Post on 10-Oct-2020
Valutazione non invasiva e
misurazione diretta della
pressione portale
• Background
• Impact of the therapy
• Diagnosis and scores
Wilma Debernardi Venon
UOADU Gastroepatologia
Molinette - Torino
Liver fibrosis and Natural History
Cirrhosis
Chronic hepatitis
Health liver
Injury
chronic tissue damage, inflamation, fibrogenesis
tissue ipoxia, angiogenesis
liver dysfunction
carcinogenesis
Portal Hypertension
Systemic disease
Esophageal varices
Ascitis
Refractory ascitis
HRS
Alcoohol
virus
iron
autoimmunity
Hemodynamic Factors in the Pathophysiology
of Cirrhotic Portal Hypertension
antiangiogenetic drugs
Antifibrotic drugs
Statins ?
Antioxidants ?
BB + vasodilators
carvedilol
splanchnic vasoconstrictors
terlipressin, somatostatin
non selective BBlockers
Anticoagulation ?
Etiologic treatments
TIPS
Portal Pressure
Diet
Steroids
Antivirals
Hepatic Fibrosis and Reversibility
fibronectin
Extensive collagen cross linking
Elastin
Paucicellular ECM
MMP expression
Resistance to apoptosis
expression lysyl oxidase 2-->
fibrosis reversibility
advanced stages
Irreversibility ?
Friedman SL. J Hepatology 2015
Classification of chronic liver disease based on histological,
clinical, hemodynamics and biological parameters
Rebleeding,
Refractory ascites
HRS/AKI
SBP
> 16-20
1 yr mortality 1% 3% 10-30% 60- 100%
Main outcome decompensation, decompensation HCC, mortali ty
to prevent HCC, varices HCC
AT1 receptor blockers
statins B Blockers
Antiviral therapy
TIPS
…. more or less severe cirrhosis? clinical decompensation?
regression of cirrhosis? response to antiviral therapy?
Sethasine S and Garcia Tsao. Hepatology 2012
Fibrosis area= area of fibrosis/ total biopsy area
• Impact of therapy
47 cirrhotics,
peg-Inf + Riba, 48 w,
HVPG 0-6 months
Roberts S. Am J Gastr 2006
96 patients, INF + Riba
Score F4
Liver biopsy
Metavir 42
18/96 (18.7%): regression of fibrosis
0 clinical events
Transplant-free survival rate at 10 yrs:
100% vs 74% without regression
Mallet V. Ann Int Med 2008
The relationship of regression of cirrhosis
to outcome in chronic hepatitis C
HCV
Prospective cohort, 933 pts,Fibrotest and
fibroscan
Regression of fibrosis=
minimum 0.20 decrease test= -1 Metavir stage
At 10 yrs, 415 pts
15 new cirrhosis, HCC (4 vs 13) Poynard T. J Hepatology 2013
Association Between Severe Portal Hypertension and Risk of Liver
Decompensation in Patients with Hepatitis C, Regardless of Response to Antiviral
Therapy
Liver decompensation at 1, 5 and 7 yrs: 3%, 19% e 22%
Lens L. Clin Gastr Hepat 2015
n=5 n=5 n=2 n=3
(+10)
CPT B CPT C
12 wk (n=30)* 24 wk (n=29)* 12 wk (n=23)* 24 wk (n=26)*
*Missing FU-4: n=2 CPT B 12 wk; n=4 CPT B 24 wk; n=2 CPT C 12 wk; n=7 CPT C 24 wk.; discontinuation 13/337 (4%)
Death in 10 for decompensation; 6 LTs
LABORATORY RESULTS: MELD SCORE
CHANGE FROM BASELINE TO FOLLOW-UP WEEK 4
36% not improved 35% not improved
Charlton et al Gastroenterology 2015
Charlton et al. Gastroenterology; 2015.
SOFOSBUVIR+LEDIPASVIR+RBV FOR RECURRENT HCV:
MELD SCORE CHANGE FROM BASELINE TO POST-TREATMENT WEEK 4
33% not improved
or worse
30% not improved
or worse
60% not improved
or worse
33% not improved
or worse
HVPG Change Over Time
Afdhal, EASL, 2015, LP13
There were clinically meaningful improvements in portal hypertension in addition to
improvements in liver biochemistry, CTP and MELD scores
The effect of SVR12 and viral suppression on HVPG is being monitored at 1 year post-
treatment
Observation Period in Patients with
BL HVPG ≥12 mmHg* (24 weeks) Changes After Treatment in Patients
with BL HVPG ≥12 mmHg (n=33)
SOF+RBV in Compensated and Decompensated Cirrhotics with Portal Hypertension
-30
-20
-10
0
10
20
30
40
n=2
HV
PG
Ch
an
ge (
%)
n=2 a
30
20
10
0
-10
-20
-30
-40
-50
-60
-70
-80 H
VP
G C
han
ge (
%)
Patients with >20% decrease (8/33)
Baseline MELD Score <10 ≥10
aPatients with HVPG ≤12 mm Hg at end of treatment
*No patient had HVPG ≤12 mm Hg at end of observation period
HVPG = hepatic venous pressure gradient
A reduction in HVPG ≥20% or below the 12-mm Hg threshold markedly reduces the risk of variceal bleeding, and varices may decrease in size
a a a
Mostly in MELD < 10
Hepatitis B
Antiviral therapy reduces portal pressure in patients with
cirrhosis due to HBeAg-negative chronic hepatitis B and
