Yukitaka Yamashita

Antibody to hepatitis B core antigen and risk for hepatitis C-related hepatocellular carcinoma : A prospective study

Context Retrospective studies suggest that exposure to hepatitis B virus (HBV) may contribute to the development of hepatocellular carcinoma (HCC) in hepatitis C virus (HCV)positive patients with cirrhosis. Contribution These investigators prospectively studied patients with chronic HCV infection and evidence of occult HBV infection (negative results for hepatitis B surface antigen and HBV DNA but positive results for antibody to hepatitis B core antigen [anti-HBc] on serologic testing). Patients with HCV-related cirrhosis and positive results for anti-HBc on serologic testing were at high risk for HCC. Anti-HBc positivity was associated with increased risk for HCC, even in patients with a virologic response to interferon therapy. Caution The effect of alcohol cannot be fully assessed because of the small number of study patients who drank moderately. Implication Anti-HBc serologic testing may be a valuable indicator of special risk for HCC in patients with HCV-related cirrhosis. The Editors Hepatocellular carcinoma (HCC) is one of the most common types of cancer worldwide, and its incidence has been increasing (1, 2). In Japan, an endemic area for hepatitis B virus (HBV) and hepatitis C virus (HCV), it is well known that more than 75% of cases of HCC are attributable to HCV-related chronic liver disease, and nearly 15% are attributable to HBV-related liver disease (3). Several reports have focused on the clinical role of HBV as a unique infection, in which HBV DNA is detectable in the liver despite the absence of serum hepatitis B surface antigen (HBsAg) (46). It is increasingly recognized that after a person is exposed to HBV, infection persists in the liver for a prolonged period (710). This unique persistent infection, known as occult (or latent) HBV infection, is characterized by HBV DNA in the liver but no HBsAg in the serum (1113). In most cases, antibody to hepatitis B core antigen (anti-HBc) is detectable, and thus anti-HBc is believed to be a surrogate marker for latent carriers (14). In fact, we recently showed that HBV infection invariably occurred through grafts from anti-HBcpositive donors in HBV-naive recipients through living-donor liver transplantation (15). In addition to our data, other reports showing frequent HBV transmission from anti-HBcpositive cadaveric donors to recipients indicate that most healthy persons who are positive for anti-HBc, even at low titers, have latent HBV infection in liver tissue (11, 1618). Indeed, we have shown that most anti-HBcpositive healthy persons have a latent episomal form of HBV infection accompanied by ongoing viral replication (19, 20). In contrast, the prevalence of latent HBV infection in anti-HBcpositive patients with HCV-related chronic liver disease, including chronic hepatitis, cirrhosis, and HCC, remains controversial (21). However, several reports have revealed that the HBV genome is frequently detectable in liver tumors in anti-HBcpositive, HBsAg-negative patients with HCV-related liver disease, which suggests that occult HBV infection may contribute to the progression of liver damage and the development of HCC in HCV-positive patients (14, 2227). In a large-scale retrospective study of the prevalence of anti-HBc among 2014 patients with chronic HCV infection, we found that nearly 50% of patients with HCV-related liver disease had anti-HBc (28). Moreover, we found a strong correlation between the prevalence of anti-HBc and the clinical progression of liver disease. The prevalence of anti-HBc was approximately 60% in patients with HCV-related HCC (28). This high prevalence of anti-HBc in HCV-positive patients, particularly those with HCC, strongly suggests that previous exposure to HBV plays an important role in the development of HCC in patients with HCV-related chronic liver disease. Therefore, we performed a prospective study to determine whether previous exposure to HBV affects the clinical course, especially in development of HCC, in patients with chronic HCV infection. Methods Patients Patients with chronic HCV infection who presented to Kyoto University, Kyoto, Japan, and 14 affiliated core hospitals from May 1995 to June 1995 were enrolled. To be eligible, patients had to have serologically confirmed HCV infection without HBsAg and HBV DNA in sera. All patients had been followed with biochemical tests, including -fetoprotein, and ultrasonography or computed tomography (CT) every 3 to 6 months before and after enrollment. We excluded patients who had elevated -fetoprotein levels or those in whom HCC had been diagnosed before enrollment. As a result, 872 patients with chronic HCV infection were enrolled. We discontinued follow-up in patients who moved from the study districts but included their clinical data until they moved. The end of follow-up was defined as the date of diagnosis of HCC, date of death, date of move from the study district, or the closing date of the