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Advances in the molecular characterization of biliary tract and gallbladder cancer
Biliary tract cancers
First described by Durand-Fardel in 1840, biliary tract tumors arise from cholangiocytes residing in the biliary tree. The biliary tract cancers include intrahepatic cholangiocarcinoma (IHCC, within the liver; see Chapter 50 ), extrahepatic cholangiocarcinoma (EHCC, within the extrahepatic biliary tree; see Chapter 51 ), and gallbladder cancer (GBCA, within the gallbladder; see Chapter 49 ). Recently, it has been recognized that some subtypes of IHCC can arise from hepatic progenitor cells or have stem cell features (see Chapter 9C ). Thus combined or mixed hepatocellular cholangiocarcinoma (C-HCC), which has cells with a phenotype that is intermediate between hepatocellular carcinoma (HCC) and cholangiocarcinoma (CCA), is occasionally seen and considered to be a subtype of IHCC (see Chapters 47 , 50 , and 89 ). These biliary tract cancers constitute a rare set of malignancies and mostly present as locally advanced or metastatic disease. Because of their rarity, as well as their common cell of origin, systemic treatment for all these tumor types has been identical, but chemotherapeutic regimens lack significant response rates. In patients with advanced disease, goals of systemic chemotherapy are still palliative in nature (see Chapters 47 and Chapter 49, Chapter 50, Chapter 51 ). With fairly recent developments in next-generation sequencing (NGS) and other molecular techniques; however, comprehensive molecular profiling now enables the identification of unique genetic signatures among these cancers and is important in clinical trial design using drugs to target specific pathways.
Classification
The vast majority of biliary tract tumors are adenocarcinomas, and they most often arise at or near the biliary confluence. The latter fall under the general category of EHCCs (see Chapter 51 ), which are further subcategorized into hilar CCA (also known as Klatskin tumor ) and distal CCA, with the transition occurring proximal to the cystic duct in the current American Joint Committee on Cancer TNM Classification and National Comprehensive Cancer Network (NCCN) guidelines. , These are further categorized as perihilar CCA by their precise location with reference to the biliary bifurcation and the hepatic lobar ducts. This classification is most useful for descriptive purposes and for operative planning. In contrast to the perihilar tumors, the distal CCAs account for a relatively small fraction of all bile duct tumors. Mid-bile duct tumors are even less common and often turn out to represent tumors of the gallbladder or cystic duct. Diffuse involvement of the entire biliary tree is a very rare condition, affecting a very small fraction of patients with biliary tract cancer. CCA may also arise from the intrahepatic bile ducts, giving rise to the subgroup known as IHCC (or peripheral CCA; see Chapter 50 ). IHCCs can also be subcategorized by their growth characteristics into three groups: mass-forming , periductal-infiltrating , or intraductal growing types. Until recently, International Classification of Disease (ICD) codes combined IHCC with HCC under the code for primary liver tumor, , but these are clearly different entities, and the second and third editions of the ICD for Oncology (ICD-O-2/3) have attempted to correct for this issue. In ICD-O-2, hilar tumors were assigned a unique histology code, but this was cross-referenced to the topography code for intrahepatic rather than extrahepatic tumors. Under the third ICD-O-3 edition, hilar tumors are cross-referenced to either location. In addition to the aforementioned coding issues, many tumors previously referred to as liver adenocarcinoma of unknown primary site were likely unrecognized IHCCs. Together, these changes in ICD classification have influenced observed changes in the incidence rates of IHCC and EHCC.
Epidemiology
Although rare, biliary tract cancer has a distinctly higher incidence in certain demographic groups and geographic regions (see Chapters 49 , 50 , and 51 ). GBCA has a higher incidence among females and in South America, whereas IHCC is more common in Asia. The peak incidence of the biliary tract cancers is the seventh decade of life, with a slightly higher male predilection. In the United States, an estimated 6,300 new IHCC cases were diagnosed, whereas 12,360 new EHCC or GBCA cases were diagnosed in 2019. Outside of the United States, the incidence rates vary globally, presumably reflecting differences in infectious causes, environmental risk factors (i.e., sedentary lifestyles, alcohol, smoking, and diet), exposure to toxic chemicals, and genomics. The highest incidence rate is in Northeast Thailand (age-standardized incidence rate [ASIR]: 85/100,000 population), where it occurs approximately 100 times more often than in the West. High prevalence of carcinogenic liver flukes is associated with the high incidence rates of biliary tract cancers. Nevertheless, in the United States, IHCC and EHCC incidence rates have steadily increased from 1999 to 2013 across sex and racial/ethnic groups (estimated annual percent change [eAPC]: 3.2% for IHCC and 1.8% for EHCC). Also, in other countries (e.g., Japan, Australia, and many European countries), increased rates for IHCC are widely reported. In contrast, the overall GBCA incidence rate has been stable or declining, although it increased among African Americans (eAPC: 1.8%) and people aged less than 45 years (eAPC: 1.8%). , The increased incidence of IHCC and EHCC may be attributable, in part, to the fact that several risk factors (e.g., cirrhosis and obesity) have increased globally over recent decades. The increased detection of early stage or smaller tumors may also be considered a reason, as would be expected if the increase were only because of an improvement in diagnostic modalities, such as magnetic resonance imaging (MRI) and computed tomography (CT). , ,
Epidemiologic data over the last few decades have also shown that the mortality rate of IHCC is rising globally, whereas the mortality rates of EHCC and GBCA have decreased in most countries. , The GBCA mortality rates declined after the increase of cholecystectomy. Despite recent imaging modality developments, most patients presenting with unresectable or metastatic disease still typically die within 12 months of diagnosis. In addition to a lack of highly efficacious systemic therapies, sepsis from cholangitis, frequently related to interventions performed for biliary obstruction and progressive liver failure, contribute to the high mortality. Although biliary tract tumors remain relatively rare, there has been increased interest in studying the biology of these diseases in recent years.
