Hepatitis, Viral, Human Clinical Trial
Official title:
Human Genes Involved in Susceptibility or Resistance to Hepatitis B Virus
This study, conducted by the Beijing University First Hospital of China and the National
Cancer (NCI), will try to identify genes associated with either susceptibility or resistance
to chronic infection by the hepatitis B virus (HBV). Some people recover from HBV infection;
others become chronically infected and may go on to develop severe liver disease such as
cirrhosis or liver cancer. About 350 million people worldwide have chronic HBV infection. Of
120 million infected Chinese, 90 percent of children infected at less than 5 years of age and
10 percent of infected adults develop persistent infection.
HBV-infected and non-infected healthy persons of Han ethnicity born before 1963 may be
eligible for this study. Offspring of infected candidates (born in any year) may also be
enrolled. Infected adults must have at least one infected parent or sibling. Persons who
resided in Fusui County of Guangxi Zhuang Autonomous Region or in the Qidong district of
Jiangsu Province for at least 6 months before 1986 may not participate.
All participants (except offspring of the study subjects) will fill out a health
questionnaire (providing information about eating, drinking, and smoking habits and a
personal and family health history) and will donate no more than 20 milliliters of blood. The
blood will be tested for antibodies, antigens, and other substances that may indicate
infection with hepatitis viruses. Some of the blood will be sent to the NCI for DNA analysis
to identify genetic factors that may influence clearance of the hepatitis virus after
infection or progression to liver diseases associated with HBV infection. Infected patients
who have had a liver biopsy in the past will be asked permission to examine tissue from the
biopsy and to review laboratory results of any tests done for diagnostic and treatment
purposes.
When the study is completed, specimens sent to the NCI will have identifiers linking the
material to the donor removed. The anonymous samples may then be used for other genetic
studies. Specimens remaining in China will continue to have identifiers linked to them and
may be used for future studies designed to identify who is at greatest risk of developing
serious liver diseases. Participants who do not want their blood used for future studies may
request that the samples be destroyed.
Because children inherit one-half of their DNA from each parent, DNA samples from HBV
infected study participants may provide additional information about the parent s DNA
structure. Offspring who participate in this study will provide a DNA sample. The sample is
obtained by swishing a mouthwash in the mouth for 30 seconds and then spitting the mouth wash
into a cup. The DNA is then isolated from the mouth cells.
Persistent hepatitis B viral (HBV) infection is a significant public health problem because
of the occurence of chronic liver disease, cirrhosis, and hepatocarcinoma (HCC) [1-3].
Roughly one-third of the world population has been infected with HBV and there are about 350
million (5-6%) persistent carriers. HBV causes 80% of all liver cancer and is the second most
important carcinogen, after smoking tobacco. There is an approximate 90% risk of becoming a
persistent carrier following perinatal infection in infants born to e antigen positive
carrier mothers and 30% risk in pre-school children. Only 5-10% of adults become persistent
carriers following infection. Like HIV, HBV is transmitted by contaminated blood through
transfusion or intravenous drug use and by high-risk sexual behavior.
The purpose of this investigation is to study how different outcomes of hepatitis B exposure
and infection are affected by host genetic factors in the Chinese population, where more than
120 million individuals are infected with HBV. Of people persistently infected with HBV,
10-30% will develop liver cirrhosis (LC) and hepatocellular carcinoma (HCC). These highly
variable outcomes in both clearance rates and disease outcomes in persistently infected
individuals cannot be fully explained by differences in viral or environmental factors. Thus,
differences in host genetic factors may affect hepatitis B natural history.
Blood will be collected from volunteers in China. Healthy donors unexposed to HBV or HCV,
individuals who have cleared HBV, and asymptomatic carriers of HBV will be identified by the
Peking University hospitals and blood bank. HBV infected individuals with chronic hepatitis,
cirrhosis or HCC will be identified by the Peking University hospital hepatitis clinics.
Targeted individuals will be asked to participate by letter or a telephone interview by
trained hospital staff. A database of clinical and family information will be created from a
questionnaire completed by hospital staff. A database of clinical and family information will
be created from a questionnaire completed by hospital staff interviewers. Blood will be
separated into plasma and peripheral blood mononuclear cells (PBMCs) and cryopreserved in
China. Serum will be tested in China for hepatitis viral markers, HBV genotypes, and HBV
viral load. Two vials of PBMC will be transferred to the LGD, NCI-USA, for mRNA expression
assays and host genetic analysis. Lymphoblastoid cell lines will be established by the
LGD-NCI as a source of renewable DNA. RNA will be extracted from PBMCs for determination of
mRNA expression by the microarray method. Results of mRNA expression assays and literature
searches will be used to identify candidate genes. DNA extracted from cell lines will be
genotyped for single nucleotide polymorphisms (SNPs) in candidate genes and DNA markers,
including HLA, cytokines, chomokines, and their receptors, and putative HBV cell entry
targets by DNA genotyping methods. SNPs in candidate genes will be identified using public
and private SNP databases and SNP discovery methods. SNPs will be genotyped study
participants and analyzed to detect associations between polymorphisms and phenotypes
obtained from clinical and laboratory testing. If a genetic marker associated with the
development of a disease phenotype is found, there are potential applications in diagnostics
and therapy. The identification of allelic polymorphisms in genes involved in the pathway
from chronic viral infection to LC and ultimately HCC would provide insight into the
carcinogenic process.
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