study (15 May 2005). A total of 384 patients were classified into the hepatitis group or cirrhosis group on the basis of histologic findings on liver biopsy. The differential diagnosis of cirrhosis or hepatitis was made in the remaining 488 patients by using the cirrhosis discriminant score (29, 30). This score is based on 3 laboratory variables: platelet count, alanine aminotransferaseaspartate aminotransferase ratio, and prothrombin time. It has been shown to be highly sensitive in identifying cirrhosis in patients with HCV infection. In accordance with the original definition, patients with a high score (8) were classified into the cirrhosis group. Patients with ascites confirmed by ultrasonography or CT or previous variceal bleeding were given a diagnosis of cirrhosis, regardless of their score, because these findings are strong indicators of portal hypertension and most likely cirrhosis. As a result, 597 (68.5%) patients had a diagnosis of chronic hepatitis and 275 (31.5%) patients had a diagnosis of cirrhosis at the time of enrollment. The patients had regular clinical assessments, biochemical tests, and ultrasonography or CT of the liver every 3 to 6 months during the follow-up period. Patients were stratified into 3 categories according to their smoking habits: nonsmokers, light smokers who smoked fewer than 20 pack-years, and heavy smokers who smoked 20 pack-years or more. Similarly, we stratified patients into 3 categories according to their drinking habits: nondrinkers, moderate drinkers with an average ethanol intake less than 30 g/d, and heavy drinkers with an average ethanol intake greater than 30 g/d. Information on average alcohol intake was based on the patients drinking habits during the 15 years before study entry. All patients provided informed consent to participate in the study, and the study was designed in accordance with the Declaration of Helsinki (31). Serologic Studies At study entry, serum samples from each patient were tested for serologic markers of HCV. Detection of HBsAg, anti-HBc, and antibody to hepatitis B surface antigen (anti-HBs) was performed by using commercial enzyme immunoassay kits (Dainabot, Tokyo, Japan) (28). Results of the anti-HBc assays were expressed as the percentage of inhibition, and the specimen was considered to be anti-HBc positive when the percentage of inhibition was greater than 50% (19). Detection of HBV DNA was done by using DNA probe assay (32). Anti-HCV was assessed by using second-generation assays (Dainabot) (28). Serum HCV RNA levels were determined in 254 patients by using a competitive reverse transcriptionpolymerase chain reaction assay, and positivity of HCV RNA was confirmed in all patients who were examined at study entry (33). History of Interferon Therapy Of the 576 patients with chronic hepatitis, 224 had a history of interferon therapy. One hundred ninety-two patients received 5 to 10 million U of interferon- intramuscularly every day for the first 2 weeks and then 3 times weekly for the following 22 weeks. The remaining 32 patients were treated with 3 to 6 million U of interferon- intravenously every day for 8 weeks. No patient received pegylated interferon or combination therapy with ribavirin. Patients who received interferon were divided into 3 groups based on their virologic response to therapy. Patients with a sustained virologic response were defined as those with no detectable HCV RNA by qualitative assay at least 24 weeks after cessation of therapy. Patients with relapse were defined as those with disappearance of viremia at the end of treatment followed by reappearance of viremia with 24 weeks. Nonresponders included patients whose serum HCV RNA remained positive during therapy. Statistical Analysis The incidence rates for HCC are expressed as the number of HCC cases per 1000 person-years. Incidence rate ratios were calculated by dividing rates, and the exact 95% CIs for the rate ratios were calculated on the basis of a binomial distribution, which is a conditional distribution for 2 independent Poisson distributions. The Cox proportional hazards model was used to calculate the incidence rate ratios for the association between HBc seropositivity and HCC incidence. The multivariate model, with adjustment for potential risk factors, included male sex, age, alcohol intake (none, 0 to 30 g/d, and 30 g/d), smoking (none, 0 to 20 pack-years, and 20 pack-years), and history of interferon therapy (yes or no). The associated 95% Wald CIs were calculated. Analyses were done by using PC-SAS, version 8.2 (SAS Institute, Inc., Cary, North Carolina) and JMP, version 4.0 (SAS Institute, Inc.). Role of the Funding Source The Japan Society for the Promotion of Science provided funding for the study. The funding source had no role in the collection, analysis, or interpretation of the data or in the decision to submit the paper for publication. Results Characteristics of Patients at Enrollment We followed 846 of the 872 enrolled patients. The remaining 26 patients were excluded from the analysis. Twenty-on