Chronic biliary inflammation and cholestasis
Clinical risk factors
There are multiple risk factors for biliary tract cancers. The heterogeneous tumor phenotypes and molecular findings can be explained by a complicated interaction between the unique genetic background of a patient and their exposure to the risk factors. Reported risk factors for these tumors are a diverse group of conditions that include infectious causes, congenital conditions, inflammatory diseases, drugs, environmental exposures, and toxins. , , Congenital biliary duct cysts (including Caroli disease; see Chapter 46 ) and cholangitis (including primary sclerosing cholangitis [PSC]; see Chapter 41 ) are established as well-known risk factors. The high prevalence of these diseases affects the high incidence rates in the female population of Asian countries (e.g., China and Japan). In addition, previous studies found that biliary cirrhosis, cholelithiasis, hepatolithiasis, alcoholic liver disease, nonalcoholic fatty liver disease/steatohepatitis (NAFLD/NASH), nonspecific cirrhosis, diabetes type II, thyrotoxicosis and chronic pancreatitis, obesity, chronic hepatitis B virus infection (HBV), hepatitis C virus (HCV) infection, human immunodeficiency virus (HIV) infection, and smoking were associated with the development of biliary tract cancers , (see Chapter 49, Chapter 50, Chapter 51 ). A recent systematic review suggests that the rising global incidence of IHCC may be associated with increases in diabetes type II, alcoholic liver diseases, and cholelithiasis. Liver flukes ( Opisthorchis viverrini and Clonorchis sinensis ) are also major causes in East Asia, especially in Thailand and Laos. Thorotrast, which was previously used as an intravascular contrast agent, is also carcinogenic and associated with a 64-fold increased odds ratio of developing CCA. Occupational exposures to 1,2-dichloropropane or asbestos have become well-known as strong risk factors in recent years. Some studies using nationwide databases support that inflammatory bowel disease is associated with the increased risk for these cancers as well. , Based on the aforementioned predisposing factors, a common theme of chronic biliary epithelial inflammation appears to be a predisposing factor for the development of biliary tract cancers. PSC is the most common condition predisposing to CCA, with incidence rates of 0.5 to 1.5 per 100 person-years reported in patients with PSC (400-fold the risk in the general population). , Although the incidence of CCA in pediatric PSC patients is very rare, CCA in adult PSC patients is seen most commonly less than 1 year after the diagnosis of PSC. , Congenital abnormalities of the biliary tree, congenital hepatic fibrosis, and choledochal cysts (cystic dilatations of the bile ducts) also carry a 15% risk of malignant change. , Furthermore, with untreated choledochal cysts, the risk of biliary tract cancers increases to 28%. , Biliary stasis, reflux of pancreatic juice, activation of bile acids, and deconjugation of carcinogens are speculated as mechanistic drivers of carcinogenesis related to the theme of chronic inflammation.
Biology of clinical risk factors
Several underlying mechanisms play a role in the induction of chronic biliary inflammation and cholestasis.
Bile content and deconjugation of xenobiotics
Polymorphisms in bile salt transporter proteins (i.e., BSEP, ATP8B1, and ABCB4) can lead to unstable bile content and deconjugation of environmental toxins (i.e., xenobiotics) previously conjugated in the liver. , In the background of congenital bile duct abnormalities, this process increases the risk of CCA. Individuals who are heterozygous for bile salt transporter polymorphisms are thought to have an increased predisposition to cancer as adults, following exposure to cofactors that result in chronic inflammation in the biliary tree.
