 4.17 (2.12–8.20)

4.35 (2.21–8.57)

Pre-eclampsia 5 (2.9%) 15 744 (2.7%) 1.07 (0.45–2.54)

0.99 (0.41–2.36)

Gestational hypertension

4 (2.3%) 6112 (1.1%) 2.21 (0.84–5.82)

2.23 (0.85–5.88)

Caesarean section

31 (18.1%) 96 622 (16.8%) 1.08 (0.79–1.49)

0.89 (0.62–1.29)

Apgar score at 5 min

7–10 166 (97.1%) 565 605 (98.1%)

Ref = 1 Ref = 1

Low birth weight (<2500 g)

17 (9.9%) 18 844 (3.3%) 3.04 (1.94–4.78)

2.51 (1.51–4.19)

Stokkeland et al Liver International 2015 In press

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Immune tolerance in Pregnancy

H

L

0

5 0

1 0 0

1 5 0

2 0 0

2 5 0

2 0 1 3 2 0 1 4 2 0 1 5 2 0 1 6

A s p a r t a t e T r a n s a m i n a s e

IU

/L

L i c e n c e , K a t a r z y n a

A s p a r t a t e T r a n s a m i n a s e ( I U / L )

H

L

2 5

3 0

3 5

4 0

4 5

5 0

5 5

2 0 1 3 2 0 1 4 2 0 1 5 2 0 1 6

G l o b u l i n

g/

L

L i c e n c e , K a t a r z y n a

G l o b u l i n ( g / L )

Remission in pregnancy followed by post delivery flare

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Immune Tolerance in Pregnancy Lessons from Multiple Sclerosis

• Classically attributed to shift to Th2 dominance

• Increased level of sex hormones

• Immunoregulatory factors in pregnancy include • tolerance-promoting signaling molecules

• pregnancy-specific serum proteins • HLA-G, CD200, Fas-ligand,

• alpha-fetoprotein, and indoleamine 2,3-dioxygenase.

• Finnish MS and Pregnancy Study Group (5000 genes) • Down regulation of HLA G region after delivery in MS

Rouass Friese et al. PNAS 2007

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Other immunological findings in pregnancy and MS activity

• Increased CD56bright NK cells in late pregnancy • (Same prevalence is seen following interferon beta and

daclizumab treatment)

• Increased Tregs prevalence

• All reversed in the postpartum situation

• ? mechanisms for keeping autoreactive T cells in check are enhanced during pregnancy.

• CD56 bright NK cell population • HLA-G-positive and CD4+CD25high regulatory T cells.

• Mechanism is lost immediately after the delivery.

Airas L. Acta Neurol Scand. 2015

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Pregnancy in AIH 1982-2009 81 self-reported in 51women

Live birth

rate

Termination Miscarriage Gestation

<37 weeks

Gestational

flare

Post-partum

flare

Any Flare

Prednisolone

monotherapy 20/27 (74%) 3/27 (11%) 4/27 (15%) 37 (28-40) 2/20 (10%) 7/20 (35%) 8/20 (40%)

Azathioprine

+/-

prednisolone

21/32 (65%) 6/32 (19%) 4/32 (13%) 38 (32-39) 0/32 (0%) 7/32 (21%) 7/32 (21%)

Any therapy

(prednisolone

, tacrolimus,

azathioprine)

42/61 (68%) 10/61 (16%) 8/61 (13%) 38 (28-40) 2/61 (3%) 15/61 (24%) 16/61 *

(26%)

No Therapy 17/20 (85%) 2/20 (10%) 0/20 (0%) 38 (27-39) 3/20 (15%) 8/20 (40%) 10/20 *

(50%)

Westbrook et al. J Autoimmunity 2012

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Foetal outcomes

Live Birth rate Prematurity

<37 weeks

SCBU

Cirrhosis vs. no Cirrhosis

(n=33) (n=48)

19/33 vs. 40/48

p=0.02

5/19 vs. 7/40

p=0.43

4/19 vs. 2/40

p=0.07

Maternal disease remission > 1year

(n=52) vs.

