Advanced search
Publication Cover
Journal of Hepatocellular Carcinoma Volume 1, 2014 - Issue
Submit an article Journal homepage
509
Views
66
CrossRef citations to date
0
Altmetric
Review

Hepatocellular carcinoma: epidemiology and risk factors

Michael C KewDepartment of Medicine, Groote Schuur Hospital and University of Cape Town, Cape Town, South Africa
Pages 115-125 | Published online: 13 Aug 2014

Abstract

Hepatocellular carcinoma is one of the major malignant tumors in the world today. The number of new cases of the tumor increases year by year, and hepatocellular carcinoma almost always runs a fulminant course and carries an especially grave prognosis. It has a low resectability rate and a high recurrence rate after surgical intervention, and responds poorly to anticancer drugs and radiotherapy. Hepatocellular carcinoma does not have a uniform geographical distribution: rather, very high incidences occur in Eastern and Southeastern Asia and in sub-Saharan Black Africans. In these regions and populations, the tumor shows a distinct shift in age distribution toward the younger ages, seen to greatest extent in sub-Saharan Black Africans. In all populations, males are more commonly affected. The most common risk factors for hepatocellular carcinoma in resource-poor populations with a high incidence of the tumor are chronic hepatitis B virus infection and dietary exposure to the fungal hepatocarcinogen aflatoxin B1. These two causative agents act either singly or synergistically. Both the viral infection and exposure to the fungus occur from early childhood, and the tumor typically presents at an early age. Chronic hepatitis C virus infection is an important cause of hepatocellular carcinoma in resource-rich countries with a low incidence of the tumor. The infection is acquired in adulthood and hepatocellular carcinoma occurs later than it does with hepatitis B virus-induced tumors. In recent years, obesity and the metabolic syndrome have increased markedly in incidence and importance as a cause of hepatocellular carcinoma in some resource-rich regions. Chronic alcohol abuse remains an important risk factor for malignant transformation of hepatocytes, frequently in association with alcohol-induced cirrhosis. Excessive iron accumulation in hereditary hemochromatosis and dietary iron overload in the Black African population and membranous obstruction of the inferior cava cause the tumor in a few countries.

Epidemiology

Hepatocellular carcinoma (HCC) is the most prevalent primary malignant tumor of the liver and is accepted as one of the major malignant diseases in the world today. Justification for this recognition is its high incidence in many of the most populous regions of the world and its increasing occurrence, in some other regions, as well as its often fulminant course, low resectability rate and high recurrence rate after resection, poor response to conservative management, and grave prognosis.

Worldwide, HCC is the fifth most common cancer in men and the seventh in women, with more than 748,000 new cases being diagnosed each year, accounting for 9.2% of all new global cancer cases (7.9% in men; 3.7% in women).Citation1,Citation2 Moreover, the number of new cases of HCC increases year by year. Of all patients worldwide with HCC, 84% live in resource-poor countries.Citation1Citation3 Seventy percent of all new HCCs worldwide occur in Asia, with patients in the People’s Republic of China accounting for 55% of liver cancer deaths each year.Citation1 Most of the remaining tumors occur in sub-Saharan Black Africans. As worrying as these figures undoubtedly are, they are likely to be an underestimate of the true incidence, because, in sub-Saharan Africa, and perhaps in other resource-constrained regions with a high incidence of HCC, the tumor is both underdiagnosed and underreported.Citation3

HCC carries a particularly poor prognosis, ranking second in the world as a cause of cancer-related mortality, and has the shortest survival time of any cancer in both males and females. Almost without exception, those who develop HCC each year die within 12 months, attesting to its rapid progression and serious prognosis.Citation1,Citation2 The outlook is particularly grave in resource-poor countries, where the annual fatality ratio (0.96) is the highest of any human tumor.Citation1,Citation2

HCC does not have a uniform geographical distribution. In those regions with high incidences of the tumor – East and Southeast Asia, some of the Western Pacific islands, and sub-Saharan Africa – HCC accounts for more than 90% of all primary malignant tumors of the liver, with incidences that exceed 20 per 100,000 of the population per year.Citation4,Citation5 Mediterranean countries, such as Italy, Spain, and Greece, as well as Western Asia, Central America, the Caribbean, Eastern and Southeastern Europe, Romania, Peru, Czech Republic, Poland, and Russia, have incidences of between ten and 20 per 100,000 of the population per year.Citation4,Citation5 In the Americas, Great Britain, and remaining countries, the incidence is less than five, and often less than three, per 100,000 of the population per year,Citation4,Citation5 despite the incidences having increased appreciably in the USA and some other resource-rich countries during recent years.

The rising incidence of HCC has been attributed mainly to the increasing occurrence of two risk factors for the tumor, namely, chronic hepatitis C virus (HCV) infection and the burgeoning incidence of obesity, nonalcoholic fatty liver disease (NAFLD), and nonalcoholic steatohepatitis (NASH), and the other components of the metabolic syndrome. For example, the occurrence of HCC in the USA has tripled during the past 2 decades (from 1.4 per 100,000 in 1975–1977 to 4.8 per 100,000 in 2005–2008Citation6,Citation7), and this tumor, paralleling the epidemics of obesity and the metabolic syndrome, is now the most rapidly increasing cause of cancer deaths in that country.Citation7,Citation8

By contrast, the incidence of the tumor has decreased in some countries, for example Spain, Israel, and Latin American countries, even before any overt decrease in the known risk factors was recorded.Citation9 In Taiwan, the universal vaccination of newborn babies against hepatitis B virus (HBV) infection has already had a telling impact on the incidence of HBV-induced HCC.

Age-adjusted incidences of HCC per 100,000 persons per year for men and women (17.4 and 6.7, respectively) in resource-poor countries have been shown to be double those in resource-rich countries (8.7 and 2.8, respectively).Citation5 The difference in incidence of the tumor between high-risk regions in resource-poor countries and low-risk regions of HCC in resource-rich countries may be as much as 100-fold, one of the highest differences recorded among cancers.Citation5

In countries with a high incidence of HCC, the tumor is not necessarily uniformly common throughout the countries. For example, in the People’s Republic of China, HCC is most prevalent in the northeastern province of Jilin, in the Guangxi autonomous region, and along the eastern seaboard,Citation11 and in Mozambique the highest incidences are in the eastern regions of Inhambane, Panda, Inharrime, and Morrumbene.Citation12 Rural southern African Blacks have an approximately fourfold higher incidence of HCC than do their urban counterparts.Citation13 Less obvious differences in incidence have been reported, especially in men, in European countries with an intermediate incidence of the tumor.Citation14