DNA mutagens
Promutagenic DNA adducts have been identified in biliary tract cancer tissue, indicating exposure to DNA-damaging agents. Although the mechanisms have not been fully elucidated, Thorotrast has a very long half-life and induces biliary tract cancers, possibly because of the release of alpha particles with high linear energy transfer, inducing mutations in various oncogenes and tumor suppressor genes, which leads to their activation. Inflammatory conditions, such as chronic viral infections (e.g., HBV and HCV) or alcoholic/nonalcoholic hepatitis, promote carcinogenesis by producing reactive oxygen and nitrogen species from inflammatory and epithelial cells, activating reparative tissue proliferation, and creating a local environment rich in cytokines and other growth factors, ultimately resulting in DNA damage. , Exposures to 1,2-dichloropropane and asbestos fibers also increase DNA double-strand breaks. ,
Inherited syndrome
Lynch syndrome, an autosomal dominant predisposition for DNA mismatch repair, is associated with a high incidence of colorectal, endometrial, stomach, ovary, pancreas, ureter and renal pelvis, bile duct, and brain tumors. The associated lifetime risk for bile duct cancer in patients with Lynch syndrome is 1% to 4% ( Cancer.Net , https://www.cancer.net/cancer-types/lynch-syndrome ). Although hereditary and not environmental, deficiency of DNA repair is a recurrent theme in the development of biliary tract cancers.
Molecular pathogenesis
The molecular pathogenesis of biliary tract tumors has recently become an area of vigorous investigation (see Chapters 9A and 9C ). In the era of advanced molecular analyses, including NGS, rapid progress is being made in our understanding of the genomic basis of these malignancies. Tumor profiling of biliary tract cancers has revealed that molecular profiles differentiate IHCC, EHCC, and GBCA and that every tumor has both biologically complex and individually unique molecular alterations, suggesting individualized therapeutic options. It is beyond the scope of this chapter to document every known molecular alteration reported or associated with biliary tract cancers. Instead, we focus on recurrent themes in altered signaling pathways that together result in the pathogenic phenotypes and potential drug targets ( Fig. 9E.1 ).
Biology of biliary epithelial injury and repair
Similar to the development of other tumors, biliary tract carcinogenesis is thought to be a multistep process dependent on the interaction between environmental factors and host genetic factors. Most of the putative environmental risk factors for CCA result in chronic biliary inflammation, leading to tissue-repair mechanisms and, ultimately, carcinogenesis.
Conceptually, exposure to an inflammatory stimulus would not have the same effect on each cell because of changes in perfusion (e.g., centrilobular versus periportal), as well as differential levels of cytochrome P450 (CYP) expression, exposure to bile salt concentrations, and exposure to inflammatory components (e.g., cytokines and immune surveillance cellular components, such as Kupffer cells and hepatic stellate cells; see Chapters 7 and 10 ). Based on this, the concept of heterogeneity can be inferred where distinct clonal populations may arise based on differential response to stimuli. In this section, we review the underlying host factors associated with bile tract cancers.
Genetic polymorphism at cytochrome P450
Genetic polymorphisms exist in the CYP450 enzyme complex, a large family of constitutive and inducible enzymes that play a central role in the oxidative metabolism of both environmental toxins and endogenous compounds. These polymorphisms play a critical role in how endogenous and exogenous toxins are biotransformed by the liver. Similar to many other cancers, which rely on a sequence of chronic injury and repair, the development of CCA may be partially regulated by the host ability to respond toxic to insults.
Several CYPs are involved in the metabolism of oxysterols, that are cholesterol oxidation products with expression that may be dysregulated in inflammation-related diseases, including cancer. For instance, 1,2-dichloropropane, a DNA mutagen as previously mentioned, influences the proliferation and apoptosis of cholangiocytes via CYP450. CYP39A1, which can metabolize 24-hydroxycholesterol, is downregulated in 70% of CCA and plays an important role in the inflammatory response and oxidative stress. Low expression of CYP39A1 correlates with disease metastasis. Also, CYP2A6 and CYP2E1 are upregulated in Opisthorchis -associated CCA and indicate that enhanced CYP2A6 activity and diminished CYP2E1 activity are involved in the progression of CCA. Finally, molecular profiling of EHCC specimens demonstrated significant enrichment of CYP-metabolic pathways, including transcription factors such as glutathione-S-transferase α1 (GSTA1) and GSTA3, which may cause abnormal gene expression and tumorigenesis through CYP450-metabolic pathways. Differential CYP activity may be involved in the initiation and/or progression of disease via modulation of chronic inflammation, metabolism of exogenous compounds (e.g., drugs, tobacco, and nitrosamines), viral hepatitis, parasitic infestation, and recurrent cholangitis.
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