no remission (n=29)

38/52 vs. 21/29

p=0.95

8/38 vs. 4/21

p=0.99

3/38 vs. 3/21

p=0.65

Therapy (n=61) vs. no therapy (n=20)

42/61 vs. 17/20

p=0.25

6/42 vs. 6/17

p=0.07

5/42 vs. 1/17

p=0.66

AIH gestational flare (n=5) vs. no

gestational flare (n=76)

4/5 vs. 55/76

p=0.99

2/4 vs. 10/55

p=0.18

2/4 vs. 4/55

p=0.047

Westbrook et al. J Autoimmunity 2012

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Maternal outcomes Patient Cirrhosis Maternal complication Peak AST Foetal Outcome Maternal Outcome

1 No Died 28 weeks gestation 24 Died Death: sudden death at 25 weeks for

pulmonary hypertension secondary

to thromoembolism

2 Yes Post-partum flare with encephalopathy –

transplanted

217 Alive / healthy Death: 14-months post-partum, from poor

compliance on chronic rejection

3 Yes Post partum flare – very difficult to

control. Significant jaundice mild

ascites.

643 Alive / healthy Transplanted: 3 years post –partum

4 a

4 b

Yes

Yes

Post partum flare with decompensation

(ascites)

Ascites at 10 weeks, unable to control

therefore Termination of pregnancy

647

151

Born 28 weeks –

SCBU, Alive

healthy

NA

Transplanted: 3 years post partum of

second child

5 No Severe flare at 24 weeks, decompensated

with ascites

200 Baby delivered at 28

weeks –

cerebral palsy

Alive

Remains stable on immunosupression

6 Yes Variceal bleed at 31 weeks, controlled

endoscopically

30 Alive healthy, 34

weeks

Death: 7 months post partum secondary to

uncontrollable variceal bleed.

7 Yes Severe Post Partum Haemorrhage Born 32 weeks

needed SCBU

Death: Variceal bleed 1 year post partum,

refused blood transfusion

8 Yes Uneventful pregnancy 28 Healthy Deterioration 12 months post partum, died

whilst having LT assessment

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Autoantibodies may affect outcome

• 42 pregnancies in 22 AIH patients

• 26% rate of adverse pregnancy outcomes

• Medical explanation elucidated in 4 of 11

• 7 unexplained adverse outcomes • associated with antibodies to SLA/LP (odds ratio 51; p < 0.003)

• and Ro/SSA (odds ratio 27; p < 0.02). Of 35 live births,

• 30 children developed normally over a mean observation period of nearly 5 yr.

• Eleven of these had been exposed to azathioprine in utero.

• The rate of serious maternal complications was 9% and a high rate (52%) of postpartum flares was noted.

Schramm et al. Am J Gastro 2006

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US FDA: Categories of Safety

• A Controlled studies show no risk

• B No evidence of risk in humans • Animal findings may show risk (but humans no) Or if no

human studies, animal studies neg

• C Risk cannot be ruled out • Human studies lacking and animal studies are positive for risk

or lacking

• D Positive evidence of risk • Investigational or post-marketing data show risk

• X Contra-indicated

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Alternative therapy in AIH: Considerations for Pregnancy

• Mycophenolate

• Tacrolimus • Levels of 5-8

• Cyclosporine • Levels 100-150

• Sirolimus

• Side effect profile

• Age

• Renal Impairment

• Diabetes

• Compliance

• Cytopaenia

• Combinations acceptable

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Categorisation of commonly used immunosuppressants

• Prednis(ol)one Class B

• Ciclosporine Class C

• Tacrolimus Class C

• Azathioprine Class D

• Mycophenolate Class D

• Sirolimus Class C

• Monoclonals Class C

Heneghan et al. J Hepatol 2008

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Summary of pregnancy outcomes with MMF

• 13 newborns exposed to MMF

• Microtia (12) with auditory canal atresia (9)

• Cleft lip and palate (6)

• Micrognathia (4); hypertelorism (4); ocular coloboma (3);