In resource-rich countries, HCC is rare in patients under the age of 40 years and progressively increases in incidence in those in their 60s and 70s.Citation2,Citation9 Accordingly, the usual age at which the diagnosis is made in these countries ranges from the early 60s to the middle 70s. Elderly patients with HCC have been shown to have a poorer prognosis compared with nonelderly patients.Citation15 This survival difference disappears when patients are compared in different treatment groups, suggesting a link between the shorter survival and undertreatment of elderly patients.Citation15 In regions with a high incidence of the tumor in Asia,Citation2,Citation9 and even more so in sub-Saharan Africa,Citation12,Citation16 there is a distinct shift in the age distribution curve toward a younger age. This difference is seen to the greatest extent in Mozambican Shangaans, in whom 50% of the patients are less than 30 years of age at the time they seek medical attention, and their average age at this time is 33 years.Citation12 In Qidong County and the Guangxi autonomous region in the People’s Republic of China, the mean age at the time of diagnosis of HCC is 40 years.Citation16

In all geographical regions, males have a higher incidence of HCC than females, although the ratio is more skewed in regions with high risk of the tumor.Citation1,Citation2,Citation13,Citation14 The male:female ratio is approximately 3:1 or 4:1 in the Asia-Pacific region and in sub-Saharan Africa, as well as in medium-risk countries,Citation1Citation4 compared with 2:1 in regions with low incidence of the tumor.Citation1Citation4 Male predominance is more striking in relatively young age ranges in high-incidence regions, but in older age ranges in low-incidence regions.Citation1Citation4

Caucasoid migrants from countries with a low incidence of HCC to those with a high incidence retain the low incidence of the tumor of their country of origin.Citation14 These individuals almost always preserve their original behavioral patterns, and they generally enjoy a higher standard of living than do the natives of the region. By contrast, migrants from high-risk to low-risk regions of HCC show a decline in the incidence of the tumor with successive generations in the new country.Citation17

Risk factors for hepatocellular carcinoma

The most common risk factors for HCC in resource-constrained geographical regions with high incidences of the tumor are chronic HBV infection and dietary exposure to the fungal toxin aflatoxin B1 (AFB1), the two often occurring together and potentiating each other’s hepatocarcinogenic effects. In resource-rich regions with low incidences of HCC, chronic HCV infection is a major risk factor. During recent years, the metabolic syndrome has become increasingly frequent and important as a cause of HCC in some resource-rich countries. Long-standing alcohol abuse remains a significant cause of the tumor in many countries, although it has received relatively little attention during recent times. Iron overload, either inherited or, in the case of Black sub-Saharan Africans, acquired, is a less common but nevertheless important cause of the tumor. Membranous obstruction of the inferior vena cava (MOIVC) causes HCC in a few regions only, and cigarette smoking plays a minor role in some countries. Cirrhosis, whatever its cause, is a risk factor for the development of the tumor. The role of cirrhosis per se in the etiology of HCC is considered elsewhere.Citation18 Oral contraceptive steroids as a cause of the tumor remains uncertain.

Chronic HBV infection

HBV infection is one of the most prevalent infections in humans, with some 2 billion people worldwide (one-third of the global population) infected or having been infected with this virus.Citation1 Moreover, HBV was one of the first viruses to be implicated as a cause of a human cancer,Citation19 and evidence for its hepatocarcinogenicity is now beyond doubt.Citation20 The virus is currently believed to be second only to tobacco smoking as an environmental carcinogen to which humans are exposed, causing approximately 55% of all HCCs worldwide.Citation1 Of the approximately 400 million persons worldwide chronically infected with HBV, as many as one-quarter will develop the tumor.Citation1,Citation21 The incidence of HCC ranges from 340 to 804 per 100,000 HBV-positive males and 120 to 178 per 100,000 positive females per year,Citation1,Citation21 with odds ratios of 20.4 and 15.6, respectively, having been calculated.Citation21

Chronic HBV infection and HCC have closely parallel geographical distributions, and chronic infection with the virus is implicated in the genesis of as many as 85% of the HCCs that occur with such high frequency in ethnic Chinese and Black African populations,Citation20Citation21 both of which have high incidences of chronic HBV infection. In countries with a low or intermediate incidence of HCC, lower prevalences of hepatitis B virus surface antigen (usually less than 25%) are found in patients with the tumor.Citation20,Citation22

In individuals chronically infected with HBV, host factors influence the risk of malignant transformation. Sex and age are important in this regard. Chronically infected males are at greater risk of developing HCC than infected females,Citation19,Citation20,Citation23,Citation24 the ratio being 2:1 to 3:1 in most populations, although it is appreciably higher in sub-Saharan Black Africans (5:1 or 6:1).Citation20,Citation24 In resource-rich countries, HCC is rare before the age of 40 years, irrespective of the HBV status.Citation25 By contrast, in resource-poor countries, there is a distinct shift toward a younger age. In sub-Saharan Black Africans with HCC, 73.5% of patients under the age of 30 years have HBV-induced tumors, compared with 28.5% in those older than 60 years.Citation20

In populations with a high rate of HBV-induced HCC, the infection is predominantly acquired either perinatally or in infancy or early childhood.Citation26Citation28 In ethnic Chinese populations, HBV infection occurs predominantly as a result of perinatal transmission from highly infectious hepatitis B e antigen-positive carrier mothers.Citation25,Citation28 Later, horizontal infection plays a lesser role. By contrast, in sub-Saharan Black Africans, horizontal spread of the virus between recently infected and hence highly infectious young siblings or playmates is the major source of infection, and perinatal transmission plays a far lesser role.Citation26,Citation28 The exact modes of horizontal spread of the infection among young Black children are not known. Weeping sores or ritual scarification of the skin by witch doctors using unsterile instruments may play a role. Bites by bloodsucking vectors, such as mosquitoes, bedbugs, and hard ticks, have been suggested as a possible route, but proof is not yet available. The differences in the modes of HBV infection between the two populations is attributed to differing frequencies of hepatitis B e antigen positivity: in ethnic Chinese women of childbearing age who are chronic carriers of HBV, 40% or more are hepatitis B e antigen-positive, and this is associated with a considerable risk of perinatal transmission,Citation19,Citation26 whereas, in Black African women of the same age, the prevalence of hepatitis B e antigen is appreciably lower.Citation27,Citation28

Children infected with HBV as neonates, infants, or very early in childhood have an 80%–90% chance of becoming chronic carriers of the virus,Citation26,Citation27 and it is these early-onset carriers of the virus that are at greatest risk for the later development of HCC.

Like all forms of carcinogenesis, HBV-induced HCC is a complex, stepwise process that evolves over years. Although the virus may act alone, more usually it interacts with endogenous mutagens, such as reactive oxygen species, as well as with the inflammatory process generated by the host’s immune response to the presence of the virus. It may also interact with a number of other environmental carcinogens, including AFB1 and HCV, in causing the tumor.

