1. Visceral fat accumulation is an independent risk factor for hepatocellular carcinoma recurrence after curative treatment in patients with suspected NASH T Ohki, R Tateishi, S Shiina, E Goto, T Sato, H Nakagawa, R Masuzaki, T Goto, K Hamamura, F Kanai, H Yoshida, T Kawabe, M Omata Gut 2009;58;839-844 R3 임 준 욱

2. Introduction Hepatocellular carcinoma (HCC) : 1. fifth leading cause of cancer death worldwide 2. >500,000 deaths annually 3. increasing incidence Non-alcoholic steatohepatitis (NASH) – considered to be another important liver disease preceding cirrhosis and HCC Non-alcoholic fatty liver disease (NAFLD)  may progress to NASH  subsequently, HCC

3. Introduction The severity of fatty liver - positively related to visceral fat accumulation and insulin resistance in both obese and non-obese NAFLD patients without viral hepatitis  suggests that hepatic fat infiltration in NAFLD may be influenced by visceral fat accumulation independently of body mass index (BMI) Hypothesis : visceral fat accumulation  directly associated with HCC development

4. Introduction Evaluate the impact of visceral fat accumulation on HCC recurrence in nonviral non-alcoholic patients with naıve HCC who received curative radiofrequency ablation (RFA) treatment

5. Methods Patients :1. between January 1999 and December 2006 2. 62 patients as a cohort and analysed the relationship between visceral fat accumulation and intrahepatic recurrence of HCC Diagnosis of HCC : 1. CT— hyperattenuation in the arterial phase and hypoattenuation in the equilibrium phase 2. Background tissue was pathologically graded based on NAFLD activity score and Ishak fibrosis Staging

6. Methods Measurement of visceral fat - CT image at the level of the umbilicus - defined as the sum of the intraperitoneal fat area (-150 to 250 Housefield units) - high VFA group (defined as VFA >130 cm2 in males and VFA >90 cm2 in females, n=27) and the controls (n=35) (Oka R, Kobayashi J, Yagi K, et al. Reassessment of the cutoff values of waist circumference and visceral fat area for identifying Japanese subjects at risk for the metabolic syndrome. Diabetes Res Clin Pract 2008;79:474– 81)

7. Methods Treatment and follow-up - monthly blood tests and monitoring of tumour markers (alpha- fetoprotein (AFP), lens culinaris agglutinin-reactive fraction of AFP (AFP-L3), and desgamma-carboxy prothrombin (DCP)) at the outpatient clinic - ultrasonography and dynamic CT scan performed every 4 months Analysis of recurrence 1. the end point - the interval between the first ablation and the detection of HCC recurrence 2. compared the number and size of tumours at the time of recurrence between the high VFA group and the controls 3. changes in VFA between the time of first diagnosis of HCC and at recurrence

8. Methods Analysis of survival Survival time - defined as the interval between the first treatment and death or the last visit to the outpatient clinic up to 31 December 2007

9. Results

13. High VFA group: 15/27(55.6%) Control group: 11/35(31.4%)

16. Conclusion Visceral fat accumulation  independent risk factor of recurrence in patients with non-B non-C non-alcoholic HCC treated with curative ablation Visceral fat  decreases HCC recurrence ?

17. NAFLD activity score (NAS) Based on three pathologic features: steatosis, lobular inflammation, and ballooning degeneration Scores range from 0–8 1. score of 5 or more is equivalent to NASH 2. score of 3 or 4 is borderline NASH 3. score of 2 or below equates to non-NASH NAFLD

18. Ishak score