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Iatreia

Print version ISSN 0121-0793

Iatreia vol.20  suppl.1 Medellín June 2007

 

Hepatocellular carcinoma – Global burden and risk factors

HUBERT T E. BLUM1

  1. Professor, Department of Medicine II, University of Freiburg, Germany. hubert.blum@uniklinik–freiburg.de

Global Burden. Hepatocellular carcinoma (HCC) is one of the most common malignant tumors worldwide and has been recently reviewed 1, 2. The incidence ranges from <10 cases per 100,000 population in North America and Western Europe as well as in Iran, Iraque and India to 50–150 cases per 100,000 population in parts of Africa and Asia (Fig. 1) where HCC is responsible for a large proportion of cancer deaths 3.

However, a rise in the incidence of and mortality from HCC, most likely reflecting the increased prevalence of hepatitis C virus (HCV) infection, has recently been observed in most industrialized countries 4.

Risk Factors. The major etiologies of HCC are well defined (Table 1) and include among the well known factors an elevated body mass index, especially in men 5 as well as diabetes mellitus 6 and some of the steps involved in the molecular pathogenesis of HCC have been elucidated in recent years.

As for most types of cancer, hepatocarcinogenesis is a multistep process involving different genetic alterations that ultimately lead to malignant transformation of the hepatocyte. While significant progress has been made in recognizing the sequence of events involved in other forms of cancer, most notably in colorectal cancer and certain hematopoietic malignancies, the molecular contribution of the multiple factors and their interactions in hepatocarcinogenesis are still poorly understood. HCCs are phenotypically (morphology, microscopy) and genetically very heterogenous tumors, possibly reflecting in part the heterogeneity of etiologic factors implicated in HCC development, the complexity of hepatocyte functions and the late stage at which HCCs usually become clinically symptomatic and detectable. Malignant transformation of hepatocytes may occur regardless of the etiologic agent through a pathway of increased liver cell turnover, induced by chronic liver injury and regeneration in a context of inflammation, immune response and oxidative DNA damage.  This may result in genetic alterations, such as the activation of cellular oncogenes, the inactivation of tumor suppressor genes, possibly in cooperation with genomic instability, including DNA mismatch repair defects and impaired chromosomal segregation, overexpression of growth and angiogenic factors, and telomerase activation 7–11. Chronic viral hepatitis B, C and D, alcohol, metabolic liver diseases such as hemochromatosis and alfa–1–antitrypsin deficiency as well as non–alcoholic fatty liver disease may act predominantly through this pathway of chronic liver injury, regeneration, and cirrhosis. Accordingly, the major clinical risk factor for HCC development is liver cirrhosis since 70–90% of HCCs develop in a cirrhotic liver. Most HCCs occur after many years of chronic hepatitis that provides the mitogenic and mutagenic environment to precipitate random genetic alterations resulting in the malignant transformation of hepatocytes and HCC development.

The HCC risk in patients with liver cirrhosis depends on the activity, duration and the etiology of the underlying liver disease. Clinical and biological variables (age, anti–HCV positivity, PTT and platelet count) allow to further identify a subset of cirrhotic patients with the highest risk of HCC development 12. Coexistence of etiologies, e. g., hepatitis B virus (HBV) and HCV infection, HBV infection and aflatoxin B1 11, 13, HBV/ HCV infection and alcohol or diabetes mellitus 14, HCV infection and liver steatosis 15, environmental factors, e.g., alcohol 11, 16, 17 as well as diabetes mellitus, obesity and tobacco 5, 17–19 increase the relative risk of HCC development. Also, occult HBV infection (anti–HBc positive only) carries a significant HCC risk 20, 21. Interestingly, coffee consumption appears to reduce the HCC risk 22.

In general, HCC are more frequent in males than in females and the incidence increases with age. On the other hand, there is evidence that HBV –and possibly also HCV– may under certain circumstances play an additional direct role in the molecular pathogenesis of HCC. Finally, aflatoxins have been shown to induce mutations of the p53 tumor suppressor gene, thus pointing to the contribution of an environmental factor to tumor development at the molecular level. Further, in a transgenic mouse model it has been shown that chronic immune–mediated liver cell injury without environmental or infectious agents is sufficient to cause HCC 23 and that inhibition of cytotoxic T lymphocyte–induced apoptosis and chronic inflammation by neutralization of the Fas ligand prevents HCC development in this model 24. In addition, also in a transgenic mouse model it has been demonstrated that NF–kappaB may be the link between inflammation and HCC development 25, 26. Finally, individual polymorphisms of drug metabolizing enzymes, e.g., various cytochrome P450 oxidases, Nacetyltransferases and glutathione–S–transferase, may contribute to the genetic susceptibility to HCC development 27.

Summary and Perspectives. HCC is one of the most common malignant tumors in some areas of the world with an increasing incidence and an extremely poor prognosis. In order to reduce morbidity and mortality from HCC, therefore, apart from early diagnosis and the development of novel systemic therapies for advanced disease, incl. drugs, gene and immune therapies primary HCC prevention is of paramount importance. Apart from avoiding liver toxins, including alcohol and certain drugs, or infections with HBV or HCV by hygienic measures, avoiding parenteral exposure to blood, blood products or contaminated needles etc. a prime example is vaccination against HBV infection. Universal vaccination in Taiwan has indeed already resulted in a decline of the incidence of HCCs 28. Further, early treatment of acute hepatitis aimed at blocking transition into chronic liver diseases well as therapy of chronic liver diseases to prevent their progression to liver cirrhosis should result in a reduced HCC incidence. Finally, in patients with established liver cirrhosis LTx before HCC development is a highly effective preventive measure.

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