Integration of HBV DNA into host DNA is thought to be a crucial step in the pathogenesis of HBV-related HCC.Citation29,Citation30 Integration occurs at multiple or single sites. The inserted DNA is always altered, usually by one or more deletions, but also by sequence rearrangements. The sites of integration are thought to be randomly distributed, although preferred sites do exist. Insertion of the viral DNA induces a series of changes in the flanking cellular sequences, including deletions, direct or inverted repeats, and chromosomal translocations. Two-thirds of the integrations occur at or near the cohesive overlap region between the direct repeat sequences DR1 and DR2. Integrated HBV DNA may also perturb the expression of cellular genes by activating transcription of these genes in trans.Citation29,Citation30

The HBx gene is often included in HBV integrants and remains functionally active, inducing many changes.Citation29,Citation30 It promotes cell cycle progression, inactivates negative growth regulators, and binds to and inhibits the expression of p53 tumor suppressor gene and other tumor suppressor genes.Citation28Citation30 HBx protein also modulates transcription of methyl transferases, causing regional hypermethylation of DNA that results in silencing of tumor suppressor genes, or global hyper methylation that results in chromosomal instability.Citation29,Citation30 The virus also has antiapoptotic and proapoptotic effects.Citation30,Citation31 In addition, HBx gene may increase the expression of telomerase reverse transcriptase and telomerase activity, prolonging the lifespan of hepatocytes. It also interferes with nucleotide excision repair. Carboxyl-truncated HBx protein loses its inhibitory effects on cell proliferation.Citation26 Dysregulation of IGF-11 enhances proliferation and antiapoptotic effects of oncogenes, giving rise to unregulated cell growth. The preS/S gene, when 3′ truncated, has transactivating functions.Citation30,Citation31

Chronic HCV infection

Evidence for a causal role for HCV in hepatocarcinogenesis is a little more recent than that for HBV, but is equally compelling. In common with HBV, the importance of HCV as a risk factor for HCC differs between resource-rich and resource-poor countries, but with HCV being an important infection and a major cause of HCC in the former rather than the latter regions. More than 170 million people in the world today, or 2.2% of the global population, are chronically infected with HCV.Citation32 A compelling characteristic of the virus is its ability to induce persistent infection in up to 75%, or in up to 85% in some cases, despite a vigorous immune response by the host. Whether there is a specific and effective cellular response, and which pathways for virus elimination are compromised, remain disputed. The mechanism of the hepatic injury in acute and chronic HCV infection is unknown, but, because there is little evidence that the virus is directly cytopathogenic, it is believed that the damage to the liver is mediated by the host’s cellular immune response to the infection.

The prevalence of chronic HCV infection ranges from 0.3% in Switzerland to more than 20% in Egypt.Citation33Citation35 In addition, prevalences vary appreciably depending upon the subpopulation examined: injecting drug users have a prevalence of 60%–90%; hemophiliacs 50%–70%; hemodialysis patients 15%–60%; and persons who received a blood transfusion before 1991 5%–10%.Citation33 In regions with a high incidence of HCV infection, 2%–2.4% of patients with HCV-induced cirrhosis develop HCC each year of follow-up. Patients with chronic HCV infection are at a greater risk of malignant transformation than those with persistent HBV infection.

The ages of the patients influences progression of the infection: 5% of patients less than 40 years of age and 20% of those over 40 years of age progress to cirrhosis in less than 20 years.Citation32Citation35 Approximately one-quarter of those with overt hepatitis will ultimately develop cirrhosis, and a significant proportion, usually but not invariably those with cirrhosis, progress to HCC.Citation32Citation35 The interval between HCV infection and the development of HCC is typically 20 years or longer. The average age at which HCC is diagnosed in Japanese patients chronically infected with HCV is 62 years.Citation34,Citation35

Chronic HCV infection is the dominant cause of HCC in resource-rich countries. In Japan, Italy, and Spain, resource-rich countries with an intermediate incidence of HCC, HCV accounts for as much as 83% of HCCs, and with odds ratios of 40 to 50.Citation32Citation34 The annual rate of development of the tumor in patients with HCV-induced HCC in most countries is between 2% and 8.9%. The interval between HCV infection and the clinical recognition of HCC is typically 17 to 30 years, although a few patients present in as short a time as 5 to 10 years.Citation32Citation37 In dying patients with HCV infection, 82% of deaths are caused by HCC. These patients are almost always approximately 10 years older than those with HBV-induced HCC. The odds ratio of HCC developing in an individual infected with HCV has been calculated to be 11.5.Citation32Citation37

The proportion of patients with HCC in whom HCV can be implicated as the cause shows a pronounced geographical variation, with risk factors differing between resource-rich and resource-constrained populations. Thus, in resource-rich countries, such as Japan, with an intermediate incidence of HCC, between 37.8% and 83% of the patients with HCC were shown to be chronically infected with HCV, whereas, in regions with low incidence of the tumor, between 10.9% and 33% were chronically infected.Citation34 During each year of follow-up, 2.4% of patients with HCV-induced cirrhosis will develop HCC.Citation35

Patients with HCV-induced HCC are generally older than those with HBV-induced tumors: the difference in age in most countries is about 10 years, although it is 20 years in sub-Saharan Black Africans.Citation37,Citation38

The ways in which HCV causes HCC are unknown. Replicative intermediates of HCV do not integrate into chromosomal DNA.

Almost all HCV-related tumors arise in cirrhotic livers or in livers with chronic hepatitis. The virus causes hepatic inflammation by complex and not yet well-understood molecular pathways, including direct viral effects and indirect mechanisms involving cytokine pathways, oxidative stress, and steatosis induction.Citation37 An increasing body of evidence recognizes the inflammatory response as pathogenically linked to the development of hepatic fibrosis, cirrhosis, and HCC.Citation37

The heterogeneity of genetic/transcriptomic/proteomic events observed in hepatocytes expressing HCV proteins and HCV-related HCCs suggests that complex mechanisms underlie malignant transformation in HCV-induced HCC.Citation32,Citation35,Citation38,Citation39 These presumably act through convoluted virus/host interactions, including HCV replication with host-cell cycles, apoptosis, proliferation, protein synthesis, lipid metabolism, and DNA damage response.

Aflatoxins

Aflatoxins are naturally occurring metabolites of the fungi Aspergillus flavus and Aspergillus parasiticus. They are structurally related difuranocoumarin derivatives, some of which are mutagenic and carcinogenic. These fungi are widely distributed in nature and are frequent contaminants of a number of staple foods, but particularly maize, ground nuts, rice, and sorghum. Aflatoxins pose serious health hazards to humans as a result of their toxic, teratogenic, mutagenic, and highly carcinogenic properties.Citation40,Citation41 Because atmospheric humidity and moisture content of plants are important in determining the growth of, and toxin production by, these molds, contamination of crops occurs mainly in subsistence-farming communities in tropical and subtropical climates with high humidity and temperature.Citation42,Citation43 In addition, prolonged storage of crops in hot and humid conditions promotes growth of the aflatoxin-producing fungi. Contamination is also likely to occur in regions where food drying and storage facilities are suboptimal, where technology and infrastructure necessary for food safety monitoring are inadequate, and where regulations to control exposure to molds are either nonexistent or unenforceable in practice.Citation42,Citation43 Most rural dwellers in such areas can afford only limited food variation, with the result that these staples comprise a significant portion of their diets.

