Presentation is loading. Please wait.

Presentation is loading. Please wait.

International Congress Highlights 2004 Clinical Update in GI disease Portal Hypertension P. Michielsen University of Antwerp 20.11.2004.

Published byLucy Snow Modified over 8 years ago

Similar presentations

Presentation on theme: "International Congress Highlights 2004 Clinical Update in GI disease Portal Hypertension P. Michielsen University of Antwerp 20.11.2004."— Presentation transcript:

1 International Congress Highlights 2004 Clinical Update in GI disease Portal Hypertension P. Michielsen University of Antwerp 20.11.2004

2 55th Annual Meeting AASLD

3 Discussed abstracts Bureau C. et al. A randomized study cmparing the use of polytrtrafluoroethylene (PFTE) covered stents and non- covered stents for TIPS: long term patency. Hepatology 2004;40 (suppl. 1): 186A. Bolondi L. et al. Potassium canrenoate decreases the incidence of portal hypertension-related complications in compensated cirrhosis. A double-blind randomized study. Hepatology 2004;40 (suppl. 1): 224A Thabut C. et al. Diagnostic value of fibrosis biochemical markers (Fibrotest-Fibrosure) for the prediction of severe portal hypertension in patients with and without cirrhosis. Hepatology 2004;40 (supppl. 1): 202A

4 Covered TIPS (Viatorr) vs uncovered stents C. Bureau et al. (Toulouse, Barcelona, Montréal) Background –50% dysfunction rate at 1 year major drawback TIPS procedure –Use of polytetrafluoroethylene (PTFE) covered stents decreases rate TIPS dysfunction at 1 year (Bureau et al. Gastroenterology 2004;126:469-75) Aim: report long-term patency at 2 years

5 Covered TIPS (Viatorr) vs uncovered stents C. Bureau et al. (Toulouse, Barcelona, Montréal) Methods –80 cirrhotic patients treated by TIPS 24 for active variceal bleeding 24 for prevention of rebleeding 32 for refractory ascites –Randomization Group A (n=39): PTFE covered stent Group B (n=41): uncovered stent –Follow-up Doppler US day 7, 1 month, then every 3 months Angiography and HVPG measurement every 6 months and when stent dysfunction suspected –Shunt dysfunction stenosis > 50% of lumen and/or HVPG > 12 mm Hg

6 Covered TIPS (Viatorr) vs uncovered stents C. Bureau et al. (Toulouse, Barcelona, Montréal) Results at 2 years –Shunt dysfunction Group A (covered): 15% Group B (uncovered): 44% (p<0.005) –Primary patency Group A (covered): 76% Group B (uncovered): 36% (p=0.001) –Recurrent complications portal hypertension Group A (covered): 19% Group B (uncovered): 38% (p=0.002) –Survival: similar –Encephalopathy Group A (covered): 33% Group B (uncovered): 49% (p<0.05)

7 Covered TIPS (Viatorr) vs uncovered stents C. Bureau et al. (Toulouse, Barcelona, Montréal) Conclusions : PTFE covered stents –improve long-term patency of TIPS –prevent clinical relapses –decrease rate of encephalopathy

8 Covered TIPS (Viatorr) vs uncovered stents Comment: M. Rössle (Freiburg) and K.D. Mullen (Cleveland, OH), Hepatology 2004;40:495-7 Risk HE lower in covered stents explained by decreased need to revise TIPS But: diameter bare stents 11.7  0.8 mm vs covered 10.5  0.9 mm –Greater bare stents to prevent early insufficiency –Smaller covered stents to reduce risk HE

9 Covered TIPS (Viatorr) vs uncovered stents Comment: M. Rössle (Freiburg) and K.D. Mullen (Cleveland, OH), Hepatology 2004;40:495-7 Proposal –Small diameter (8 mm) covered stents to be used in patients with variceal bleeding (where partial pressure reduction may be effective in preventing rebleeding) –Bare stents In patients with higher risk HE and liver failure In patients with refractory ascites (10-12 mm): large stent more effective + protection against HE at long-term follow-up

10 K canrenoate and portal hypertension related complications in compensated cirrhosis L. Bolondi et al., Italy Background –Aldosterone-dependent renal sodium retention in compensated cirrhosis contributes to portal hypertension and ascites formation –Chronic spironolactone administration has been shown to effectively reduce variceal pressure (Nevens et al., Hepatology 1996;23:1047-52)

11 K canrenoate and portal hypertension related complications in compensated cirrhosis L. Bolondi et al., Italy Aim: Evaluation oral K canrenoate in patients with preascitic cirrhosis for 1 year on –Appearance of esophageal varices –Worsening stage F1 esophageal varices –De novo appearance of ascites

