研究者詳細 - 井本効志

お知らせ

写真a

イモト　コウジ

井本効志

IMOTO KOJI

所属

九州大学病院肝臓・膵臓・胆道内科学術研究員

外部リンク

論文

Clinicopathologic Features of Adult-onset Still's Disease Complicated by Severe Liver Injury.

Miho Kurokawa, Tomonobu Hioki, Tomomi Aoyagi, Motoi Takahashi, Koji Imoto, Takeshi Goya, Masatake Tanaka, Motoyuki Kohjima, Yoshihiro Ogawa

Internal medicine (Tokyo, Japan) 2023年6月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Adult-onset Still's disease (AOSD) is a systemic inflammatory disorder. Severe liver injury has rarely been reported, although liver enzyme elevation is a common complication of AOSD. We herein report four cases of relapsed AOSD with severe liver disorder by tapering or terminating corticosteroids. Liver specimens revealed robust infiltration of inflammatory cells throughout the lobule, especially cluster of differentiation (CD) 8-positive cells. Relapsed AOSD was refractory to corticosteroid reintroduction and required immunosuppressants. Severe liver injury with AOSD is pathologically characterized by extensive lobular infiltration of CD8-positive cells, and we should consider additive immunosuppressive agents on corticosteroids for treatment.

DOI： 10.2169/internalmedicine.2043-23
Transcatheter arterial steroid injection therapy improves the prognosis of patients with acute liver failure. 国際誌

Akifumi Kuwano, Tasuku Okui, Motoyuki Kohjima, Miho Kurokawa, Takeshi Goya, Masatake Tanaka, Tomomi Aoyagi, Motoi Takahashi, Koji Imoto, Shigeki Tashiro, Hideo Suzuki, Nobuhiro Fujita, Yasuhiro Ushijima, Kousei Ishigami, Shoji Tokunaga, Masaki Kato, Yoshihiro Ogawa

Medicine 102 ( 10 ) e33090 2023年3月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Acute liver failure (ALF) is a disorder defined by coagulopathy and encephalopathy with a poor prognosis. No effective therapies have been established except for liver transplantation. We previously reported a subgroup of patients with acute liver injury who developed microcirculatory disturbance. We also established and reported transcatheter arterial steroid injection therapy (TASIT) as a new treatment of ALF. Here, we analyze the effectiveness of TASIT in a larger cohort and evaluate the impact on ALF patients with or without microcirculatory disturbance. We conducted a single-center retrospective study to evaluate the effectiveness of TASIT in patients with ALF admitted at Kyushu University Hospital between January 2005 and March 2018. TASIT is performed by injecting methylprednisolone via the proper hepatic artery for 3 days. One hundred ninety-4 patients with ALF were enrolled and analyzed in this study. Of the 87 patients given TASIT, 71 (81.6%) recovered without any complications and 16 (18.4%) died or underwent liver transplantation. Of the 107 patients not administered TASIT, 77 (72.0%) recovered and 30 (28.0%) progressed to irreversible liver failure. In the high-lactate dehydrogenase subgroup, 52 (86.7%) of the 60 patients with TASIT recovered, and the survival rate was significantly higher than that in patients who did not receive TASIT. Multivariate regression analysis revealed that the TASIT procedure was one of the significant prognostic factors in the high-lactate dehydrogenase subgroup and was significantly associated with prothrombin activity percentage improvement. TASIT is an effective treatment for patients with ALF, especially in those with microcirculatory disturbance.

DOI： 10.1097/MD.0000000000033090
Elevated Pancreatic Enzymes Associated with Acute Liver Injury Were Mediated by Tumor Necrosis Factor-Alpha Signaling

Takeshi Goya, Miho Kurokawa, Tomonobu Hioki, Tomomi Aoyagi, Motoi Takahashi, Koji Imoto, Shigeki Tashiro, Hideo Suzuki, Masatake Tanaka, Masaki Kato, Motoyuki Kohjima, Yoshihiro Ogawa