Aflatoxins are the most common known noninfectious food-borne risk factors for HCC. It is estimated that 4.5 to 5.5 billion people worldwide are at risk of exposure to these toxins.Citation44 The geographical regions involved are in sub-Saharan Africa, Eastern Asia, and parts of South America, with the association with aflatoxin exposure being closest in sub-Saharan Africa.Citation42Citation44

Exposure to the toxins begins in utero as a consequence of transplacental transmission of the toxins, continues in the postnatal period by means of breast-feeding, and is perpetuated thereafter in the contaminated food eaten throughout life.Citation45

It has been estimated that HCC may be attributed to exposure to AFB1 in between 25,200 and 155,000 people (28.2% of all cases of the tumor worldwideCitation44), and that aflatoxins play a causative role in at least 4.6%, and at most 28.2%, of all cases of HCC worldwide.Citation44 Reducing AFB1 exposure to non-detectable levels would thus significantly reduce the incidence of HCC cases in high-risk regions by this amount.Citation40

Although the parent molecule of aflatoxin is harmless, it is converted by members of the cytochrome p450 superfamily into electrophilic intermediates that are mutagenic and carcinogenic.Citation40

AFB1 is the most potent known hepatocarcinogen.Citation46,Citation47 It is metabolized in the liver by p450 enzymes into AFB1–8,9-exo-epoxide, which is highly reactive and forms derivatives with DNA, RNA, and proteins, and which can react with the p53 tumor suppressor gene.Citation48 In turn, AFB1 binds to DNA to form the predominant promutagenic 8,9 dihydro-8-(N7-guanyl)-9-hydroxy AFB1 adduct. The latter can be converted into a more stable AFB1-formaminopyrimidine adduct, which causes guanine to thiamine transversion mutations. AFB1-formaminopyrimidine, incorporated into double-stranded DNA, is mutagenic, whereas the dominant species in single-stranded DNA blocks DNA replication.Citation49

The correlation between the degree of exposure to AFB1 and the incidence of HCC in humans is direct, with odds ratio for developing the tumor of 6.37:1.0 (range 3.74:1.0 to 10.86:1.0).Citation41,Citation42 An arginine to serine (G to T) mutation at codon 249 of the p53 tumor suppressor gene is specific for exposure to aflatoxin and is detected in as many as 64% of patients with HCC.Citation49Citation52 This mutation accounts for 90% of p53 mutations in AFB1-related HCC.Citation50

Synergistic interaction between AFB1 and HBV infection in hepatocarcinogenesis

The first evidence that AFB1 and HBV might act synergistically in causing HCC was provided by a study in which individuals infected with HBV who lived in villages with a “high” consumption of AFB1 were shown to have a mortality rate ten times higher than that of individuals living in villages with a “low” consumption.Citation53 A later study confirmed this observation by showing a 3.5-fold (95% confidence interval [CI]: 1.5–8.1) or a 6.0-fold (95% CI: 2–29) increase in the risk of HCC development in carriers of HBV exposed to AFB1, in comparison with those not exposed.Citation54 These clinical observations were confirmed in that HBsAg-transgenic mice developed HCC when exposed to AFB1, whereas their unexposed littermates did not.Citation55

The metabolic syndrome

In recent years, the incidence of obesity has increased alarmingly in many resource-rich countries, none more so than in the USA. In the great majority of these obese individuals, the obesity is attributed to the metabolic syndrome. Paralleling this increase in obesity has been an increase in the incidence of HCC, and it has become increasingly evident that the burgeoning incidence of obesity in the inhabitants of resource-rich countries has been the dominant reason for the striking increase in the incidence of the tumor in these countries.Citation56,Citation57 For example, the occurrence of HCC in the USA has tripled during the past 2 decades,Citation58 and the tumor, paralleling the epidemic of obesity, is now the most rapidly increasing cause of cancer deaths in that country.Citation6 This increase in the number of cancer deaths in the USA has occurred at a time when it is estimated that 25% of the population (approximately 47 million people) meet the diagnostic criteria for the metabolic syndrome: the rates are 32% in Mexican Americans, 24% in European Americans, and 22% in African Americans.Citation59 A recent meta-analysis showed the relative risk for HCC to be 1.17 (95% CI: 1.02–1.34) in those who were overweight (body mass index [BMI] 25–30 kg/m2) and 1.89 (95% CI: 1.51–2.36) in those who were obese (BMI >30 kg/m2).Citation60 In the great majority of obese individuals in whom HCC has developed, the obesity has been attributed to the metabolic syndrome. This syndrome is defined as a constellation of metabolic and other abnormalities indicated by the presence of central obesity (BMI in excess of 30 kg/m2 or increased waist circumference), plus at least two of the following clinical or biochemical components: fatty infiltration of the liver in the form of NAFLD or NASH; type 2 insulin resistance; hyperinsulinemia or overt type 2 diabetes mellitus; cirrhosis; hyperlipidemia; and systemic arterial hypertension.Citation61

The incidence of the metabolic syndrome in different parts of the world ranges from 9% to 34%,Citation62,Citation63 and it is estimated that as many as 90% of obese adults will develop the syndrome. NAFLD is currently the most common liver disease in resource-rich countries.Citation64 Ten to twenty-six percent of patients with NAFLD progress to NASH, and 8.6% of the latter become cirrhotic, although the latter progression may take many years.Citation65 Up to 50% of patients with cirrhosis as a component of the syndrome, and a significant proportion of those without cirrhosis, develop HCC. Moreover, obesity in childhood has been shown to increase the risk of HCC in adulthood.Citation65,Citation66 Depending upon geographic location, socioeconomic circumstances, and ethnicity, the metabolic syndrome continues to increase in each of these locations and circumstances. The highest incidences are believed to occur in the USA, where it has been estimated that 34% of the adult population (32.2% in males and 35.5% in females) currently meet the diagnostic criteria for the syndrome,Citation67 and the number continues to increase.

