Factors
Associated with Development of Hepatocellular Carcinoma in Chronic Hepatitis B
Patients By
Liz Highleyman Over
years or decades, people with chronic hepatitis
B virus (HBV) infection may progress to advanced liver disease including cirrhosis
and hepatocellular
carcinoma (HCC). 
HCC
has a high mortality rate, in part because it is often diagnosed at an advanced
stage. Knowing which hepatitis B patients are at greatest risk could allow for
more targeted liver cancer screening. Pre-existing cirrhosis and a specific HBV
mutation increase the risk for HCC, according to 2 studies presented at the recent
44th Annual Meeting of the European Association for the
Study of the Liver (EASL 2009) in Copenhagen. HCC
in Younger Patients Since
liver disease progression typically takes many years, people with HCC are usually
older than 40 years of age. In the first study, C.J. Chen and colleagues evaluated
the risk of HCC among participants in the REVEAL-HBV cohort who were younger than
40 at the time of enrollment into the cohort. The
analysis included 1216 patients. The median age was 35 years and a majority (62%)
were men. Within this group, 280 (23%) were hepatitis B "e" antigen
(HBeAg) positive and 12 (1%) had cirrhosis. 60% had serum ALT < 15 IU/L, 33%
had 15-44 IU/L, and 6% had > 45 IU/L. About one-fifth (22%) had undetectable
HBV DNA (< 300 copies/mL), 31% had 300-9999 copies/mL; 16% had 10,000-99,999
copies/mL, 9% had 100,000-999,999 copies/mL, and 22% had > 1,000,000.
Results
Over a median 12 years of follow-up (reflecting 14,393 person-years [PY]), 16
patients -- all men -- developed HCC.
This represented an incidence rate of 111 per 100,000 PY of follow-up.
Elevated serum ALT and liver cirrhosis were independent predictors of HCC.
Compared with a serum ALT < 15 IU/L, patients with baseline ALT 15-44 were
3 times more likely to develop HCC (adjusted hazard ratio [HR] 3.0), while those
with ALT > 45 were about 8 times more likely (adjusted HR 8.3).
Liver cirrhosis at baseline was also associated with an increased risk of HCC
(adjusted HR 12.5).
Alcohol consumption, older age, higher serum HBV DNA, and HBeAg positive status
were all associated with a trend towards higher HCC risk, but these did not reach
statistical significance.
"The overall risk of developing HCC in subjects below age 40 over a 12 year
follow up was very low in this cohort," the investigators concluded. "The
strongest risk predictor is the presence of cirrhosis, already present in a small
number of these young subjects."
Genomics
Research Center, Academia Sinica, Taipei, Taiwan; Graduate Institute of Epidemiology,
College of Public Health, National Taiwan University, Taipei, Taiwan; Research
and Development, Bristol-Myers Squibb Company, Wallingford, CT. Pre-S
Deletion A.P.
Yeung and colleagues looked at the role of pre-S deletions in the HBV genome and
HBeAg status in the development of HCC. Recent case-control studies have suggested
that HBV pre-S/S mutations are associated with HCC, the researchers noted as background,
but these patients were not matched for age, sex, and HBeAg status. In
the present analysis, the researchers investigated the association between pre-S
deletions and HCC using both a matched case-control approach and a longitudinal
approach. In addition, they also looked at the association between pre-S deletions
and HBeAg seroconversion. The
study included 117 chronic hepatitis B patients with HCC and 117 without HCC,
matched with regard to age, sex, and HBeAg status. Serum samples collected 1 to
7 years before development of HCC were assessed in 16 HCC patients with pre-S
deletions. HBV
pre-S deletions were also determined in 76 chronic hepatitis B patients without
HCC 1 to 8 months (median about 6 months) before HBeAg seroconversion and 2 to
8 months (median about 6 months) after seroconversion. Results
Pre-S deletions were detected in 33 out of 117 patients with HCC (28%).
Nucleotide sequence analysis of 78 HCC/non-HCC matched pairs showed that 26 patients
with HCC (33%) and 15 (19%) without HCC acquired pre-S deletions.
In the longitudinal study, pre-S deletions were absent in 4 case patients (25%)
before they developed of HCC.
In the second analysis, 7 of 76 patients (9%) had newly emergent pre-S deletions
after HBeAg seroconversion, while 5 (7%) had pre-S deletions before HBeAg seroconversion.
In
conclusion, the investigators stated, "These findings suggested that pre-S
deletions were associated with HCC development. "25%
of HCC patients had developed pre-S deletions within 1 year before the occurrence
of HCC," they continued. "However its association with HBeAg seroconversion
was not clear." The
researchers are currently conducting further research to validate these findings
in a larger number of patients. Department
of Medicine, Queen Mary Hospital, University of Hong Kong, Hong Kong S.A.R., China 6/2/09 References CJ
Chen, HI Yang, J Su, and others. Risk and Predictors of HCC in People Less than
40 Years of Age: Update from the REVEAL HBV Study. 44th Annual Meeting of the
European Association for the Study of the Liver (EASL 2009). Copenhagen, Denmark.
April 22-26, 2009. AP
Yeung, DKH Wong, J Fung, and others. Association of Hepatitis B Virus Pre-S Deletions
with the Risk of Development of Hepatocellular Carcinoma. 44th Annual Meeting
of the European Association for the Study of the Liver (EASL 2009). Copenhagen,
Denmark. April 22-26, 2009.
EASL
2009 MAIN PAGE
15th
Conference on Retroviruses and Opportunistic Infections (CROI 2009)
Coverage
by HIV and Hepatitis.com - February 8 - 11, 2009, Montreal
HIV and AIDS Treatment
News, Experimental News, FDA-approved News Highlights
of the 15th Conference on Retroviruses and Opportunistic Infections (CROI 2009)
- Coverage by HIV and Hepatitis.com, February 8 - 11, 2009, Montreal
|