Post on 16-Apr-2018
Biliary system and liver: new insights from immune system for
understanding the natural history, therapy and outcomes
AISF Annual Meeting 2016 Rome
Ana Lleo, MD PhDLiver Unit and
Center for Autoimmune Liver DiseasesHumanitas Clinical and Research Center
ana.lleo@humanitas.it
Il sottoscritto dichiara di non aver avuto negli ultimi 12 mesi conflitto d’interesse in relazione a questa presentazione
e
che la presentazione contiene discussione di farmaci in studio o ad uso off-label
An interdisciplinary branch of the biomedical field supported by three main pillars: benchside, bedside and community.
The goal of TM is to combine disciplines, resources, expertise, and techniques within these pillars to promote enhancements in prevention, diagnosis, and therapies.
Translational Medicine
European Society for Translational Medicine
An interdisciplinary branch of the biomedical field supported by three main pillars: benchside, bedside and community.
The goal of TM is to combine disciplines, resources, expertise, and techniques within these pillars to promote enhancements in prevention, diagnosis, and therapies.
Translational Medicine
European Society for Translational Medicine
TURNING BASIC RESEARCH INTO MEDICINES AND TREATMENTS
PBC
From Cirrhosis to Cholangitis
(1) the name ‘primary biliary cirrhosis’ should be changed [as advocated by Dame Sheila Sherlock in 1959] since the majority of patients are free of cirrhosis at the time of diagnosis and the the disease has a good prognosis
(2) the acronym ‘PBC’ should be kept if possible (3) a simple and short term should be used as long as the exact
pathogenesis of primary biliary cirrhosis remained undefined and, therefore, an ‘ideal’ replacement is not available
European Association for the Study of the Liver (EASL) American Association for the Study of Liver Disease (AASLD)
American Gastroenterological Association (AGA) Asian Pacific Association for the Study of the Liver (APASL)
1. Primary Biliary Cholangitis (PBC) is an autoimmune liver disease that predominantly affects adult women and leads to destruction of intrahepatic bile ducts and eventually biliary cirrhosis
2. multi-lineage loss of tolerance to the E2 subunit of the pyruvate dehydrogenase complex (PDC-E2): presence of highly specific anti-mitochondrial antibodies (AMA) and circulating autoreactive T cells, both directed against components of the inner mitochondrial membrane, mainly PDC-E2.
3. genetic susceptibility and environmental factors that modify the auto-antigen motif contribute to the breakdown of tolerance
Primary Biliary Cholangitis
1. Primary Biliary Cholangitis (PBC) is an autoimmune liver disease that predominantly affects adult women and leads to destruction of intrahepatic bile ducts and eventually biliary cirrhosis
2. multi-lineage loss of tolerance to the E2 subunit of the pyruvate dehydrogenase complex (PDC-E2): presence of highly specific anti-mitochondrial antibodies (AMA) and circulating autoreactive T cells, both directed against components of the inner mitochondrial membrane, mainly PDC-E2.
3. genetic susceptibility and environmental factors that modify the auto-antigen motif contribute to the breakdown of tolerance
Primary Biliary Cholangitis
1. Primary Biliary Cholangitis (PBC) is an autoimmune liver disease that predominantly affects adult women and leads to destruction of intrahepatic bile ducts and eventually biliary cirrhosis
2. multi-lineage loss of tolerance to the E2 subunit of the pyruvate dehydrogenase complex (PDC-E2): presence of highly specific anti-mitochondrial antibodies (AMA) and circulating autoreactive T cells, both directed against components of the inner mitochondrial membrane, mainly PDC-E2.
3. genetic susceptibility and environmental factors that modify the auto-antigen motif contribute to the breakdown of tolerance
Primary Biliary Cholangitis
1. Primary Biliary Cholangitis (PBC) is an autoimmune liver disease that predominantly affects adult women and leads to destruction of intrahepatic bile ducts and eventually biliary cirrhosis
2. multi-lineage loss of tolerance to the E2 subunit of the pyruvate dehydrogenase complex (PDC-E2): presence of highly specific anti-mitochondrial antibodies (AMA) and circulating autoreactive T cells, both directed against components of the inner mitochondrial membrane, mainly PDC-E2.
3. genetic susceptibility and environmental factors that modify the auto-antigen motif contribute to the breakdown of tolerance
Primary Biliary Cholangitis
Primary Biliary Cholangitis
1. Primary Biliary Cholangitis (PBC) is an autoimmune liver disease that predominantly affects adult women and leads to destruction of intrahepatic bile ducts and eventually biliary cirrhosis
2. multi-lineage loss of tolerance to the E2 subunit of the pyruvate dehydrogenase complex (PDC-E2): presence of highly specific anti-mitochondrial antibodies (AMA) and circulating autoreactive T cells, both directed against components of the inner mitochondrial membrane, mainly PDC-E2.