Obesity is present in 33% to 100% of patients with NAFLD, and the risk of steatosis is appreciably higher in obese than in non-obese individuals.Citation6,Citation59 NAFLD is commonly associated with insulin resistance and hyperinsulinemia.Citation65 Patients with steatosis are at risk for developing cirrhosis and HCC.Citation64 Cohorts with NASH and cirrhosis have a risk of developing HCC, which is as high as 12.8% over a 3.2-year median follow-up period.Citation68,Citation69 Although NAFLD is currently the most common liver disease in resource-rich countries, the incidence of HCC complicating NAFLD is lower than that of HCC complicating NASH (4%–27%).Citation64,Citation65 The risk of HCC developing in patients with NASH-related cirrhosis rivals that in patients with HCV-induced cirrhosis.Citation70

Much remains to be learnt about the mechanisms by which obesity and the metabolic syndrome cause HCC, although insulin resistance, increased tissue necrosis factor activity, alterations in serum lipids, NAFLD, and NASH play central roles.

Alcohol abuse

Abuse of alcohol is common in the Americas and Western Europe, and is increasing in Asia. More than 18 million adults in the USA (7% of the USA adult population) abuse alcohol, a prevalence five times higher than that of chronic HCV infection,Citation71,Citation72 Chronic alcohol abuse (consumption in excess of 80 g/day) is complicated by the development of HCC. Such abuse for more than 10 years increases the chance of HCC development approximately fivefold.Citation72 Meta-analysis has shown a dose–response relationship between alcohol intake and HCC with relative risks of 1.19 (95% CI: 1.12–1.27), 1.40 (95% CI: 1.25–1.56), and 1.81 (95% CI: 1.50–2.19) with intakes of alcohol of 25, 50, and 100 g per day, respectively.Citation73,Citation74 Alcohol abuse has been calculated to account for 32% of cases of HCC in the USACitation72 and 45% of the cases in Italy.Citation75 With very few exceptions, patients who develop the tumor have alcohol-induced cirrhosis.Citation76

Chronic alcohol consumption over at least 10 years significantly increases the risk for HCC development in patients chronically infected with either HCV or HBV, compared with patients with either viral infection who do not drink excess alcohol. Moreover, the tumor may occur at an earlier age in these patients.Citation72

Patients with both alcohol abuse and diabetes mellitus have an odds ratio of developing HCC of 9.9, suggesting a synergistic interaction between the two factors in causing the tumor.Citation77

Iron overload

Iron is ubiquitous in human cells and essential for their normal functioning, but, in excess, iron cannot be disposed of and is harmful to cells.

Only a small fraction of total body iron enters or leaves the body on a daily basis,Citation78Citation80 with both iron absorption and loss being finely regulated and balanced. Hepatocytes are the main storage sites of iron, which is stored as ferric oxyhydroxyapatite, with one molecule of ferritin binding as many as 4,500 molecules of iron.Citation78,Citation79 Hepcidin, the most important regulator of systemic iron metabolism, is influenced by body iron stores, erythropoietic activity, and hypoxia, and plays the dominant role in controlling iron absorption.Citation80 All circulating plasma iron is bound to transferrin.Citation81 Most of the iron in humans exists either in storage as ferritin or as heme.Citation82

Iron overload is generally defined as an increase in total body iron exceeding 5 g. When the level of safe sequestration of the metal is exceeded, the storage protein is denatured, releasing large amounts of iron into the cytoplasm of the hepatocytes. Accordingly, the liver is the organ most likely to be afflicted by iron overload.

Evidence continues to accrue that iron accumulation in the liver is an important risk factor for the development of HCC. The amount and duration of exposure to excess iron is crucial to the development of hepatic damage, and, with few exceptions, the development of HCC in patients with hereditary hemochromatosis (HH) occurs in the presence of cirrhosis.Citation83

Hereditary hemochromatosis

HH is an autosomally recessive inherited disorder in individuals of Celtic descent. It is characterized by increased absorption of dietary iron that results in progressive deposition of the metal in multiple organs, but particularly in the liver.Citation84 The disorder is the consequence of mutations in a number of genes concerned with iron absorption,Citation84,Citation85 the most common of which (in 70%–95% of patients) is homozygosity for the C282Y mutation of the HFE gene.Citation85,Citation86 Inappropriately low secretion of hepcidin is postulated to be the mechanism causing the consequent iron overload.Citation87

The incidence of HCC in patients with HH is 8% to 10% in most surveys, with the tumor accounting for as many as 45% of the deaths.Citation86,Citation87 Cirrhosis is present in almost all of the patients who develop the tumor.Citation88

The hepatotoxic and hepatocarcinogenic potential of excessive iron is based upon its ability to generate reactive oxygen intermediates and oxidative stress, which damage DNA, lipids, and proteins and result in necrosis and apoptosis of hepatocytes.Citation85,Citation89 In addition, there is a close link between increased iron stores and type 2 insulin resistance, which promotes hepatocarcinogenesis (see the section “The metabolic syndrome”).

It is currently not known if the direct hepatocarcinogenic effect of HH is solely attributed to the iron molecule, by virtue of its capacity to generate oxidative stress, form mutagenic hydroxyl radicles, and suppress host defense. Excess iron also acts indirectly through the induction of chronic inflammation leading to cirrhosis and hence to HCC.Citation89,Citation90 HCC has been documented to occur in iron-overloaded patients in the absence of cirrhosis,Citation90,Citation91 supporting the belief that increased hepatic iron may also directly cause or promote malignant transformation of hepatocytes.

Oxidative stress leads to lipid peroxidation of unsaturated fatty acids in membranes of cells and organelles. Cytotoxic byproducts of lipid peroxidation, such as malondialdehyde and 4-hydroxy-2′-nonenol, are produced, and these impair cellular function and protein synthesis and induce DNA damage.Citation85,Citation89 Iron is also thought to be involved in the beta-cleavage of lipid hydroperoxide, producing biogenic aldehydes that interact with DNA. In addition, deoxyguanosine residues of DNA are hydroxylated by reactive oxygen intermediates to form 8-hydroxy-2′ deoxyguanosine, a major promutagenic adduct that causes G:C to T:A transversions and DNA unwinding and strand breaks. In addition, free iron induces immunologic abnormalities that may decrease immune surveillance for malignant transformation.Citation85,Citation89

Dietary iron overload in Black Africans

Dietary iron overload has been described in rural Black Africans in at least 15 sub-Saharan African countries. The condition may affect as many as 15% of the adult male population.Citation90 It results from the consumption, over time, of large volumes of homemade beer, which has a high iron content as a consequence of it being homebrewed in iron drums or pots.Citation90 The high iron content (46–82 mg/L) of this beer contrasts with that of commercial beers (less than 0.5 mg/L).Citation92 During the fermentation of the sorghum or other locally grown crops, the pH of the ferment decreases to a very low level (pH 3.5–3.8), leaching iron from the container into the contents.Citation92 The iron is in an ionized, highly bioavailable form. Serum iron values in the iron-overloaded individuals range between 32 and 519 mmol/g dry weight (geometric mean 128 mmol/g). Hepatic iron concentrations greater than 1% dry weight are present in 43.2% of the males and 16.6% of the females.Citation90 Portal fibrosis is present in 58% of the individuals, and cirrhosis in 10%. Females are protected against the iron overload as a result of iron losses during menstruation and childbearing.