Risk of Cancer in Patients With Autoimmune Pancreatitis

OBJECTIVES:Although simultaneous occurrences of autoimmune pancreatitis (AIP) and cancer are occasionally observed, it remains largely unknown whether cancer and AIP occur independently or these disorders are interrelated. The aim of this study was to examine the relationship between AIP and cancer.METHODS:We conducted a multicenter, retrospective cohort study. One hundred and eight patients who met the Asian diagnostic criteria for AIP were included in the study. We calculated the proportion, standardized incidence ratio (SIR), relative risk, and time course of cancer development in patients with AIP. We also analyzed the clinicopathological characteristics of AIP patients with cancer in comparison with those without cancer.RESULTS:Of the 108 AIP patients, 18 cancers were found in 15 patients (13.9%) during the median follow-up period of 3.3 years. The SIR of cancer was 2.7 (95% confidence interval (CI) 1.4–3.9), which was stratified into the first year (6.1 (95% CI 2.3–9.9)) and subsequent years (1.5 (95% CI 0.3–2.8)) after AIP diagnosis. Relative risk of cancer among AIP patients at the time of AIP diagnosis was 4.9 (95% CI 1.7–14.9). In six of eight patients whose cancer lesions could be assessed before corticosteroid therapy for AIP, abundant IgG4-positive plasma cell infiltration was observed in the cancer stroma. These six patients experienced no AIP relapse after successful cancer treatment.CONCLUSIONS:Patients with AIP are at high risk of having various cancers. The highest risk for cancer in the first year after AIP diagnosis and absence of AIP relapse after successful treatment of the coexisting cancers suggest that AIP may develop as a paraneoplastic syndrome in some patients.

Genetic heterogeneity of hepatitis C virus in association with antiviral therapy determined by ultra-deep sequencing.

Background and Aims The hepatitis C virus (HCV) invariably shows wide heterogeneity in infected patients, referred to as a quasispecies population. Massive amounts of genetic information due to the abundance of HCV variants could be an obstacle to evaluate the viral genetic heterogeneity in detail. Methods Using a newly developed massive-parallel ultra-deep sequencing technique, we investigated the viral genetic heterogeneity in 27 chronic hepatitis C patients receiving peg-interferon (IFN) α2b plus ribavirin therapy. Results Ultra-deep sequencing determined a total of more than 10 million nucleotides of the HCV genome, corresponding to a mean of more than 1000 clones in each specimen, and unveiled extremely high genetic heterogeneity in the genotype 1b HCV population. There was no significant difference in the level of viral complexity between immediate virologic responders and non-responders at baseline (p = 0.39). Immediate virologic responders (n = 8) showed a significant reduction in the genetic complexity spanning all the viral genetic regions at the early phase of IFN administration (p = 0.037). In contrast, non-virologic responders (n = 8) showed no significant changes in the level of viral quasispecies (p = 0.12), indicating that very few viral clones are sensitive to IFN treatment. We also demonstrated that clones resistant to direct-acting antivirals for HCV, such as viral protease and polymerase inhibitors, preexist with various abundances in all 27 treatment-naïve patients, suggesting the risk of the development of drug resistance against these agents. Conclusion Use of the ultra-deep sequencing technology revealed massive genetic heterogeneity of HCV, which has important implications regarding the treatment response and outcome of antiviral therapy.

High prevalence of anti-hepatitis B virus serological markers in patients with hepatitis C virus related chronic liver disease in Japan

BACKGROUND/AIMS Evidence is accumulating that hepatitis B virus (HBV) is present in patients who are hepatitis B surface antigen negative but have antibody to hepatitis B core antigen (anti-HBc). Furthermore, recent studies have shown that patients with hepatocellular carcinoma who have antibody to hepatitis C virus (HCV) often possess HBV related serological markers. Data on the seroprevalence of HBV infection in patients with HCV related chronic liver disease were collected to evaluate the significance of the presence of antibodies to HBV. METHODS The prevalence of HBV related serological markers was analysed in a total of 2014 Japanese patients with HCV infection. The control group comprised 352 subjects without liver disorder. RESULTS A large number of patients (49.9%) with HCV related chronic liver disease including hepatocellular carcinoma were positive for anti-HBc. In addition, the prevalence of anti-HBc closely correlated with the clinical stage of the liver disease. There was no relation between a past history of blood transfusion and the prevalence of anti-HBc. Notably, anti-HBc was the only serological marker for HBV infection in a significant number of patients with HCV related chronic liver disease (24.1%). CONCLUSIONS Our data provide further evidence for the high prevalence of anti-HBc in patients with HCV related chronic liver disease, particularly those with hepatocellular carcinoma, suggesting that HBV infection, probably including latent infection, may play an important role in carcinogenesis in these patients.

Covered self-expandable metal stents with an anti-migration system improve patency duration without increased complications compared with uncovered stents for distal biliary obstruction caused by pancreatic carcinoma: a randomized multicenter trial.