HEPATITIS MONTHLY 22 ( 1 ) 2022年12月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Background: Acute liver failure (ALF) is caused by massive hepatocyte death and accompanied by severe coagulation disorder and encephalopathy. It often leads to multiple organ failure and subsequently death. However, the association between ALF and other organ failure remains unclear.Objectives: Here, we evaluated patients with acute liver injury (ALI) and elevated pancreatic enzymes to demonstrate the association between ALI and pancreatic disorder.Methods: We conducted a single-center retrospective study to analyze patients with ALI. Between 2012 and 2017, 163 patients with ALI were treated in our hospital. We stratified patients based on whether serum amylase and lipase were elevated above 1.5 times the upper limit of normal. We compared the baseline characteristics, severity, prognosis, and serum cytokine levels between the two groups.Results: Of the 163 patients, 75 (54.0%) presented elevated pancreatic enzymes above 1.5 times the upper limit of normal. Computed tomography imaging findings associated with pancreatitis were observed in 29 patients (17.8%). The elevation of pancreatic enzymes was associated with ALI severity. High level of serum tumor necrosis factor-alpha (TNF-alpha) was associated with the elevation of pancreatic enzymes (elevation group Vs. no elevation group: 134.0 +/- 177.2 pg/mL Vs. 89.4 +/- 159.8 pg/mL).Conclusions: The elevation of pancreatic enzymes was often accompanied by ALI and associated with ALI severity. TNF-alpha signaling was involved in the elevation of pancreatic enzymes. It is possible that the pancreatic disorder reflected ALI severity, consequently correlated with mortality, and did not directly aggravate ALI pathogenesis. These findings provide novel insights into the pathogenesis of ALF.

DOI： 10.5812/hepatmon-128106
Corticosteroid suppresses urea-cycle-related gene expressions in ornithine transcarbamylase deficiency. 査読国際誌

Koji Imoto, Masatake Tanaka, Takeshi Goya, Tomomi Aoyagi, Motoi Takahashi, Miho Kurokawa, Shigeki Tashiro, Masaki Kato, Motoyuki Kohjima, Yoshihiro Ogawa

BMC gastroenterology 22 ( 1 ) 144 - 144 2022年3月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

BACKGROUND: Ornithine transcarbamylase deficiency (OTCD) is most common among urea cycle disorders (UCDs), defined by defects in enzymes associated with ureagenesis. Corticosteroid administration to UCD patients, including OTCD patients, is suggested to be avoided, as it may induce life-threatening hyperammonemia. The mechanism has been considered nitrogen overload due to the catabolic effect of corticosteroids; however, the pathophysiological process is unclear. METHODS: To elucidate the mechanism of hyperammonemia induced by corticosteroid administration in OTCD patients, we analyzed a mouse model by administering corticosteroids to OTCspf-ash mice deficient in the OTC gene. Dexamethasone (DEX; 20 mg/kg) was administered to the OTCspf-ash and wild-type (WT) mice at 0 and 24 h, and the serum ammonia concentrations, the levels of the hepatic metabolites, and the gene expressions related with ammonia metabolism in the livers and muscles were analyzed. RESULTS: The ammonia levels in Otcspf-ash mice that were administered DEX tended to increase at 24 h and increased significantly at 48 h. The metabolomic analysis showed that the levels of citrulline, arginine, and ornithine did not differ significantly between Otcspf-ash mice that were administered DEX and normal saline; however, the level of aspartate was increased drastically in Otcspf-ash mice owing to DEX administration (P < 0.01). Among the enzymes associated with the urea cycle, mRNA expressions of carbamoyl-phosphate synthase 1, ornithine transcarbamylase, arginosuccinate synthase 1, and arginosuccinate lyase in the livers were significantly downregulated by DEX administration in both the Otcspf-ash and WT mice (P < 0.01). Among the enzymes associated with catabolism, mRNA expression of Muscle RING-finger protein-1 in the muscles was significantly upregulated in the muscles of WT mice by DEX administration (P < 0.05). CONCLUSIONS: We elucidated that corticosteroid administration induced hyperammonemia in Otcspf-ash mice by not only muscle catabolism but also suppressing urea-cycle-related gene expressions. Since the urea cycle intermediate amino acids, such as arginine, might not be effective because of the suppressed expression of urea-cycle-related genes by corticosteroid administration, we should consider an early intervention by renal replacement therapy in cases of UCD patients induced by corticosteroids to avoid brain injuries or fatal outcomes.