Dietary iron overload may be complicated by the development of HCC, with the relative risk ranging from 1.5 to 76.8, with a mean figure of 10.6%.Citation91

The association between the iron overload and the development of HCC has been confirmed in studies in rats fed a high-iron diet. After 15 months, the iron-loaded liver developed HCC in the absence of cirrhosis.Citation92

Membranous obstruction of the inferior vena cava

Membranous obstruction of the inferior vena cava (MOIVC) is an occlusive lesion of the inferior vena cava, usually complete, but occasionally with a small central opening, which is located close to the entrance of the inferior vena cava into the right atrium or just below the level of the diaphragm. Although usually in the form of a membrane of variable thickness, it may take the form of a fibrotic occlusion of variable length. The condition occurs more often in men than in women, and most patients are in their 30s, 40s, or 50s. MOIVC is rare in most countries, but occurs more frequently in Southern Africa, India, Japan, Nepal, the People’s Republic of China, and Korea.Citation93 For example, it occurs in 4% of sub-Saharan Black Africans.Citation93 It is uncertain whether the lesion is a congenital vascular anomaly or the result of organization of a thrombus in the hepatic portion of the inferior vena cava.Citation93 The lesion impedes hepatic venous drainage, causing chronic hepatic venous congestion and centrilobular fibrosis of the liver.

MOIVC may be complicated by the development of HCC. The risk varies between different geographical regions, being highest in South African Blacks, with a risk of 40% to 48%.Citation94 Incidences in countries other than South Africa range between 4.7% and 23%.Citation94,Citation95 African patients with HCC complicating MOIVC are younger than those with the tumor but without the obstruction resulting from MOIVC.Citation94

The reason for the malignant transformation is unknown, although it is not thought to be a direct consequence of the occlusive lesion. Rather, the centrilobular necrosis and regeneration resulting from the hepatic venous hypertension and congestion, by acting as a tumor promoter, predisposes to one or more environmental carcinogens prevalent in those countries where HCC often complicates MOIVC. This belief is supported by the geographical distribution of the complicating HCC in Southern Africa.Citation94,Citation96

Tobacco smoking

A relatively small number of studies have addressed the question of smoking as a cause of HCC.Citation97,Citation98 Nevertheless, these have shown increased odds ratios for the development of the tumor in cigarette smokers. For example, odds ratios of 1.7 (95% CI: 1.0–2.9) in current smokers compared with nonsmokersCitation97 and 1.56 (95% CI: 1.29–1.87) in current smokers compared with never-smokersCitation98 have been documented, as has a ratio of 1.49 (95% CI: 1.06–2.10) in former smokers compared to never-smokers.Citation98 On the basis of studies of the odds ratios, some authorities have not regarded smoking as a risk factor because of the uncertainty introduced by the confounding effects of alcohol consumption and HBV and HCV infections.Citation99 However, the International Agency for Research in CancerCitation99 regards smoking as a risk factor, and most authorities concur with this conclusion.Citation99

Oral contraceptive steroids

Although a number of studies devoted to the hepatocarcinogenicity of oral contraceptives have been published, the evidence available in this regard is inconclusive at present.Citation100

Disclosure

The author reports no conflicts of interest in this work.