OBJECTIVES:The requirements of biliary stents used in the palliation of malignant biliary obstruction are a long duration of patency and minimal adverse effects. Covered self-expandable metal stents (SEMSs) have been shown to prevent tumor ingrowth, which is the most frequent complication of uncovered SEMSs. However, because they are prone to migration, the superiority of covered SEMS has yet to be convincingly demonstrated. The aim of this study was to evaluate the superiority of covered over uncovered SEMSs in the palliation of distal biliary obstruction due to unresectable pancreatic carcinoma, using both stent types with relatively low axial force and uncovered flared ends to prevent their migration.METHODS:From April 2009 to December 2010, 120 patients who were admitted to 22 tertiary-care centers because of distal biliary obstruction from unresectable pancreatic carcinomas were enrolled in this prospective randomized multicenter study. Patients were randomly assigned to receive a covered or uncovered SEMS deployed at the site of the biliary stricture during endoscopic retrograde cholangiopancreatography. Stent patency time, patient survival time, patient survival time without stent dysfunction (time to stent dysfunction or patient death), cause of stent dysfunction (ingrowth, overgrowth, migration, or sludge formation), and serious adverse events were compared between covered and uncovered SEMS groups.RESULTS:Patient survival time in the two groups did not significantly differ (median: 285 and 223 days, respectively; P=0.68). Patient survival time without stent dysfunction was significantly longer in the covered than in the uncovered SEMS group (median: 187 vs. 132 days; P=0.043). Stent patency was also significantly longer in the covered than in the uncovered SEMS group (mean±s.d.: 219.3±159.1 vs. 166.9±124.9 days; P=0.047). Reintervention for stent dysfunction was performed in 14 of 60 patients with covered SEMSs (23%) and in 22 of 60 patients with uncovered SEMSs (37%; P=0.08). Stent dysfunction was caused by tumor ingrowth, tumor overgrowth, and sludge formation in 0 (0%), 3 (5%), and 11 (18%) patients in the covered SEMSs group, and in 15 (25%), 2 (3%), and 6 (10%) patients in the uncovered SEMSs group, respectively. Stent migration was not observed in either group. Rates of tumor overgrowth and sludge formation did not significantly differ between the two groups, whereas the rate of tumor ingrowth was significantly lower in the covered than in the uncovered SEMS group (P<0.01). Acute pancreatitis occurred in only one patient in the covered SEMS group. Acute cholecystitis occurred in one patient in the covered SEMS group and in two patients in the uncovered SEMS group. There was no significant difference between the two groups in the incidence of serious adverse events.CONCLUSIONS:By preventing tumor ingrowth and migration, covered SEMSs with an anti-migration system had a longer duration of patency than uncovered SEMSs, which recommends their use in the palliative treatment of patients with biliary obstruction due to pancreatic carcinomas.

Risk of HCV transmission after needlestick injury, and the efficacy of short-duration interferon administration to prevent HCV transmission to medical personnel

Background. We carried out this study to assess the risk of hepatitis C virus (HCV) transmission after needlestick injuries in medical personnel, and to evaluate the efficacy of short-duration interferon administration to prevent HCV transmission. Methods. A total of 684 personnel who had been occupationally exposed to an anti-HCV-positive source and followed for more than 3 months were retrospectively examined. Results. Of the 684 subjects, 279 (41%) were treated with 1 to 3 days of interferon either just after or 1 to 12 days after the injury. One case of HCV infection was found in each of the treated (1/279; 0.4%) and nontreated (1/405; 0.2%) groups. There was no significant difference in the transmission of HCV between the two groups. Both infected patients were treated with interferon after developing acute hepatitis, and HCV was subsequently cleared. Conclusions. There is a lower risk of HCV transmission after needlestick accident than previously reported, and short-duration interferon administration at an early stage after the needlestick injury, to prevent HCV transmission, is unnecessary.

Photodynamic therapy using pheophorbide-a and Q-switched Nd:YAG laser on implanted human hepatocellular carcinoma.