• Short fingers (2) and hypoplastic nails (2)

• Cardiac defects (Aortic arch or conotruncal defects)

• (EMFO tetrada: Ear, Mouth, Fingers, Ocular/Organ malformation)

Merlob et al. Reprod Toxicol 2009 Anderka et al. Am J Med Genet 2009

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Microtia

Micrognathia

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Abnormal Physiology in Cirrhosis

• Men

• Testosterone

• LH and FSH

• Blunting of Pituitary responses

• Oestrogens

• Prolactin

• Women

• LH and FSH

• Oestrogens

• Blunting of Pituitary responses

Ongoing alcohol use in ESLD also impacts in men and Women

Van Thiel et al. Hepatology 1981

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62 Pregnancies in 29 Women with cirrhosis

• Cirrhosis on biopsy 41/62 (66%)

• Radiology and lab parameters 21/62 (34%).

• Median age at conception was 29 years (range 16-40 years).

• Three patients conceived using IVF

• 21/62 (34%) of pregnancies were unplanned.

• 2 twin pregnancies,(women who had not undergone IVF.

AIH

Alc

Viral

Bil Atr

Genetic

Vascular

Other

Westbrook et al Clin Gastro Hepatol 2011

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Demographics at Conception

• Median MELD 7 (range 6-17),

• Median Meld-Na 9 (6-17),

• Median UKELD 44 (range 36-53)

• Median CP score was 5 (5-8).

• 11 pregnancies occurred in 8 women who had a previous decompensation

• 3 encephalopathy,

• 5 ascites

• 3 variceal bleed

Childs A

Childs B

Missing

Westbrook et al Clin Gastro Hepatol 2011

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62 Conceptions in Cirrhosis

Westbrook et al Clin Gastro Hepatol 2011

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Prognostic Scoring and Foetal Outcome

MELD MELD-Na UKELD CP

Live birth v

miscarriage

or still birth

7(6-15) v 7(6-16)

P=0.88

8(6-15) v 9(8-17)

p=0.45

43(36-50) v 44(40-51)

P=0.45

5(5-8) v 6(5-8)

p=0.29

Live birth v

termination

7(6-15) v 8(6-15)

p=0.64

9(6-14) v 9(7-17)

p=0.28

43(36-50) v 45(37-51)

p=0.46

6(5-8) v 6(5-8)

p=0.24

Gestational week

<37 v > 37

8(6-15) v 6(6-15)

p=0.01

11(6-15) v 9(6-13)

p=0.01

47 (41-50) v 42(39-47)

P=0.01

7(5-7) v 7(5-8)

p=0.02

Caesarean v

vaginal

delivery

7(6-15) v 6(6-15)

p=0.31

9(7-15) v 8(6-13)

p=0.91

43 (36-50) v 42 (20-48)

P=0.29

6(5-8) v 6(5-7)

p=0.86

Neonatal ICU v

ward

10(7-15) v 6(6-15)

p=0.02

7(6-14) vs. 9(6-15)

p= 0.28

48(42-50) v 42(36-48)

P=0.02

7(5-8) v 6(5-7)

p=0.08

Westbrook et al Clin Gastro Hepatol 2011

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Maternal Deaths

Age at

conception

MELD UKELD Live birth Significant pregnancy

related complication

Interval from birth

to death (months)

Transplanted

16 7 43 Yes Yes 16 Yes – 2/12

post partum

34 15 47 Yes No 28 No

33 14 47 Yes Yes 6 No

25 10 48 Yes Yes At delivery No

Westbrook et al Clin Gastro Hepatol 2011

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Predicting outcome at conception in Cirrhotic patients who become pregnant

• UKELD Score

(48,(43-48) v 43, (36-51), p=0.02)

• MELD score

(10,(7-14) v 7,(6-17), p=0.01)

• Associated with an increased risk a significant liver related adverse event for the mother.

• Child Pugh score

(7, (5-8) vs. 5, (5-8) p=0.2).