References

  • FerlayJShinHBrayFFormanDMathersCParkinDMEstimates of worldwide burden of cancer in 2008: GLOBOCAN 2008Int J Cancer20101272893291721351269
  • JemalABrayFCenterMMGlobal cancer statisticsCarcinogenesis2011616990
  • KewMCHepatocellular Carcinoma in Sub-Saharan AfricaTrafford Publishing (North America and International)2012810
  • GLOBOCANLyon International Agency for Research on Cancer (IARC) Available from: http://www-dep.iarc.fr. Accessed
  • Mortality DatabaseWHO Statistical Information SystemGenevaWorld Health Organization2008 Available from: http://www.who.int/whosis. Accessed
  • AltekruseSFMcGlynnKAReichmanMEHepatocellular carcinoma incidence, mortality, and survival trends in the United States from 1975 to 2005J Clin Oncol2009271485149119224838
  • MittalSEl-SeragHBEpidemiology of hepatocellular carcinoma: consider the populationJ Clin Gastroenterol201347SupplS2S623632345
  • LlovetJMBurroughsABruixJHepatocellular carcinomaLancet20033621907191714667750
  • BoschFXRibesJBorràsJEpidemiology of primary liver cancerSemin Liver Dis19991927128510518307
  • ChangMHChenCJLaiMSUniversal hepatitis B vaccination in Taiwan and the incidence of hepatocellular carcinoma in children. Taiwan Childhood Hepatoma Study GroupNew Engl J Med1997336185518599197213
  • Chinese Academy of Medical SciencesAtlas of Cancer Mortality in the People’s Republic of ChinaBeijingChina Map Press1981
  • PratesMDTorresFOA cancer survey in Lourenço Marques, Portuguese East AfricaJ Natl Cancer Inst1965357297575892211
  • KewMCRossouwEHodkinsonHJPatersonADusheikoGMWhitcuttJMHepatitis B virus status of southern African Blacks with hepatocellular carcinoma: comparison between rural and urban patientsHepatology1983365686295908
  • BoschFXGlobal epidemiology of hepatocellular carcinomaOkudaKTaborELiver CancerNew YorkChurchill Livingstone19971328
  • PignataSGalloCDanieleBCLIP InvestigatorsCharacteristics at presentation and outcome of hepatocellular carcinoma (HCC) in the elderly. A study of the Cancer of the Liver Italian Program (CLIP)Crit Rev Oncol Hematol20065924324916916608
  • KewMCMacerolloPThe effect of age on the role of hepatitis B virus in hepatocellular carcinoma in blacksGastroenterology1988944394422446950
  • PisaniPParkinDMBrayFFerlayJEstimates of the worldwide mortality from 25 cancersInt J Cancer19991087087310602059
  • KewMCThe role of cirrhosis in the etiology of hepatocellular carcinomaJ Gastrointest Cancer201445122124203525
  • BlumbergBSLarouzéBLondonWTThe relation of infection with the hepatitis B agent to primary hepatic carcinomaAm J Pathol197581669682174434
  • KewMCEpidemiology of chronic hepatitis B virus infection, hepatocellular carcinoma, and hepatitis B virus-induced hepatocellular carcinomaPathol Biol (Paris)20105827327720378277
  • ParkinDMBrayFFerlayJPisaniPEstimating the world cancer burden: Globocan 2000Int J Cancer20019415315611668491
  • NguyenVTTAminJLawMPredictors and survival in hepatitis B virus-related hepatocellular carcinoma in New South Wales, AustraliaJ Gastroenterol Hepatol20082443644219175834
  • OkudaKClinical aspects of hepatocellular carcinoma: analysis of 134 casesOkudaKPetersRLHepatocellular CarcinomaNew YorkJohn Wiley and Sons387436
  • HigginsonJThe geographical pathology of primary liver cancerCancer Res1963231624163314098901
  • KewMCDos SantosHASherlockSDiagnosis of primary cancer of the liverBr Med J197144084115124443
  • BeasleyRPHwangLYHepatocellular carcinoma and hepatitis B virusSemin Liver Dis198441131216087457
  • BothaJFRitchieMJDusheikoGMMoutonHWKewMCHepatitis B virus carrier state in black children in Ovamboland: role of perinatal and horizontal infectionLancet19842121012126144925
  • No authors listedHepatocellular carcinoma: differences between high and low incidence regionsLancet19872118311842890810
  • ShafritzDAShouvalDShermanHIHadziyannisSJKewMCIntegration of hepatitis B virus DNA into the genome of liver cells in chronic liver disease and hepatocellular carcinoma. Studies in percutaneous liver biopsies and post-mortem tissue specimensN Engl J Med1981305106710736268980
  • KewMCHepatitis B virus x protein in the pathogenesis of hepatitis B virus-induced hepatocellular carcinomaJ Gastroenterol Hepatol201126Suppl 114415221199526
  • FeitelsonMABonamassaBArzumanyanAThe roles of hepatitis B virus-encoded X protein in virus replication and the pathogenesis of chronic liver diseaseExpert Opin Ther Targets20141829330624387282
  • KewMCFrançoisGLavanchyDViral Hepatitis Prevention BoardPrevention of hepatitis C virus infectionJ Viral Hepat20041119820515117321
  • HutinYKitlerMEDoreGGlobal burden of disease for hepatitis CJ Clin Pharmacol2003432029
  • Hepatitis VirusesLyonInternational Agency for Research on Cancer (IARC)1994165221
  • KewMCHepatitis C virus and hepatocellular carcinoma in developing and developed countriesViral Hepatit Rev19984259269
  • BrunoSSiliniECrosignaniAHepatitis C virus genotypes and risk of hepatocellular carcinoma in cirrhosis: a prospective studyHepatology1997257547589049231
  • ZampinoRMarroneERestivoLChronic HCV infection and inflammation: clinical impact on hepatic and extra-hepatic manifestationsWorld J Hepatol2013552854024179612
  • KewMCHepatitis C virus and hepatocellular carcinomaFEMS Microbiol Rev1994142112198086196
  • Di BisceglieAMSimpsonLHLotzeMTHoofnagleJHDevelopment of hepatocellular carcinoma among patients with chronic liver disease due to hepatitis C viral infectionJ Clin Gastroenterol1994192222267528758
  • International Agency for Research on CancerSome Traditional Herbal Medicines, Some Mycotoxins, Naphthalene and Styrene IARC Monographs on the Evaluation of the Carcinogenic Risks to Humans82LyonIARC Press2002
  • WilliamsJHPhillipsTDJollyPEStilesJKJollyCMAggarwalDHuman aflatoxicosis in developing countries: a review of toxicology, exposure, potential health consequences, and interventionsAm J Clin Nutr2004801106112215531656
  • StrosniderHAzziz-BaumgartnerEBanzigerMWorkgroup report: public health strategies for reducing aflatoxin exposure in developing countriesEnviron Health Perspect20061141898190317185282
  • LiuYChangCCMarshGMWuFPopulation attributable risk of aflatoxin-related liver cancer: systematic review and meta-analysisEur J Cancer2012482125213622405700
  • WildCPPionneayFMontesanaRAflatoxin detected in milk by immunoassayVir Hepatit Rev19984259269
  • WildCPTurnerPCThe toxicology of aflatoxins as a basis for public health decisionsMutagenesis20021747148112435844
  • BressacBKewMCWandsJOzturkMSelective G to T mutations of p53 gene in hepatocellular carcinoma from southern AfricaNature19913504294311672732
  • BrownRLChenZYClevelandTERussinJSAdvances in the development of host resistance in corn to aflatoxin contamination by Aspergillus flavusPhytopathology19998911311718944783
  • HsuICMetcalfRASunTWelshJAWangNJHarrisCCMutational hotspot in the p53 gene in human hepatocellular carcinomasNature19913504274281849234
  • KirkGDCamus-RandonAMMendyMSer-249 p53 mutations in plasma DNA of patients with hepatocellular carcinoma from The GambiaJ Natl Cancer Inst20009214815310639517
  • GouasDShiHHainautPThe aflatoxin-induced TP53 mutation at codon 249 (R249S): biomarker of exposure, early detection and target for therapyCancer Lett2009286293719376640
  • KewMCAflatoxins as a cause of hepatocellular carcinomaJ Gastrointest Liver Dis201322306310
  • YehFSMoCCYenRCRisk factors for hepatocellular carcinoma in Guangxi, People’s Republic of ChinaNatl Cancer Inst Monogr19896947483010122