12 K canrenoate and portal hypertension related complications in compensated cirrhosis L. Bolondi et al., Italy Methods –Multicenter prospective double-blind randomized controlled study with 2 arms. –Inclusion: Child A viral cirrhosis No present or past ascites F1 or no varices Presence of endoscopic or US signs portal hypertension –120 patients enrolled Group 1: K canrenoate 100 mg/d (n=66) Group 2: placebo (n = 54) –Evaluation: baseline, wk 2, 17, 34, 52

13 K canrenoate and portal hypertension related complications in compensated cirrhosis L. Bolondi et al., Italy Results –Complete follow-up K canreanoate: 50/66 Placebo: 43/54 –Worsening varices: 30.1% in placebo vs 18% in K canrenoate (ns) –Appearance ascites: 10.6% in placebo vs 2% in K canrenoate (ns) –Any primary endpoint (risk ascites, appearance or worsening esophageal varices): 38.3% in placebo vs 17.6% in K canrenoate (p<0.05) –Adverse events: no difference

14 K canrenoate and portal hypertension related complications in compensated cirrhosis L. Bolondi et al., Italy Conclusion Oral K canrenoate is well tolerated and significantly decreases development of portal hypertension related complications in compensated liver disease over 1 year.

15 Diagnostic value fibrosis biochemical markers (Fibrotest- Fibrosure) for prediction of severe portal hypertension Thabut et al., Paris, France Background –Best way to estimate degree PH is measurement HVPG –Fibrotest ® (Biopredictive) is a marker of liver fibrosis, combining 5 components 3 proteins: –α2 macroglobulin –apolipoprotein-A2 –haptoglobin bilirubin γ-GT adjusted to age and gender. It ranges from 0 to 1

16 Diagnostic value fibrosis biochemical markers (Fibrotest- Fibrosure) for prediction of severe portal hypertension Thabut et al., Paris, France Aim –Assess predictive value Fibrotest (FT) for diagnosis of severe PH in cirrhosis –Determine if FT can help in diagnosis severe PH in patients without cirrhosis Methods –Transjugular catheterisation (end point HVPG > 12 mm Hg) and biopsy –Measurement biochemical values

17 Diagnostic value fibrosis biochemical markers (Fibrotest- Fibrosure) for prediction of severe portal hypertension Thabut et al., Paris, France Results : 179 patients included HistologyFibrotestHVPG Normal architecture (26%) 0.434 Fibrosis (21%) 0.76*10* Cirrhosis (53%) 0.93*18* *p<0.001 Significant correlation HVPG and FT

18 Diagnostic value fibrosis biochemical markers (Fibrotest- Fibrosure) for prediction of severe portal hypertension Thabut et al., Paris, France Results : Cirrhosis HVPGFT <12 mm Hg (n=8)0.76 >12 mm Hg 0.87 (p=0.04) Fibrosis (n = 38) HVPGFT <12 mm Hg0.67 >12 mm Hg (n=12)0.86 (p=0.003) Normal liver architecture (n = 46) HVPGFT <12 mm Hg 0.47 >12 mm Hg (n = 3)0.97 (p=0.02)

19 Diagnostic value fibrosis biochemical markers (Fibrotest- Fibrosure) for prediction of severe portal hypertension Thabut et al., Paris, France

20 Conclusions –In cirrhosis, FT can discriminate patients with severe PH –In non cirrhosis, FT can help to detect severe PH

Download ppt "International Congress Highlights 2004 Clinical Update in GI disease Portal Hypertension P. Michielsen University of Antwerp 20.11.2004."

Similar presentations

Intermediate stage HCC management

Intermediate stage HCC management
Measurement of liver fibrosis Amar Dhillon Royal Free and University College Medical School.

Measurement of liver fibrosis Amar Dhillon Royal Free and University College Medical School.
Bruix J, et al. Presented at the 44 th Annual Meeting of the European Association for the Study of the Liver (EASL), April 24, 2009, Copenhagen, Denmark.04/28/09.

Bruix J, et al. Presented at the 44 th Annual Meeting of the European Association for the Study of the Liver (EASL), April 24, 2009, Copenhagen, Denmark.04/28/09.
Management of Chronic Hepatitis C in 2013

Management of Chronic Hepatitis C in 2013
Teaching Liver cirrhosis with varices. Discussion  Approximately half of patients with cirrhosis have esophageal varices  One-third of all patients.

Teaching Liver cirrhosis with varices. Discussion  Approximately half of patients with cirrhosis have esophageal varices  One-third of all patients.
The DRASTIC Trial. Dutch Renal Artery Stenosis Intervention Cooperative Reference van Jaarsveld BC, Krijnen P, Derkx FHM, et al. Resistance to antihypertensive.