3. genetic susceptibility and environmental factors that modify the auto-antigen motif contribute to the breakdown of tolerance
PBC
Area Year Patients(No.)
Prevalence(per mln)
Incidence(per mln/yr)
Age(years)
Sex(M:F)
Europe 1984 569 23 54 54 1:10Sweden 1985 111 151 13.3 55 1:6Newcastle, UK 1989 347 154 19 58 1:9Ontario, Canada 1990 225 22 3.3 59 1:13Victoria, Australia 1995 84 19 - - 1:11Estonia 1995 69 27 2.3 - 1:22Newcastle, UK 1997 160 240 22 66 1:10Norway 1998 21 146 16 - 1:9Minnesota, USA 2000 46 402 27 - 1:8Newcastle, UK 2001 770 251 31 - 1:10Victoria, Australia 2004 249 51 - 61 1:9Japan 2005 9761 78 - - 1:9
Canada 2009 137 227 30 53 1:5
Geoepidemiology of PBC
Zhang, Lleo, et al, Dig Dis 2015
Administrative databases
LOMBARDIA:Inhabitants at 1-Jan-2010: 9.742.676
DENMARK: Inhabitants at 1-Jan-2010: 5.534.738
(2000-2010)
Sex ratio
LOMBARDIA:Inhabitants at 1-Jan-2010: 9.742.676
DENMARK: Inhabitants at 1-Jan-2010: 5.534.738
M:F RATIO1:2
M:F RATIO1:4
Lleo A, et al., submitted
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
2970 2373 2077 1851 1634 1390 1185 983 781 5 52 297 N umber at risk
95% CI Survival function
Survival from diagnosis
86% (CI 85%-87%) at 1 year70% (CI 69%-72%) at 5 years61% (CI 59%-64%) at 10 years
LOMBARDIA
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 108 120months
722 575 473 396 321 259 198 135 88 42 3 Number at risk
95% C I Survival function
Survival from diagnosis
87% (CI 84%-89%) at 1 year 67% (IC 63%-71%) at 5 years 54% (IC 48%-60%) at 10 years
DENMARK
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
897 627 516 442 382 3 24 273 230 173 1 20 64Maschi2073 1746 1561 1409 1252 1 066 912 753 608 4 32 233Femmine
Number at risk
95% CI 95% CIFemale Male
Survival from diagnosis
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
897 627 516 442 382 3 24 273 230 173 1 20 64Maschi2073 1746 1561 1409 1252 1 066 912 753 608 4 32 233Femmine
Number at risk
95% CI 95% CIFemale Male
Survival from diagnosis
Lleo A, et al., submitted
Survival rate
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
2970 2373 2077 1851 1634 1390 1185 983 781 5 52 297 N umber at risk
95% CI Survival function
Survival from diagnosis
86% (CI 85%-87%) at 1 year70% (CI 69%-72%) at 5 years61% (CI 59%-64%) at 10 years
LOMBARDIA
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 108 120months
722 575 473 396 321 259 198 135 88 42 3 Number at risk
95% C I Survival function
Survival from diagnosis
87% (CI 84%-89%) at 1 year 67% (IC 63%-71%) at 5 years 54% (IC 48%-60%) at 10 years
DENMARK
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
897 627 516 442 382 3 24 273 230 173 1 20 64Maschi2073 1746 1561 1409 1252 1 066 912 753 608 4 32 233Femmine
Number at risk
95% CI 95% CIFemale Male
Survival from diagnosis
0.2
5.5
.75
1
0 12 24 36 48 60 72 84 96 1 08 120months
897 627 516 442 382 3 24 273 230 173 1 20 64Maschi2073 1746 1561 1409 1252 1 066 912 753 608 4 32 233Femmine
Number at risk
95% CI 95% CIFemale Male
Survival from diagnosis
Lleo A, et al., submitted
Survival rate
Factor Hazard Ratio 95% Confidence Interval
Male sex 2,36 2,08 2,69
Age at diagnosis 1,06 1,06 1,07
Year of diagnosis 1,29 1,24 1,34
International data base
Since 20101379 patients
Since 20124845 patients
www.uk-pbc.com www.globalpbc.com
To assess the proportion of patients achieving:
– ALP <1.67x ULN (& ≥15% reduction)
– bilirubin ≤ULN
ResponderNon-Responder
Lammers W, Lleo A et al. Gastroenterology. 2014
The Global PBC Study Group (N=4845) confirmed ALP <1.67 xULN and normal bilirubin after 1 year of UDCA highly predictive of outcome1
Prognosis: surrogate end-points
Response to UDCA and symptoms are related to sex and age at presentation.