DOI： 10.1186/s12876-022-02213-0
The Combination of Nucleotide Analog Therapy and Steroid Pulse Therapy for Acute HBV Infection Effectively Promotes HBV Clearance

Takeshi Goya, Tomoyuki Kurashige, Miho Kurokawa, Masatake Tanaka, Tomomi Aoyagi, Motoi Takahashi, Koji Imoto, Shigeki Tashiro, Hideo Suzuki, Masaki Kato, Motoyuki Kohjima, Yoshihiro Ogawa

GASTROENTEROLOGY INSIGHTS 13 ( 1 ) 1 - 8 2022年3月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Acute hepatitis B virus (HBV) infection occasionally progresses to acute liver failure, often with poor prognosis. The appropriate pharmacological approach is yet to be established. Although nucleotide analogs (NA) and corticosteroids are candidates for the treatment of acute HBV infection, their therapeutic effects, especially their effect on HBV clearance, remain unclear. To clarify effects on the HBV clearance of combination therapy of NA and steroid pulse therapy (SPT) for acute HBV infection, we first analyze the effectiveness of this therapy in patients with HBV infection compared with NA monotherapy (NAM). Of the 57 consecutive patients with acute hepatitis B infection from May 2007 to December 2018, we have included 25 patients for this study, whom we followed up until HBV clearance. According to the administration of NA and SPT, we divided patients into two groups (NAM group and NA + SPT group) and compared their results. Of the 25 patients, 10 received NAM, whereas 15 received NA + SPT. There were no appreciable adverse effects related to SPT. The time required for the clearance of HBsAg (76 (43-116) days vs. 26 (14-51) days, p = 0.0418) and HBV-DNA (NAM group vs. NA + SPT group: 180 (83.5-220) vs. 69 (43-136) days, p = 0.0420) was significantly shorter in the NA + SPT group than in the NAM group. The hazard ratio of NA + SPT for the clearance of HBsAg and HBV-DNA were 0.45 (0.19-1.09) and 0.35 (0.14-0.89), respectively. In conclusion, we showed that NA + SPT promoted HBV elimination. These findings support the use of the NA + SPT combination for acute HBV infection without the concern of persistent HBV infection.

DOI： 10.3390/gastroent13010001
The Efficacy of Tofogliflozin on Metabolic Dysfunction-Associated Fatty Liver Disease

Takeshi Goya, Koji Imoto, Shigeki Tashiro, Tomomi Aoyagi, Motoi Takahashi, Miho Kurokawa, Hideo Suzuki, Masatake Tanaka, Masaki Kato, Motoyuki Kohjima, Yoshihiro Ogawa

GASTROENTEROLOGY INSIGHTS 13 ( 1 ) 20 - 26 2022年3月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

The increasing number of patients with fatty liver disease is a major health problem. Fatty liver disease with metabolic dysfunction has been recognized as nonalcoholic fatty liver disease (NAFLD). Although there is no standard therapy for NAFLD, previous reports support the effect of sodium-glucose cotransporter 2 (SGLT2) inhibitors on NAFLD. Recently, fatty liver disease with metabolic dysfunction was proposed to be defined as a novel concept, "metabolic associated fatty liver disease (MAFLD)", and it was proposed that new criteria for MAFLD diagnosis be established. To clarify the effect of SGLT2 inhibitors on MAFLD, we analyzed the efficacy of tofogliflozin in patients with MAFLD. We conducted a single-center, retrospective study to evaluate the efficacy of tofogliflozin in patients with MAFLD treated at Kyushu University Hospital between 2017 and 2019. Tofogliflozin was used to treat 18 patients with MAFLD. To determine the efficacy of tofogliflozin, we evaluated glucose metabolism, insulin resistance, liver injury, hepatic steatosis, and body composition three and six months after drug initiation. Although our study was a preliminary study because of some limitations (e.g., retrospective, observational, single-arm study, small sample size), we show that tofogliflozin could improve liver injury in patients with MAFLD by improving glucose metabolism and insulin resistance without causing muscle loss.

