SURVIVAL AND PROGNOSTIC FACTORS IN 366 PATIENTS WITH COMPENSATED CIRRHOSIS TYPE-B - A MULTICENTER STUDY

被引:227
作者
REALDI, G
FATTOVICH, G
HADZIYANNIS, S
SCHALM, SW
ALMASIO, P
SANCHEZTAPIAS, J
CHRISTENSEN, E
GIUSTINA, G
NOVENTA, F
机构
[1] UNIV PADUA,IST MED CLIN,I-35100 PADUA,ITALY
[2] HIPPOKRAT GEN HOSP,ACAD DEPT MED,ATHENS,GREECE
[3] UNIV ROTTERDAM HOSP,ROTTERDAM,NETHERLANDS
[4] UNIV PALERMO,CATTEDRA CLIN MED R,PALERMO,ITALY
[5] UNIV BARCELONA,HOSP CLIN BARCELONA,LIVER UNIT,BARCELONA,SPAIN
[6] BISPEBJERG UNIV HOSP,DEPT MED B,COPENHAGEN,DENMARK
关键词
CIRRHOSIS; CLINICAL COURSE; HEPATITIS B VIRUS INFECTION; HEPATITIS D VIRUS INFECTION; LONGITUDINAL STUDY; PROGNOSTIC INDEX;
D O I
10.1016/S0168-8278(94)80115-0
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
A multicenter longitudinal study was performed to assess the survival of hepatitis B surface antigen positive compensated cirrhosis, primarily in relation to hepatitis B virus replication and hepatitis delta virus infection, and to construct a prognostic index based on entry characteristics. This cohort study involved nine university medical centers in Europe. Three hundred and sixty-six Caucasian HBsAg positive patients with cirrhosis who had never had clinical manifestations of hepatic decompensation were enrolled and followed for a mean period of 72 months (6 to 202 months). Inclusion criteria were biopsy-proven cirrhosis, information on serum hepatitis B e antigen and antibody to hepatitis D virus at the time of diagnosis and absence of complications of cirrhosis. At entry 35% of the patients were HBeAS positive, 48% of the patients tested were HBV-DNA positive and 20% anti-HDV positive. Death occurred in 84 (23%) patients, mainly due to liver failure (45 cases) or hepatocellular carcinoma (23 cases). The cumulative probability of survival was 84% and 68% at 5 and 10 years, respectively. Cox's regression analysis identified six variables that independently correlated with survival: age, albumin, platelets, splenomegaly, bilirubin and HBeAg positivity at time of diagnosis. According to the contribution of each of these factors to the final model, a prognostic index was constructed that allows calculation of the estimated survival probability. No difference in survival of hepatitis D virus infected and uninfected patients was observed. Termination of hepatitis B virus replication and/or biochemical remission during follow up correlated with a highly significant better survival. These data show that in compensated cirrhosis B, hepatitis B virus replication, age and indirect indicators of poor hepatic reserve and established portal hypertension significantly worsen the clinical course of the disease, whereas hepatitis D virus infection does not influence the prognosis. The highly significant improvement in life expectancy following cessation of hepatitis B virus replication and biochemical remission favors antiviral therapy in those patients with a guarded prognosis, as estimated by a prognostic index. (C) Journal of Hepatology.
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收藏
页码:656 / 666
页数:11
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