  • YuMWLienJPChiuYHSantellaRMLiawYFChenCJEffect of aflatoxin metabolism and DNA adduct formation on hepatocellular carcinoma among chronic hepatitis B carriers in TaiwanJ Hepatol1997273203309288607
  • MingLThorgeirrsonSSGailMHDominant role of hepatitis B and cofactor role of aflatoxin in hepatocarcinogenesis in Qidong, ChinaHepatology2002361214122012395332
  • SellSHuntJMDunsfordHJChisariFVSynergy between hepatitis B virus expression and chemical hepatocarcinogens in transgenic miceCancer Res199151127812851847661
  • CalleEERodriguezCWalt-ThurmondKOver-weight, obesity, and cancer riskLancet Oncol20023486251638
  • BianchiniFKaaksRVainioHOverweight, obesity, and cancer riskLancet Oncol2002356557412217794
  • El-SeragHBHepatocellular carcinomaN Engl J Med20113651118112721992124
  • BorenaWStrohmaierSLukanovaAMetabolic risk factors and primary liver cancer in a prospective study of 578,700 adultsInt J Cancer201213119320021805476
  • WelzelTMGraubardBIZeuzemSEl-SeragHBDavilaJAMcGlynnKAMetabolic syndrome increases the risk of primary liver cancer in the United States: a study in the SEER-Medicare databaseHepatology20115446347121538440
  • MarchesiniGBriziMMorselli-LabateAMAssociation of nonalcoholic fatty liver disease with insulin resistanceAm J Med199910745045510569299
  • TakumatsoSNoguvchiNKurdoleKInfluence of risk factors for metabolic syndrome and in alcoholic fatty liver disease on the prognosis and progress of hepatocellular carcinomaHepatogastroenterology20085560961418613418
  • FordESGilesWHMokdadHHPrevalence of metabolic syndrome among US AdultsDiabetes Care20042102444244915451914
  • LazoMClarkJMThe epidemiology of nonalcoholic fatty liver disease: a global perspectiveSemin Liver Dis20082833935018956290
  • NobiliVAlisiAGrimaldiCNon-alcoholic fatty liver disease and hepatocellular carcinoma in a 7-year-old obese boy: coincidence or comorbidity?Pediatr Obes Epub1232013
  • ErvinRBPrevalence of metabolic syndrome among adults 20 years of age and over, by sex, age, race and ethnicity, and body mass index: United States, 2003–2006Natl Health Stat Report2009131719634296
  • AdamsLALympJFSt SauverJThe natural history of nonalcoholic fatty liver disease: a population-based cohort studyGastroenterology200512911312116012941
  • AschaMSHanounehIALopezRTamimiTAFeldsteinAFZeinNNThe incidence and risk factors of hepatocellular carcinoma in patients with nonalcoholic steatohepatitisHepatology2010511972197820209604
  • SchlesingerSAleksandrovaKPischonTAbdominal obesity, weight gain during adulthood and risk of liver and biliary tract cancer in a European cohortInt J Cancer201313264565722618881
  • MatteoniCAYounossiZMGramlichTBoparaiNLiuYCMcCulloughAJNonalcoholic fatty liver disease: a spectrum of clinical and pathological severityGastroenterology19991161413141910348825
  • GrantBHarfordTDawsonDAlcohol abuse and dependence: United States 1992Alcohol Health Res World199418243248
  • MorganTRMandayamSJamalMMAlcohol and hepatocellular carcinomaGastroenterology20041275 Suppl 1S87S9615508108
  • BoffettaPHashibeMAlcohol and cancerLancet Oncol2006714915616455479
  • ChiesaRDonatoFTaggerAEtiology of hepatocellular carcinoma in Italian patients with and without cirrhosisCancer Epidemiol Biomarkers Prev2000921321610698484
  • DonatoFTaggerAChiesaRHepatitis B and C virus infection, alcohol drinking, and hepatocellular carcinoma: a case-control study in Italy. Brescia HCC StudyHepatology1997265795849303486
  • NzeakoUCGoodmanZDIshakKGHepatocellular carcinoma in cirrhotic and noncirrhotic livers. A clinico-histopathologic study of 804 North American patientsAm J Clin Pathol199610565758561091
  • DonatoFTaggerAGelattiUAlcohol and hepatocellular carcinoma: the effect of lifetime intake and hepatitis virus infections in men and womenAm J Epidemiol200215532333111836196
  • AndrewsNCDisorders of iron metabolismN Engl J Med19993411986199510607817
  • HuangXIron overload and its association with cancer risk in humans: evidence for iron as a carcinogenic metalMutat Res2003533152171
  • McCordJMIron, free radicals, and oxidative injurySemin Hematol1998355129460805
  • GreeneCMVarleyRBLawlessMWMicroRNAs and liver cancer associated with iron overload: therapeutic targets unravelledWorld J Gastroenterol2013195212522623983424
  • LudwiczekEAignerITheurlIWeissGCytokine-mediated regulation of iron transport in human monocytic cellsBlood20031014148415412522003
  • TothIYuanLRogersJTBoyceHBridgesKRHypoxia alters iron-regulatory protein-I binding capacity and modulates cellular iron homeostasis in human hepatoma and erythroleukemia cellsJ Biol Chem1999274446744739933651
  • ToyokuniSRole of iron in carcinogenesis: cancer as a ferrotoxic diseaseCancer Sci200910091619018762
  • HaddowJEPalomakiGEMcClainMCraigWHereditary haemochromatosis and hepatocellular carcinoma in males: a strategy for estimating the potential for primary preventionJ Med Screen200310111312790309
  • StrohmeyerGNiederauCStremmelWSurvival and causes of death in hemochromatosis. Observations in 163 patientsAnn NY Acad Sci19885262452573389643
  • PowellLWYappTRHemochromatosisClin Liv Dis20004211228
  • FrancanzaniALConteDFraquelliMIncreased cancer risk in a cohort of 230 patients with hereditary hemochromatosis in comparison to matched control patients with non-iron-related chronic liver diseaseHepatology20013364765111230745
  • OlnykJKSt PierreTGBrittonRSBruntEMBaconBRDuration of hepatic iron exposure increases the risk of significant fibrosis in hereditary hemochromatosis: a new role for magnetic resonance imagingAm J Gastroenterol200510083784115784029
  • KowdleyKVIron, hemochromatosis, and hepatocellular carcinomaGastroenterology20041275 Suppl 1S579S586
  • HassanMMHwangLYHattenCJRisk factors for hepatocellular carcinoma: synergism of alcohol with viral hepatitis and diabetes mellitusHepatology2002361206121312395331
  • KewMCAsareGADietary iron overload in the African and hepatocellular carcinomaLiver Int20072773574117617115
  • KewMCHodkinsonHJMembranous obstruction of the inferior vena cava and its causal relation to hepatocellular carcinomaLiver Int2006261716420504
  • SimsonIWMembranous obstruction of the inferior vena cava and hepatocellular carcinoma in South AfricaGastroenterology1982821711786274728
  • GwonD2ndKoGYYoonHKHepatocellular carcinoma associated with membranous obstruction of the inferior vena cava: incidence, characteristics, and risk factors and clinical efficacy of TACERadiology201025461762620093533
  • KewMCMcKnightALakisNMembranous obstruction of the inferior vena cava by tumor in hepatocellular carcinomaTrop Gastroenterol1989101731782554548
  • ChuangSCLa VecchiaCBoffettaPLiver cancer: descriptive epidemiology and risk factors other than HBV and HCV infectionCancer Lett200928691419091458
  • GandiniSBotteriEIodiceSTobacco smoking and cancer: a meta-analysisInt J Cancer200812215516417893872
  • International Agency for Research on CancerTobacco Smoke and Involuntary Smoking IARC Monographs on the Evaluation of the Carcinogenic Risks to Humans83LyonIARC200411438
  • MaheswariSSarrajAKramerJEvidence at this time is inconclusive to establish the relation between oral contraceptive steroids and risk of hepatocellular carcinomaJ Hepatol20074750651317462781
Download PDF

Related research

People also read lists articles that other readers of this article have read.

Recommended articles lists articles that we recommend and is powered by our AI driven recommendation engine.

Cited by lists all citing articles based on Crossref citations.
Articles with the Crossref icon will open in a new tab.