DOI： 10.3390/gastroent13010003
Pirfenidone attenuates acetaminophen-induced liver injury via suppressing c-Jun N-terminal kinase phosphorylation. 国際誌

Shigeki Tashiro, Masatake Tanaka, Takeshi Goya, Tomomi Aoyagi, Miho Kurokawa, Koji Imoto, Akifumi Kuwano, Motoi Takahashi, Hideo Suzuki, Motoyuki Kohjima, Masaki Kato, Yoshihiro Ogawa

Toxicology and applied pharmacology 434 115817 - 115817 2022年1月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Acetaminophen (APAP)-induced liver injury is the most frequent cause of acute liver failure in Western countries. Pirfenidone (PFD), an orally bioavailable pyridone derivative, is clinically used for idiopathic pulmonary fibrosis treatment and has antifibrotic, anti-inflammatory, and antioxidant effects. Here we examined the PFD effect on APAP-induced liver injury. In a murine model, APAP caused serum alanine aminotransferase elevation attenuated by PFD treatment. We performed terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick-end labeling (TUNEL) and vital propidium iodide (PI) stainings simultaneously. APAP induced TUNEL-positive/PI-negative necrosis around the central vein and subsequent TUNEL-negative/PI-positive oncotic necrosis with hemorrhage and caused the upregulation of hypercoagulation- and hypoxia-associated gene expressions. PFD treatment suppressed these findings. Western blotting revealed PFD suppressed APAP-induced c-Jun N-terminal kinase (JNK) phosphorylation despite no effect on JNK phosphatase expressions. In conclusion, simultaneous TUNEL and vital PI staining is useful for discriminating APAP-induced necrosis from typical oncotic necrosis. Our results indicated that PFD attenuated APAP-induced liver injury by suppressing TUNEL-positive necrosis by directly blocking JNK phosphorylation. PFD is promising as a new option to prevent APAP-induced liver injury.

DOI： 10.1016/j.taap.2021.115817
Upregulated expression of hypoxia reactive genes in peripheral blood mononuclear cells from chronic liver disease patients. 国際誌

Akifumi Kuwano, Masatake Tanaka, Hideo Suzuki, Miho Kurokawa, Koji Imoto, Shigeki Tashiro, Takeshi Goya, Motoyuki Kohjima, Masaki Kato, Yoshihiro Ogawa

Biochemistry and biophysics reports 27 101068 - 101068 2021年9月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Liver fibrosis induces intrahepatic microcirculation disorder and hypoxic stress. Hypoxic stress has the potential for an increase in the possibility of more liver fibrosis and carcinogenesis. Liver biopsy is a standard method that evaluates of intrahepatic hypoxia, however, is invasive and has a risk of bleeding as a complication. Here, we investigated the hypoxia reactive gene expressions in peripheral blood mononuclear cells (PBMC) from chronic liver disease patients to evaluate intrahepatic hypoxia in a non-invasive manner. The subjects enrolled for this study were composed of 20 healthy volunteers (HV) and 48 patients with chronic liver disease (CLD). CLD patients contained 24 patients with chronic hepatitis（CH）and 24 patients with liver cirrhosis (LC). PBMC were isolated from heparinized peripheral blood samples. We measured the transcriptional expression of hypoxia reactive genes and inflammatory cytokines by quantitative RT-PCR. mRNA expression of adrenomedullin (AM), vascular endothelial growth factor A (VEGFA) superoxide dismutase (SOD), glutathione peroxidase (GPx) (p < 0.05), Interleukin-6 (IL-6), transforming growth factor-beta (TGF-β) and heme oxygenase-1 (HO-1) in CLD group were significantly higher than HV. AM mRNA expression is correlated with serum lactate dehydrogenase (LDH), serum albumin (Alb), IL6, and SOD mRNA expression. The hypoxia reactive gene expression in PBMCs from CLD patients was more upregulated than HV. Especially, angiogenic genes were notably upregulated and correlated with liver fibrosis. Here, we suggest that mRNA expression of AM in PBMCs could be the biomarker of intrahepatic hypoxia.