SummaryTo evaluate whether administration of pheophorbide-a, a new photosensitizer, followed by use of Q-switched Nd:YAG Laser produces a photodynamic reaction, we administered pheophorbide-a to female nude mice (BALB/c-nu) that had been implanted with human hepatocellular carcinoma. Intra-tumoral concentrations of pheophorbide-a were measured by high-performance liquid chromatography. 3 hours after peroral administration of 1 mg/kg body weight, the intra-tumoral concentration was too low to reveal photodynamic effects. Peroral administration of 250 mg/kg body weight, intra-peritoneal administraion of 5 mg/kg body weight, and intra-tumoral injection of 200 μg yielded 0.24 μg/g, 0.83 μg/g and 3.68-108 μg/g tumor concentrations, respectively. All tumors were irradiated interstitially using a Q-switched Nd:YAG Laser at 1064 nm. Only tumors that had been intra-tumorally injected had areas of necrosis larger than those in control tumors. The results suggest that the injection of pheophorbide-a followed by interstitial irradiation using a Q-switched Nd: YAG Laser does not induce sufficient photodynamic reaction if the intratumoral pheophorbide-a concentration is less than 0.83 μglg tumor tissue, and that photodynamic therapy may be useful if the pheophorbide-a tumor concentration is within the range of 0.83-108 μg/g.

Surgically resected needle tract seeding following endoscopic ultrasound-guided fine-needle aspiration in pancreatic cancer.

Needle tract seeding is a rare complication of endoscopic ultrasound-guided fine-needle aspiration (EUS-FNA), with an estimated prevalence of 0.003%–0.009% [1]. We are aware of only six previous case reports in the published literature [2–7]. Herein, we report a case of needle tract seeding on the gastric wall after EUS-FNA of a pancreatic body adenocarcinoma. A 64-year-old woman with elevated serum CA19-9 levels was referred to our hospital. She underwent distal pancreatectomy 8months before. The pathological diagnosis was a T3N0M0 moderately differentiated tubular adenocarcinoma with a 20-mm maximum diameter and clear resection margins. A repeat computed tomography (CT) scan and magnetic resonance imaging showed no evidence of tumor recurrence; however, upper gastrointestinal endoscopy demonstrated a 12-mm submucosal tumor-like mass on the posterior gastric wall (Fig. 1a). Before surgery, she underwent EUS-FNA (three passes) through the posterior gastric wall using a 22gauge needle (EchoTip ProCore, Cook Medical, Limerick, Ireland) with a 10-mL syringe suction. The mass was located near the previous EUS-FNA puncture site where no masses had been detected during the initial preoperative examination. On EUS, this mass was heterogeneous and was mainly present in the third layer of the gastric wall (Fig. 1b). Positron emission tomography also showed abnormal accumulation in the proximal gastric body but with no abnormal uptake at the previous resection margin.

Clinical Significance of the Genotype and Core Promoter/Pre-Core Mutations in Hepatitis B Virus Carriers

It has been shown that clinical and virological characteristics vary among hepatitis B virus (HBV) genotypes. In this study, we measured the virus level, disease severity, and presence or absence of core promoter (CP)/pre-core (PC) mutations in 241 HBV carriers, and investigated the clinical significance of measuring the HBV genotype. In genotype C HBV carriers, the proportion of hepatitis B e antigen (HBeAg)-positive patients was significantly higher than that in genotype B HBV carriers (0 vs. 34.4%, p < 0.05), and the virus level was higher (4.9 vs. 4.05 LGE/ml). In the genotype B HBV carriers, the incidence of PC mutation was significantly higher (69 vs. 34%, p < 0.05). In the genotype C HBV carriers, the incidence of CP mutation was significantly higher (13 vs. 78%, p < 0.05). We compared patients with the wild (W)/mutant (M) pattern in the CP/PC regions to those with the M/W pattern in the CP/PC regions among the genotype C HBV carriers. Both the proportion of HBeAg-positive patients (65.8 vs. 15.4%, p < 0.05) and the alanine aminotransferase (ALT) level (48 vs. 21.5 IU, p < 0.05) were higher in the patients with the M/W pattern in the CP/PC regions, and the disease severity was deteriorated. In conclusion, genotype B HBV may more frequently induce HBe seroconversion via PC mutation compared to genotype C HBV. Among the genotype C HBV carriers, hepatitis activity and the deterioration of the disease severity were significantly inhibited in the group in which PC mutation initially occurred, in comparison to the group in which CP mutation initially occurred.

Multicenter prospective evaluation study of endoscopic ultrasound‐guided hepaticogastrostomy combined with antegrade stenting (with video)

Endoscopic ultrasonography‐guided hepaticogastrostomy (EUS‐HGS) is often indicated for advanced stage patients. Therefore it is important to prevent adverse events associated with EUS‐HGS procedures and obtain long stent patency. EUS‐guided antegrade stenting (AS) has been developed as an advanced technique. Thus, to prevent adverse events and achieve long stent patency, EUS‐AS combined with EUS‐HGS (EUS‐HGAS) has been reported. The aim of the present study was to evaluate the technical feasibility and efficacy of EUS‐HGAS in a multicenter, prospective study.