Hepatocellular Carcinoma Clinical Trial
Official title:
The Influence of Metabolic Syndrome and Circulating Bile Acid Levels on the Development of Hepatocellular Carcinoma and Biliary Tract Cancers
Increasing rates of highly malignant hepatocellular carcinoma (HCC) and biliary tract cancers
(GBTC) observed in Western populations may be related to obesogenic lifestyle factors and
their metabolic consequences, such as metabolic syndrome (MetS), inflammation and altered
production of bile acids (BA). Such lifestyle behaviours may induce changes in the gut
microflora which in turn affect BA profiles, increasing their carcinogenicity. Some elevated
BA may be oncogenic in exposed liver, bile ducts and gall bladder. Vertical sleeve
gastrectomy may change bile acid composition.
The aims of this study are:
1. whether specific presurgical bila acid profiles are predictive of efficacy of vertical
sleeve gastrectomy, reflective of liver function and metabolic dysfunction;
2. whether specific presurgical bile acid profiles are predictive of the efficacy of sleeve
gastrectomy
"Increasing rates of highly malignant hepatocellular carcinoma (HCC) and biliary tract
cancers (GBTC) observed in Western populations may be related to obesogenic lifestyle factors
and their metabolic consequences, such as metabolic syndrome (MetS), inflammation and altered
production of bile acids (BA). Such lifestyle behaviours may induce changes in the gut
microflora which in turn affect BA profiles, increasing their carcinogenicity. Some elevated
BA may be oncogenic in exposed liver, bile ducts and gall bladder. Data from case-control
studies show higher blood BA in patients with various liver diseases, but from these designs
it is unclear if the differences in BA levels are etiologic or consequential. To date no
prospective studies have investigated the role of circulating BA levels in the development of
HCC/GBTC, nor any potential interactions with diet, obesity and MetS. Interestingly, Vertical
Sleeve Gastrectomy (VSG), an anti-obesity intervention, may alter BA profiles in some
patients towards a potentially detrimental composition, but this is largely unexplored.
Project description: This project is composed of two complementary studies designed to
explore the role of BA in obesity, liver function and tumourigenesis. The 1st study is a
case-control study of hepatobiliary cancers (191 HCC; 266 GBTC; 457 matched controls) nested
within a large prospective cohort of Franco-European populations (EPIC, >520,000 subjects)
with extensive and detailed dietary/lifestyle data, body size measures and biological samples
taken at baseline prior to disease development. The aim of this study is to explore
associations between pre-diagnostic MetS markers and BA levels and the risk of HCC and GBTC,
and to establish whether the observed associations are modulated, in part, by
dietary/lifestyle factors or metabolic dysfunction.
The 2nd study is based on a clinical setting and aims to recruit 100 morbidly obese subjects
undergoing VSG to compare their BA and metabolic profiles pre- to 1 year post-surgery. This
study is based on observations that post-VSG BA synthesis is increased, but changes in BA
composition towards possibly harmful profiles have not previously been studied. It is also
hypothesized that the degree of weight loss and metabolic improvement in VSG patients may be
related to pre-surgical BA profiles.
In both studies, comprehensive panel of 17 serum BA (primary, secondary, (un)-conjugated,
sulphated) and metabolic biomarkers (inflammation, liver function, dyslipidemia, HbA1c, MetS
indicators, hepatitis status) will be assessed using validated methods. Study 2 will also
assess expression of liver FXR, a BA receptor gene. Statistical Methods: Study 1 will
calculate odds ratios and 95% confidence intervals for circulating BA levels/MetS markers in
relation to HCC and GBTC risk by multivariable conditional logistic regression, controlling
for potential confounding variables and effect modifiers. Receiver operating characteristics
(ROC) analyses will be performed to assess a combination of BA and metabolic markers with
best performance to prospectively distinguish between cancer cases and controls. In study 2,
GLM (repeated measures) ANOVA will be used to compare pre-/post-surgery changes in
biomarkers. BA profiles from both studies, will be compared and correlations between BA and
other biomarkers, lifestyle and body size measures will be assessed.
Expected results: This project is based on two related concepts. First, that lifestyle
behaviours and obesity may alter gut microflora leading to changes in BA metabolism,
enhancing production of specific BA known to be cancer promoting. Second, observations of
increased BA levels post-VSG surgery, which may improve metabolic function, but some BA may
be pro-carcinogenic over the longer term. The project will provide improved understanding of
the inter-relations between BA, lifestyle behaviours and metabolic factors and the
development of hepatobiliary cancers. It will also identify specific BA most strongly
associated with these highly malignant cancers. The findings will contribute to the evidence
base for advice on lifestyle and metabolic modifications for cancer prevention. The clinical
implications are two-fold. First, the findings will provide insight as to whether BA profiles
are predictive of the efficacy of VSG with potential implications in personalized medicine,
and second, identified biomarker profiles may be used for more refined risk stratification
for development of these cancers and subsequent closer patients' surveillance for early
detection "
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