DOI： 10.1016/j.bbrep.2021.101068
Microcirculatory disturbance in acute liver injury. 国際誌

Akifumi Kuwano, Miho Kurokawa, Motoyuki Kohjima, Koji Imoto, Shigeki Tashiro, Hideo Suzuki, Masatake Tanaka, Seiji Okada, Masaki Kato, Yoshihiro Ogawa

Experimental and therapeutic medicine 21 ( 6 ) 596 - 596 2021年6月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Microcirculatory disturbance is thought to be involved in the pathogenesis of acute liver injury (ALI). The current study examined the pathophysiologic role of hepatic microcirculatory disturbance in patients with ALI and in mouse models of ALI. Using serum aminotransferase (ALT)/lactate dehydrogenase (LDH) ratio as a hypoxic marker, 279 patients with ALI were classified into the low ALT/LDH ratio (ALT/LDH ≤1.5) and high ALT/LDH ratio group (ALT/LDH >1.5). In the low ALT/LDH ratio group, serum ALT, LDH, fibrinogen degradation products and prothrombin time-international normalized ratio were increased relative to the high ALT/LDH ratio group. Histologically, hepatic expression of tissue factor (TF) and hypoxia-related proteins was enhanced in the low ALT/LDH ratio group, and this was accompanied by sinusoidal fibrin deposition. Sinusoidal hypercoagulation and intrahepatic hypoxia was also analyzed in two different mouse models of ALI; Concanavalin A (ConA) mice and Galactosamine/tumor necrosis factor (TNF)-α (G/T) mice. Serum ALT/LDH ratio in ConA mice was significantly lower compared with G/T mice. Pimonidazole staining revealed the upregulation of hypoxia-related proteins in ConA mice. Recombinant human soluble thrombomodulin improved liver damage in ConA mice in association with reduced sinusoidal hypercoagulation and intrahepatic hypoxia. The present study provides evidence that serum ALT/LDH ratio aids in the identification of patients with ALI and intrahepatic hypoxia as a result of microcirculatory disturbance. The results facilitate the improved understanding of the pathogenesis of ALI, thereby offering a novel therapeutic strategy against ALI, which arises from sinusoidal hypercoagulation.

DOI： 10.3892/etm.2021.10028
Hypoxic hepatitis with marked elevation of serum ferritin probably due to activation of intrahepatic macrophages: Another form of hypoxic hepatitis hitherto not reported?

M. Tanaka, T. Goya, H. Suzuki, M. Takahashi, K. Imoto, M. Kurokawa, S. Tashiro, A. Kuwano, S. Okada, M. Kato, Motoyuki Kohjima, K. Kotoh, Y. Ogawa

Acta Gastro-Enterologica Belgica 84 ( 2 ) 317 - 320 2021年4月

　詳細を見る

記述言語：その他掲載種別：研究論文（学術雑誌）

Background and study aims: Hypoxic hepatitis (HH) is an acute liver injury that develops in patients with underlying diseases, such as heart failure, respiratory failure, septic/toxic shock. However, some patients do not have underlying diseases or episodes which are known to result in HH. Here, we analyzed the clinical characteristics of this particular patient group (called ‘unknown HH’ hereafter) to understand its pathogenesis. Patients and methods: Between October 2010 and January 2016, 157 consecutive patients with acute liver injury were admitted to our hospital. Among these patients, 15 patients were categorized as unknown HH. Medical histories and blood test results of unknown HH were analyzed. Results: Among 15 patients of unknown HH, 11 were habitual drinkers and all experienced one of digestive symptoms which might result in mild hypovolemia such as vomiting, diarrhea, appetite loss, and epigastralgia. All patients of unknown HH presented marked elevation of serum ferritin concentration paralleled with aspartate transaminase (AST), alanine transaminase (ALT), and lactate dehydrogenase (LDH) concentrations. The serum levels of ferritin, ALT, LDH, and prothrombin time-international normalized ratio (PT-INR) were rapidly decreased during hospitalization and all 15 patients of unknown HH recovered without any complication. Conclusions: We found the particular group of HH with marked elevation of serum ferritin probably due to intrahepatic macrophage activation. Anti-inflammatory treatments might be effective for this group of hypoxic hepatitis.