Men were significantly less likely to have responded to UDCA than women; male sex was an independent predictor of nonresponse on multivariate analysis.
Lowest response rates to UDCA in those younger than age 30
Carbone M et al. Gastroenterology. 2013
Prognosis: sex and age
Gender differences in the age-related likelihood of achieving UDCA response criteria.
Male
Female
Long-term prediction of end-stage liver disease in PBC
Scoring system
Carbone M et al. Hepatology. 2015 Lammers W et al. Gastroenterology. 2015
1. Males with PBC have worse prognosis and survival rates and seem to be more frequent than previously expected
2. ALP is a good surrogate marker of outcome.
Epidemiology
PBC
PBC
- Geo-epidemiology of PBC prevalence
- Local clustering
- Risk factors
- Experimental evidence for a role of xenobiotics, infectious agents
ENVIRONMENTALFACTORS
GENETICFACTORS
Etiopathogenesis of PBC
- Familial clustering
- High concordance rate of PBC in monozygotictwins
- Polymorphisms associated with susceptibility and progression
Genetics of PBC
Risk variantsHLA
IL12A IL12RB2
IRF5IKZF3/ORMDL3
SPIB
536 Canadian & US PBC vs. 1536 controls (300K SNPs)PLUS 457 Italian PBC vs. 947 controls (1Mb SNPs)
Invernizzi, Italian PBC Genetics Study Group, et al. Nat Genetics, 2010
Genetics of PBC: list of genes
Webb, et al. J Autoimmun, 2016
Genetics of PBC: pathways
Cordell, Italian PBC Genetics Study Group, et al. Nat Commun, 2015
PBC
Apoptotic cholangiocyte
Apoptotic NON-cholangiocyte
Odin JA, J Clin Invest 2001
Intact PDC-E2
Excess glutathione
Reduced environment
glutathione
Oxidated PDC-E2
PDC-E2 remains immunologically active during apoptosis in BECs
Lleo A, Hepatology 2009
Non apoptotic HIBEC
*
*
Lleo A, Hepatology 2009
Non apoptotic HIBEC
*
*
HIBEC HeLa CACO-2 Human keratinocytes Human bronchial cells
0
1000
2000
3000
4000 ***TN
F (p
g/m
l)
Figure 3. Macrophages from PBC cultured withapoptotic bodies from HIBEC secrete pro-inflammatory cytokines in the presence of AMA.MDMΦ from patients with PBC or healthy controls(HC) were cultured with apoptotic bodies and antibody(AMA IgG or IgG control). The triad of MDMΦ frompatients with PBC, but not from controls, apoptoticbodies from HIBEC cells, and AMA leads tosignificantly increased secretion of TNF-α comparedto IgG control. ***p<0.001, based on a two tailed Mann-Whitney test with 95% CI.
MDMФ PBC PBC PBC HC PBCAb AMA IgG ctr AMA AMA AMABlebs HIBEC HIBEC Kerat HIBEC HIBEC
Other - - - - anti-CD16
PBC HC M1 HC0
1000
2000
3000
4000***
*
ns
TNF
(pg/
ml)
Figure 4. Stimulation of PBC macrophages in thepresence of AMA and HIBEC apoptotic bodies is aconsequence of M1 polarization. Comparison of TNFαsecretion from MDM from patients with PBC (n = 8)and healthy controls (n = 8) after M1 polarization (HCM1), and untreated (HC) cultured with HIBECapoptotic bodies in the presence of AMA. (***p<0.001,*p<0.05). For full M1 polarization, MDM from healthycontrols were stimulated with 100 U/ml IFN-γ(Boehringer Ingelheim) and 1 ng/ml LPS (Cambrex)during the last 24 h of culture.
Lleo A, Hepatology 2010
1. Following apoptosis human BECs translocate PDC-E2 immunologically intact into the apoptotic bodies
2. Monocyte derived macrophages (MDMf), from patients with PBC to produce pro-inflammatory cytokines in response to biliary apotopes in the presence of AMAs.
