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Clinical and pathological progression of non-alcoholic steatohepatitis to hepatocellular carcinoma

Aim:  Non‐alcoholic steatohepatitis (NASH) can progress to hepatocellular carcinoma (HCC). We aimed to examine the clinical and pathological course of how NASH progresses to HCC. Methods:  In this retrospective multicenter study conducted in Japan, we examined 19 patients (53% female), who had been...

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Published in:Hepatology research 2012-08, Vol.42 (8), p.767-773
Main Authors: Yasui, Kohichiroh, Hashimoto, Etsuko, Tokushige, Katsutoshi, Koike, Kazuhiko, Shima, Toshihide, Kanbara, Yoshihiro, Saibara, Toshiji, Uto, Hirofumi, Takami, Shiro, Kawanaka, Miwa, Komorizono, Yasuji, Okanoue, Takeshi
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cited_by cdi_FETCH-LOGICAL-c5266-b440555ee7e4b32f131dc1f0b5092111a4cf1693848391a4615bab473cef7b0a3
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container_title Hepatology research
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creator Yasui, Kohichiroh
Hashimoto, Etsuko
Tokushige, Katsutoshi
Koike, Kazuhiko
Shima, Toshihide
Kanbara, Yoshihiro
Saibara, Toshiji
Uto, Hirofumi
Takami, Shiro
Kawanaka, Miwa
Komorizono, Yasuji
Okanoue, Takeshi
description Aim:  Non‐alcoholic steatohepatitis (NASH) can progress to hepatocellular carcinoma (HCC). We aimed to examine the clinical and pathological course of how NASH progresses to HCC. Methods:  In this retrospective multicenter study conducted in Japan, we examined 19 patients (53% female), who had been previously diagnosed with histologically proven NASH and developed HCC during the follow‐up period. The median age of the patients at the time of initial diagnosis of NASH was 65 years. Results:  NASH progressed to HCC after a median follow‐up period of 3.8 years (range: 0.5–11.6 years). All patients had been identified as having HCC during screening, which included 12 patients assessed by ultrasound, four patients assessed with computerized tomography, two patients that underwent serum des‐γ‐carboxy prothrombin testing and one patient that underwent serum α‐fetoprotein testing. The median diameter of HCC tumors was 1.8 cm (range: 0.8–3.0 cm). The majority of patients (n = 13; 68%) presented with only one HCC tumor. The stage of liver fibrosis was significantly more advanced at the time of diagnosis of HCC than at the time of initial diagnosis of NASH, whereas there were no significant differences in the degree of steatosis. Conclusion:  Screening for HCC with imaging is necessary not only in NASH patients with advanced fibrosis, but also in those with less advanced forms of fibrosis, particularly if they are old men. Liver fibrosis progresses to a more advanced stage during the development of HCC in NASH patients.
doi_str_mv 10.1111/j.1872-034X.2012.00986.x
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We aimed to examine the clinical and pathological course of how NASH progresses to HCC. Methods:  In this retrospective multicenter study conducted in Japan, we examined 19 patients (53% female), who had been previously diagnosed with histologically proven NASH and developed HCC during the follow‐up period. The median age of the patients at the time of initial diagnosis of NASH was 65 years. Results:  NASH progressed to HCC after a median follow‐up period of 3.8 years (range: 0.5–11.6 years). All patients had been identified as having HCC during screening, which included 12 patients assessed by ultrasound, four patients assessed with computerized tomography, two patients that underwent serum des‐γ‐carboxy prothrombin testing and one patient that underwent serum α‐fetoprotein testing. The median diameter of HCC tumors was 1.8 cm (range: 0.8–3.0 cm). The majority of patients (n = 13; 68%) presented with only one HCC tumor. The stage of liver fibrosis was significantly more advanced at the time of diagnosis of HCC than at the time of initial diagnosis of NASH, whereas there were no significant differences in the degree of steatosis. Conclusion:  Screening for HCC with imaging is necessary not only in NASH patients with advanced fibrosis, but also in those with less advanced forms of fibrosis, particularly if they are old men. 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We aimed to examine the clinical and pathological course of how NASH progresses to HCC. Methods:  In this retrospective multicenter study conducted in Japan, we examined 19 patients (53% female), who had been previously diagnosed with histologically proven NASH and developed HCC during the follow‐up period. The median age of the patients at the time of initial diagnosis of NASH was 65 years. Results:  NASH progressed to HCC after a median follow‐up period of 3.8 years (range: 0.5–11.6 years). All patients had been identified as having HCC during screening, which included 12 patients assessed by ultrasound, four patients assessed with computerized tomography, two patients that underwent serum des‐γ‐carboxy prothrombin testing and one patient that underwent serum α‐fetoprotein testing. The median diameter of HCC tumors was 1.8 cm (range: 0.8–3.0 cm). The majority of patients (n = 13; 68%) presented with only one HCC tumor. The stage of liver fibrosis was significantly more advanced at the time of diagnosis of HCC than at the time of initial diagnosis of NASH, whereas there were no significant differences in the degree of steatosis. Conclusion:  Screening for HCC with imaging is necessary not only in NASH patients with advanced fibrosis, but also in those with less advanced forms of fibrosis, particularly if they are old men. 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subjects liver cancer
liver fibrosis
screening
title Clinical and pathological progression of non-alcoholic steatohepatitis to hepatocellular carcinoma
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