The DRASTIC Trial. Dutch Renal Artery Stenosis Intervention Cooperative Reference van Jaarsveld BC, Krijnen P, Derkx FHM, et al. Resistance to antihypertensive.
Consistent Venous Thromboembolism Risk Reduction by Extended- Versus Standard-Duration Enoxaparin Prophylaxis in Subgroups of Acutely Ill Medical Patients.

Consistent Venous Thromboembolism Risk Reduction by Extended- Versus Standard-Duration Enoxaparin Prophylaxis in Subgroups of Acutely Ill Medical Patients.
TROPHY TRial Of Preventing HYpertension. High-normal BP increases CV risk Vasan RS et al. N Engl J Med. 2001;345:1291-7. Incidence of CV events in women.

TROPHY TRial Of Preventing HYpertension. High-normal BP increases CV risk Vasan RS et al. N Engl J Med. 2001;345: Incidence of CV events in women.
A retrospective cohort study of Childhood post-streptococcal glomerulonephritis as a risk factor for chronic renal disease in later life Andrew V White,

A retrospective cohort study of Childhood post-streptococcal glomerulonephritis as a risk factor for chronic renal disease in later life Andrew V White,
Can we prevent stent restenosis after coronary stent implantation

Can we prevent stent restenosis after coronary stent implantation
CREATININE AND CYSTATIN-C BASED GFRs VS 51 Cr-EDTA GFR IN PATIENTS WITH DECOMPENSATED CIRRHOSIS 1 4th Department of Internal Medicine, Hippokration General.

CREATININE AND CYSTATIN-C BASED GFRs VS 51 Cr-EDTA GFR IN PATIENTS WITH DECOMPENSATED CIRRHOSIS 1 4th Department of Internal Medicine, Hippokration General.
Protein GP73 (GOLGI PROTEIN 73) A NEW NON-INVASIVE BIOMARKER FOR ASSESSING LIVER FIBROSIS AND RISK OF PROGRESSION TO HEPATOCELLULAR CARCINOMA N.K. Gatselis,

Protein GP73 (GOLGI PROTEIN 73) A NEW NON-INVASIVE BIOMARKER FOR ASSESSING LIVER FIBROSIS AND RISK OF PROGRESSION TO HEPATOCELLULAR CARCINOMA N.K. Gatselis,
Sum Scores and Scores of Individual Components in Clinical Practice and Clinical Trials Lillian W. Gaber University of Tennessee.

Sum Scores and Scores of Individual Components in Clinical Practice and Clinical Trials Lillian W. Gaber University of Tennessee.
1 Hepatitis B Treatment Dr R.V.S.N.Sarma., M.D., Consultant Physician & Chest Specialist.

1 Hepatitis B Treatment Dr R.V.S.N.Sarma., M.D., Consultant Physician & Chest Specialist.
BEAUTI f UL: morBidity-mortality EvAlUaTion of the I f inhibitor ivabradine in patients with coronary disease and left ventricULar dysfunction Purpose.

BEAUTI f UL: morBidity-mortality EvAlUaTion of the I f inhibitor ivabradine in patients with coronary disease and left ventricULar dysfunction Purpose.
Www.ias2015.org Liver fibrosis regression after anti HCV therapy and the rate of death, liver-related death, liver- related complications, and hospital.

Liver fibrosis regression after anti HCV therapy and the rate of death, liver-related death, liver- related complications, and hospital.
Creatinine (mg/dL) 6 4 3 2 1 0 5 MonthsWeeks -4-6-20123 Therapeutic paracentesis Cefotaxime Type-2 HRSType-1 HRS Encephalopathy Jaundice CLINICAL TYPES.

Creatinine (mg/dL) MonthsWeeks Therapeutic paracentesis Cefotaxime Type-2 HRSType-1 HRS Encephalopathy Jaundice CLINICAL TYPES.
LONG-TERM OUTCOME OF INTERFERON/RIBAVIRIN TREATMENT IN GERMAN REAL-LIFE SETTING: DURABLE SVR ASSOCIATED WITH LOW RATES OF LIVER-RELATED EVENTS S. Mauss.

LONG-TERM OUTCOME OF INTERFERON/RIBAVIRIN TREATMENT IN GERMAN REAL-LIFE SETTING: DURABLE SVR ASSOCIATED WITH LOW RATES OF LIVER-RELATED EVENTS S. Mauss.
Transjugular Intrahepatic Portosystemic Shunt (TIPS) Presented by R2 吳佳展 2002/10/01.

Transjugular Intrahepatic Portosystemic Shunt (TIPS) Presented by R2 吳佳展 2002/10/01.
FT in diagnostic of HCV FibroTest in the diagnosis of HCV Publications on diagnostic performance.

FT in diagnostic of HCV FibroTest in the diagnosis of HCV Publications on diagnostic performance.

Similar presentations

Ads by Google