significant portal hypertension
19 cirrotics, HVPG > 10mmHg, lamivudine 100 mg/d
Manolacopoulus S. H Hepatology 2009
ALT, HBV-DNA
MELD reduction
HBV
Antiviral Therapy reduces Portal Hypertension
5/7 (71%) OV disappearance
Debernardi Venon W et al; AISF 2013
0
20
40
60
80
100
0 12 24 36 48 60 72 84 96 108 120 Months
27 24 19 9 4 3
80%
21 27 15 8 4
27 26 23 2
0
14 9 24 27 21 18 14
12% EV progression
EV regression
0
20
40
60
80
100
0 12 24 36 48 60 72 84 96 108 120
Patients
at risk 80 78 74 62 45 33 80 67 78 56 39
8%
EV progression
Changes of esophageal varices (EV) in
compensated cirrhotics treated with LAM±TDF for 10 years
No varices at baseline (n=80)
F1 varices at baseline (n=27)
Overall, EV worsening rate per year: 0.9%*
* 6 of 7 progressors (86%) had either LMV-R and/or HCC
Marengo, & Marzano Antiviral Therapy 2013
Decompensation Death
* 2 CH
CH
Cirrhosis
Clinical experience with III gen NUCs:
Entecavir 100 pts (55 compensated cirrhosis)
Decompensated cirrhosis
Mutimer DJ, Gut 2012
• Diagnosis and scores
• Septal fibrosis
• Small nodularity
• Portal tracts lost
• Interface inflammation
• Alcohol
Clinical Significant Portal Hypertension HVPG > 10 mmHg
43 cirrhotics, 56% viral etiology
Nagula S. J Hepatology 2006. Garcia Tsao. Hepatology 2010
HVPG
Fibrosis stage
Relationship between Fibrosis Stage and HVPG
Blasco. Hepatology 2006
Vizzuti. Hepatology 2007
Fibroscan Liver Stiffness predicts Severe
Portal Hypertension in Cirrhosis
Liver stiffnes > 13 kaP cirrhosis
Gaia, J Hepatol 2011
Gaia, J Hepatol 2011
Fibroscan
Figura patologia non-HBV
Non invasive scores to detect Liver Fibrosis
APRI
Fibrotest*
Forns index
HUI
AST/ALT
Platelet count/Ø spleen
Platelets
Type IV collagen
GUCI
SAPI
Hyaluronic acid
Transient elastography*
LSPS (Liver stiffness X Ø spleen/platelet count*)
* Compared to liver biopsy or HVPG
algorytm
LSPS is a predictor for EBV risk in B viral liver cirrhosis Berzigotti A. Gastr 2013
KIM B. Am J Gastr 2011
LSPS ed HCC
• <1.13.5%
• > 2.5 32%
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
123 pts
Antiviral therapy: 23 LAM, 17 LAM+NUC, 77 NUC (53 NUC ab initio)
Time of treatment: mean 8.7 yrs (1-17)
49% with PH (32% EV)
111 pts with Fibroscan, HVPG
ALT 27.8 (9-138)
Ø Spleen 12.5 (8.2-14.8)
LS 9.3 (3-22.5)
PLTS 153 (34-653)
HBsAg q 2596 (0-47000)
LSPS 1.25 (0.15-11.25)
(LSxØ spleen/PLTS)
Marzano. Personal data
LSPS in HBV: our experience
0
10
20
30
40
50
60
70
80
90
100 after T
after T
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
%
P<0.05
New EV reduction or
desappearance EV
0
20
40
60
80
100
LSPS < 0.62
LSPS > 0.62
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
LSPS ≤ 0.62 after therapy has 100% NPV for predicting an HVPG < 6 mmHg
HVPG
< 6 mmHg > 6 mmHg
% pts
56 pts
44pts
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
ALT 27.46 30.93 ns
Age 62 63 ns
LS 6.6 13.6 < 0.0001
Ø spleen 10.6 14.2 < 0.0001
PLTS 195.9 112.7 < 0.0001
56 pts 44 pts
LSPS ≤ 0.62 LSPS >0.62 p
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
56 pts 44 pts
LSPS ≤ 0.62 LSPS >0.62
ALT mean N pts ALT mean N pts
ALT
≤ 19
≤ 30
16.6
20.7
32%
77%
15.7
20.5
34%
42%*
HBsAg q
≤ 19
≤ 30
3014.7°°
2143°°
29%**
71%**
1918,6 °
1708,2 °
32%*
58%*
*p< 0.05 vs **, ° p<0.05 vs °°
Liver fibrosis and portal hypertension in HBV compensated cirrhotics
long term treated with antiviral therapy
Incidence of HCC: 20%
HCC vs no HCC: no significant difference in ALT, LS, Ø spleen, PLTS,HBsAg q
≤ 0.62 > 0.62
HCC 2/56 (3%) 6/44 (14%)*
HbsAg q (mean) 3122.88 2119.1*
LS ≥ 11 5/56 ( 13.9) 18/44 (17.1)*
ALT (mean) 27 41*
Ø spleen (cm) 10.6 14.2*
PLTS 195000 112000*
* p < 0.05 vs patients group with LSPS ≤0.62
Conclusions
• Portal hypertension can influence outcome post antiviral therapy, also in responders
• The degree of portal hypertension and a “more severe” cirrhosis should be
consider before treating decompensated cirrhotics
• Fibroscan is a good predictor of cirrhosis and is a usefull non invasive tool for monitoring
patients during antiviral therapy in HCV+ patients
• In HBV + patients LSPS, performed at the bedside,is predictor of portal hypertension and
of clinical response to antiviral theraphy. In compensated patients can avoid the EGDS.
• The risk of HCC in patiens with >0.62 seems to be related to viral activity.