Biliary epithelial cells and macrophages
Trypsin digestionIE fractionation
LC-MS/MSHiBEC n=4
BrEPC n=6
HRPTEpiC n=6
ISOLATIONOF APOPTOTIC
BODIES
STATISTICAL COMPARISON OF
PROTEIN INVENTORIES DIFFERENCIAL
PROTEINLIST
Shotgun proteomic analysis of apoptotic bodies
Apoptotic bodies
HiBEC HRPTepiC BrEPC
Lleo A, Hepatology 2014
LRP1
RAB11A ANXA6
Lleo A, Hepatology 2014
PBC
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 containing apoptotic
bodies
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 containing apoptotic
bodies
AMAs
Immune complex
formation
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 containing apoptotic
bodies
AMAs
Immune complex
formation
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 containing apoptotic
bodies
AMAs
Immune complex
formation
Phagocytocis ↓
Proinflammatory cytokine secretion
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
Lleo A, et at Hepatology 2009Lleo A, et at Hepatology 2010
NORMAL APOPTOTIC
CHOLAGIOCYTE
PDC-E2 containing apoptotic
bodies
AMAs
Immune complex
formation
Phagocytocis
Proinflammatory cytokine secretion
PDC-E2 GLUTATHIOLATION
Intact PDC-E2
1. BECs apoptotic bodies2. Macrophages from PBC patients3. AMA
Lleo A, J Hepatol 2012
PBC: multi-faceted pathophysiology
PBC
UDCA in a dose of 13-15 mg/kg/day orally is recommended for patients with PBC who have abnormal liver enzyme values regardless of
histologic stage (Class I, Level A).
Is there need for new therapies in PBC?
Pares A, Gastroenterology 2006
Author Endpoint criteria Non-response
Barcelona ALP 40% decrease or normalization 39%
Paris IALP < 3 x ULNAST< 2 x ULNBil < 1 x ULN
39%
Paris IIALP < 1.5 x ULNAST< 21.5x ULN
Bil < 1 x ULN52%
Toronto ALP < 1.67 x ULN 43%
Primary Biliary Cholangitis: the future?
Obeticholic acid (Waiting for registration)
Bezafibrate in combination with UDCA in PBC. Phase 3.
Ustekinumab in patients with PBC who had an inadequate response to UDCA
Apical Sodium-dependent Bile Acid Transporter Inhibitor (ASBTi), open label.
UDCA plus budesonide versus UDCA alone in PBC
High-protein high-fiber diet in patients with PBC
Abatacept to treat PBC (CTLA-4)
Umbilical cord mesenchymal stem cells for patients with PBC
IBAT Inhibitor A4250 for Cholestatic Pruritus
ClinicalTrials.gov
IL-12
IL12 Genetic defect
Anti-IL12 Clinical trial
Ongoing trials
Nuclear Receptors (FXR, PPARs):at the crossroad of metabolism, inflammation and regeneration
Karpen, Trauner J Hepatol 2010
Farnesoid Receptor (FXR) protects against toxic effects of hydrophobic bile acids
Courtesy of U. Beuers
POISE: Significant Reductions in ALP Within 2 Weeks
* p-values from an ANCOVA model with baseline value as a covariate and fixed effects for treatment and randomization strata factor.Data are least squares mean(SE)
*p<0.0001 vs. placebo
% Drop inALP
Obeticholic Acid
Fibrates
Bile duct protection
Nakai et al, Am J Gastroenterol 2000Honda et al, Hepatology 2013
UDCA
UDCA+BF
UDCA
UDCA+BF
ALP (range 35-118)
Bil tot (mg/dl) PT INR MELD OCA
Apr 2012 932 1.77 0.89 4.2 -Dec 2013 713 1.82 1.36 8.2 10 mgMar 2014 654 1.78 1.55 10.3 10 mgJun 2014 300 3.15 1.30 10.5 10 mgSep 2014 264 3.00 1.50 12.0 10 mg
Female, DOB 22-Dec-1967PBC Stage IV - portal hypertension – UDCA 14 mg/kg
Clinical Case
June 2015: OLT
PBC
Conclusions
PBC
Conclusions- UDCA non-responders have a
poor prognosis
- Male and very young women have lower response to UDCA
- Male have lower survival rates than women
- ALP can be used as surrogate marker of outcome
PBC
Conclusions
- Genetics of PBC, the mechanisms of injury of BECs, and the immune response may offer important therapy opportunities
- Cholestasis is an important modifier of the disease process and may drive ongoing bile duct destruction after an initial immune response
- LOTS OF DATA AND TIME
- UDCA non-responders have a poor prognosis
- Male and very young women have lower response to UDCA
- Male have lower survival rates than women
- ALP can be used as surrogate marker of outcome
PBC- There is need for new therapies in PBC
- OCA and Fibrates seem to offer realistic alternatives to UDCA
Conclusions
- Genetics of PBC, the mechanisms of injury of BECs, and the immune response may offer important therapy opportunities
- Cholestasis is an important modifier of the disease process and may drive ongoing bile duct destruction after an initial immune response
- LOTS OF DATA AND TIME
- UDCA non-responders have a poor prognosis
- Male and very young women have lower response to UDCA
- Male have lower survival rates than women
- ALP can be used as surrogate marker of outcome
Acknowledgments
Humanitas Clinical & Research CenterSavino Bruno
Università degli Studi di Milano-BicoccaPietro Invernizzi
University of California - DavisM. Eric Gershwin
Università degli Studi di Milano - Ospedale San PaoloMassimo Zuin