preneoplastic lesions in human hepatocarcinogenesis

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PRENEOPLASTIC LESIONS IN HUMAN HEPATOCARCINOGENESIS

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Preneoplastic lesions in human hepatocarcinogenesis. Hepatocellular carcinoma (HCC) is the fifth most frequent cancer in the world and the third most common cause of cancer mortality. - PowerPoint PPT Presentation

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Page 1: Preneoplastic  lesions in human hepatocarcinogenesis

PRENEOPLASTIC LESIONS IN HUMAN

HEPATOCARCINOGENESIS

Page 2: Preneoplastic  lesions in human hepatocarcinogenesis

Hepatocellular carcinoma (HCC) is the fifth most frequent cancer in the world and the third most common cause of cancer mortality.

Page 3: Preneoplastic  lesions in human hepatocarcinogenesis

The early stages of hepatocarcinogenesis in human chronic liver diseases are characterized by the emergence of preneoplastic lesions of whichsome will eventually develop into hepatocellular carcinoma (HCC).

Page 4: Preneoplastic  lesions in human hepatocarcinogenesis

Basic studies on the genetic and epigenetic alterations of these preneoplastic lesionsmay eventually lead to new therapeutic strategies.

Page 5: Preneoplastic  lesions in human hepatocarcinogenesis

Clinicopathological studies are also important in order to determine optimal management of patients with apreneoplastic lesion.

Page 6: Preneoplastic  lesions in human hepatocarcinogenesis

The microscopical small-cell dysplastic focus is the smallest morphologically recognizable precursor lesion of HCC and therefore is a logical target ofstudy to elucidate the earliest events in hepatocarcinogenesis.

Page 7: Preneoplastic  lesions in human hepatocarcinogenesis

In contrast, large-cell dysplasia is not a precursor lesion, but appears to be of clinical value because of its good predictive value for development of HCC.

Page 8: Preneoplastic  lesions in human hepatocarcinogenesis

Dysplastic nodules (DNs) are macroscopically recognizable precursor lesions of HCC and high-grade DNs (HGDNs) have a risk of malignant transformation.

Page 9: Preneoplastic  lesions in human hepatocarcinogenesis

Detection of DNs and correct differentiation from small HCC (0.2 cm) is sometimes difficult, especially when only imaging techniques are used.

Page 10: Preneoplastic  lesions in human hepatocarcinogenesis

Additional clinicopathological studies on identification and optimal treatment of DNs are necessary.

Page 11: Preneoplastic  lesions in human hepatocarcinogenesis

Molecular studies on HGDNs and small HCCs may yield much information on the genetic mechanisms involved in the transition from severe dysplasia to early malignancy

Page 12: Preneoplastic  lesions in human hepatocarcinogenesis

In contrast,currently available data indicate that (large) regenerative nodules do notrepresent a distinct step in hepatocarcinogenesis.

Page 13: Preneoplastic  lesions in human hepatocarcinogenesis

HCCs mostly develop in patients with chronic liver disease caused by viral hepatitis, alcohol abuse and inborn metabolic errors.

Page 14: Preneoplastic  lesions in human hepatocarcinogenesis

Eighty percent of all HCCs worldwide occur when the underlying chronic liver disease has reached the cirrhotic stage.

Page 15: Preneoplastic  lesions in human hepatocarcinogenesis

These numbers and percentages clearly illustrate the important impact of this malignant tumor on public health and underscore the relevance of studies focusing on the development and evolution of HCC

Page 16: Preneoplastic  lesions in human hepatocarcinogenesis

The development and progression of a HCC in a chronically diseased liver, frequently referred to as ‘hepatocarcinogenesis’, is a multistep and long-term process characterized by the progressive accumulation and interplay of genetic alterations

Page 17: Preneoplastic  lesions in human hepatocarcinogenesis

causing aberrant growth and malignant transformationof liver parenchymal cells, followed by vascular invasion and metastasis (3). Hepatitis Bvirus (HBV), hepatitis C virus (HCV) and alcohol

Page 18: Preneoplastic  lesions in human hepatocarcinogenesis

a large geographic variation ranging from 120 in Eastern Asia to two in Australia. The incidence of HCC in Europe and the USA is rather low but steadily increasing, The annual rate of HCC per 100 000 person-years shows are some of the most frequent hepatocarcinogens in humans and they probably cause direct damage to the DNA.

Page 19: Preneoplastic  lesions in human hepatocarcinogenesis

Recent studies of gene expression patterns using microarray analysis suggest that each HCC has its ownunique profile and history of genetic alterations

Page 20: Preneoplastic  lesions in human hepatocarcinogenesis

These carcinogens also cause indirect damage and impaired repair of DNA via chronic necro-inflammation, intensive regeneration and fibrogenesis

Page 21: Preneoplastic  lesions in human hepatocarcinogenesis

To render things even more complex, there isnot only heterogeneity between HCCs, but oftenalso within a given tumor: the growth and progressionof a well-differentiated HCCs usuallyoccurs via the emergence of less differentiated clonal areas within the tumor resulting in a tumoral mosaic of multiple differentiation stages.

Page 22: Preneoplastic  lesions in human hepatocarcinogenesis

Although a numberof general pathways have been discovered the types of genetic alterations and their sequence of occurrence are very variable

Page 23: Preneoplastic  lesions in human hepatocarcinogenesis

at least partly because of the high number of persons infected with HCV in recent decades. At the turn of the millennium, the annual incidence of HCC in the United States has reached 5.9/100 000 inhabitants