DOI： 10.51821/84.2.317
Recombinant human soluble thrombomodulin ameliorates acetaminophen-induced liver toxicity in mice. 国際誌

Akifumi Kuwano, Motoyuki Kohjima, Hideo Suzuki, Akihiro Yamasaki, Tomoko Ohashi, Koji Imoto, Miho Kurokawa, Yusuke Morita, Masaki Kato, Yoshihiro Ogawa

Experimental and therapeutic medicine 18 ( 2 ) 1323 - 1330 2019年8月

　詳細を見る

記述言語：英語掲載種別：研究論文（学術雑誌）

Recombinant human soluble thrombomodulin alpha (rhTM) has been developed as an anticoagulant with anti-inflammatory activity. Notably, acetaminophen (APAP) -induced liver disease (AILI) is caused by direct metabolite-induced hepatotoxicity as well as hepatic hyper-coagulation. To evaluate the utility of anticoagulant for the treatment of AILI, rhTM was administered in a mouse AILI model and liver damage was analyzed. AILI was induced in 8-week-old mice by intraperitoneal injection of APAP. rhTM (20 mg/kg) or placebo was injected at the same time as APAP administration. Serum alanine aminotransferase, fibrin degradation products and high-mobility group box 1 levels were significantly decreased in the rhTM-treated group compared with the control group. Furthermore, rhTM reduced the necrotic area and fibrin deposition in liver sections. rhTM suppressed the mRNA expression of heme oxygenase-1, plasminogen activator inhibitor type-1, tissue factors, and inflammatory cytokines compared with the control group. rhTM did not change the hepatic GSH content at 2 h after APAP injection, but restored them at 4 h after the insult. rhTM ameliorated liver damage in mice with AILI, probably via the improvement in liver perfusion induced by it's anticoagulant acitivity, which can lead to the suppression of secondary liver damage.

DOI： 10.3892/etm.2019.7665
Successful endoscopic treatment of hepatoduodenal fistula formed during sorafenib treatment for hepatocellular carcinoma with duodenal invasion 査読

Koji Imoto, Motoyuki Kohjima, Tomoyuki Kurashige, Taiji Mutsuki, Shigeki Tashiro, Hideo Suzuki, Akifumi Kuwano, Masaki Kato, Yoshihiro Ogawa

Acta Hepatologica Japonica 60 ( 3 ) 91 - 98 2019年3月

　詳細を見る

記述言語：その他掲載種別：研究論文（学術雑誌）

DOI： 10.2957/kanzo.60.91

▼全件表示

MISC

肝非実質細胞を介した閉経後NASHの発症増悪メカニズムの解析

合谷孟, 青柳知美, 鈴木秀生, 東夕喜, 日置智惟, 高橋基, 井本効志, 黒川美穂, 田代茂樹, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2023年4月

　詳細を見る

記述言語：日本語
NASHモデルマウスにおける肝線維化機序の解明

井本効志, 東夕喜, 大野あかり, 青柳知美, 高橋基, 黒川美穂, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2023年4月

　詳細を見る

記述言語：日本語
リンパうっ滞がフォンタン関連肝疾患の肝線維化に及ぼす影響についての基礎的検討

田中正剛, 東夕喜, 日置智惟, 青柳知美, 高橋基, 井本効志, 黒川美穂, 合谷孟, 国府島庸之, 小川佳宏

肝臓 2023年4月

　詳細を見る

記述言語：日本語
組織学的な診断の得られた,免疫チェックポイント阻害剤による肝障害の臨床的特徴

日置智惟, 東夕喜, 大野あかり, 青柳知美, 高橋基, 黒川美穂, 井本効志, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2023年4月

　詳細を見る

記述言語：日本語
鉄中毒による急性肝不全に対し集学的治療を行い救命した一例

黒川美穂, 倉重智之, 日置智惟, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 加藤正樹

肝臓 2023年3月

　詳細を見る

記述言語：日本語
高度肝障害を伴った急性発症still病4例の検討

黒川美穂, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2023年2月

　詳細を見る

記述言語：日本語
急性肝不全に対する治療内科,外科の立場から急性肝障害の病型分類とステロイド動注療法の治療効果

国府島庸之, 倉重智之, 正月泰士, 黒川美穂, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 加藤正樹, 小川佳宏

肝臓 2023年2月

　詳細を見る

記述言語：日本語
経皮的肝生検によるフォンタン関連肝疾患の肝線維化評価:非侵襲的線維化予測に向けて

田中正剛, 東夕喜, 日置智惟, 青柳知美, 高橋基, 井本効志, 黒川美穂, 合谷孟, 西崎晶子, 柿野貴盛, 永田弾, 山村健一郎, 坂本一郎, 国府島庸之, 筒井裕之, 小川佳宏