1 - Specificity

1.0 0.8 0.6 0.4 0.2 0.0

Se

nsit

ivit

y

1.0

0.8

0.6

0.4

0.2

0.0

UKELD MELD

ROC Curve

AU ROC

MELD = 0.798 (95% CI 0.661 – 0.935)

UKELD = 0.801 (95% CI 0.950 – 0.953)

Westbrook et al Clin Gastro Hepatol 2011

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Platelet count as a predictor of varices on endoscopy in the 2nd trimester

• 3 patients had variceal bleed

• All had varices prior to conception

• 1 had prior bleed

• MELD (p=0.06) and UKELD (p=0.08) associated with a trend towards variceal bleeding.

• Women with varices on screening endoscopy more likely to deliver by cesarean when compared with women without (13/18 vs. 4/15, p=0.02).

• No patient with varices had significant bleeding following CS from the presence of abdominal wall varices.

Westbrook et al Clin Gastro Hepatol 2011

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Breastfeeding

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Azathioprine treatment during lactation

AP&T 2008;28:1209-13.

Plasma concentration of 6MP Concentration of 6MP in Milk

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Absolute number of children with various infectious diseases. n = 15 in each group; AZA =

children breastfed by mothers under maintenance AZA treatment, no AZA = children breastfed

by mothers without maintenance AZA treatment; median observation period in AZA = 3.3 years,

in no AZA = 4.7 years.

Sieglinde Angelberger et al. J Crohns Colitis 2011;5:95-100

© 2010 European Crohn's and Colitis Organisation

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Absolute number of children hospitalised due to infections. n = 15 in each group; AZA = children

breastfed by mothers under maintenance AZA. Treatment, no AZA = children breastfed by

mothers without maintenance AZA. Treatment; median observation period in AZA = 3.3 years, in

no AZA = 4.7 years.

Sieglinde Angelberger et al. J Crohns Colitis 2011;5:95-100

© 2010 European Crohn's and Colitis Organisation

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Considerations of Age and Cirrhosis and Ethnicity in AIH

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Feld et al. Hepatology 2005

Age and Prevalence of Symptoms

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Prevalence of Cirrhosis or advanced fibrosis at

diagnosis according to age

Ngu et al. Hepatol 2013:57:2399-2406

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Presence of Cirrhosis at baseline and

Survival

Feld et al. Hepatology 2005

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Survival According to Age and features

associated with Death/Tx

Incomplete

normalization of

ALT at 6 months.

Low albumin at

diagnosis

Age at presentation

≤20 years

>60 years

Ngu et al. Hepatol 2013:57:2399-2406

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Risk factors for HCC development in AIH

Features At

Presentation

Hazard Ratio (CI) p

Jaundice

Variceal Bleed

Cirrhotic

0.26 (0.052-1.32)

8.41 (1.75-40.47)

8.01 (1.64-39.07)

0.105

0.008

0.001

Yeoman et al. Hepatology 2008

10.9/1000 yrs follow-up

6.2% of all patients

12.3% of cirrhotic

Male = Female

After 9yrs of cirrhosis

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Mortality & risk of malignancy in AILD

Ngu et al Hepatology 2012;56:622-629.

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AIH in non-Caucasian populations

Publication

Country

No of Patients Ethnicity Clinical

Observations

Zolfino 2003

UK

12 6 African

5 Asian

↓ Responsiveness

↑ Transplant

Falalla 2010

Saudi Arabia

33 Middle East ↓ Responsiveness

↑ Cirrhosis

Choudhuri 2005

India

38 Indian ↑ Cirrhosis

All type 1 AIH

Toda 1997

Japan

317 Japanese ↑ Responsiveness

↓ Cirrhosis

Peng 2014

Northern China

83 Chinese 50% Definite AIH

Minuk 2008

Canada

33 First Nation ↑ Fibrosis

↑ Inflammation

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Take Home Messages

Pregnancy possible

Considerations around Immunosuppression

Considerations around cirrhosis

Counselling pre-conception

Cirrhosis as a special population

Age

Ethnicity

Screening