日本成人先天性心疾患学会雑誌 2023年1月

　詳細を見る

記述言語：日本語
肝障害を契機に診断した肝類洞閉塞症候群の2例

田中亮太郎, 井本効志, 黒川美穂, 東夕喜, 日置智惟, 青柳知美, 高橋基, 田代茂樹, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

日本消化器病学会九州支部例会・日本消化器内視鏡学会九州支部例会プログラム・抄録集 2022年12月

　詳細を見る

記述言語：日本語
肝非実質細胞に注目した閉経後NASHの発症・増悪メカニズムの解析

青柳知美, 鈴木秀生, 高橋基, 井本効志, 東夕喜, 大野あかり, 黒川美穂, 田代茂樹, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
APAP肝障害マウスモデルにおけるPirfenidoneによる肝障害抑制効果の検討

田代茂樹, 東夕喜, 大野あかり, 青柳知美, 高橋基, 黒川美穂, 井本効志, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
NASH関連肝癌モデルマウスを用いた抗PD-1抗体の肝癌に対する効果についての検討

高橋基, 国府島庸之, 東夕喜, 大野あかり, 青柳知美, 井本効志, 黒川美穂, 田代茂樹, 合谷孟, 田中正剛, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
OTC欠損モデルマウスにおけるアンモニア代謝動態の検討

井本効志, 東夕喜, 大野あかり, 青柳知美, 高橋基, 黒川美穂, 田代茂樹, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
急性肝不全モデルマウスにおけるExtracellular trapsの関与についての検討

高橋基, 田中正剛, 東夕喜, 大野あかり, 青柳知美, 井本効志, 黒川美穂, 田代茂樹, 合谷孟, 国府島庸之, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
急性肝障害時の類洞血流障害発症におけるIFNγの関与

黒川美穂, 高橋基, 井本効志, 田代茂樹, 青柳知美, 大野あかり, 東夕喜, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2022年4月

　詳細を見る

記述言語：日本語
好酸球増多症による肝障害を発症した一例

伊地知嵩治, 日置智惟, 川元美緒, 高橋基, 井本効志, 黒川美穂, 田代茂樹, 鈴木秀生, 合谷孟, 田中正剛, 国府島庸之, 小川佳宏

日本消化器病学会九州支部例会・日本消化器内視鏡学会九州支部例会プログラム・抄録集 2021年6月

　詳細を見る

記述言語：日本語
非アルコール性脂肪性肝疾患の組織学的特徴に関連した臨床病態及び遺伝子発現変化の検討

井本効志, 田代茂樹, 日置智惟, 川元美緒, 高橋基, 黒川美穂, 鈴木秀生, 合谷孟, 田中正剛, 加藤正樹, 国府島庸之, 小川佳宏

肝臓 2021年4月

　詳細を見る

記述言語：日本語
IFNγは急性肝障害の類洞血流障害に関与する

黒川美穂, 桑野哲史, 日置智惟, 川元美緒, 高橋基, 井本効志, 田代茂樹, 鈴木秀生, 合谷孟, 田中正剛, 加藤正樹, 国府島庸之, 小川佳宏

肝臓 2021年4月

　詳細を見る

記述言語：日本語
肝生検で診断した免疫チェックポイント阻害剤による肝障害の臨床的特徴

日置智惟, 川元美緒, 高橋基, 井本効志, 黒川美穂, 鈴木秀生, 田代茂樹, 合谷孟, 田中正剛, 加藤正樹, 国府島庸之, 小川佳宏

肝臓 2021年4月

　詳細を見る

記述言語：日本語
肝細胞癌における糖・脂質代謝関連遺伝子発現の変化高分化型肝細胞癌における脂肪蓄積のメカニズム

鈴木秀生, 高橋基, 井本効志, 黒川美穂, 田代茂樹, 合谷孟, 田中正剛, 加藤正樹, 伊藤心二, 吉住朋晴, 森正樹, 中牟田誠, 国府島庸之, 小川佳宏

肝臓 2021年4月

　詳細を見る

記述言語：日本語
肝細胞癌患者におけるlenvatinib血中濃度と奏功率および有害事象の関連

高橋基, 日置智惟, 川元美緒, 井本効志, 黒川美穂, 田代茂樹, 鈴木秀生, 秦晃二郎, 合谷孟, 田中正剛, 加藤正樹, 国府島庸之, 小川佳宏

肝臓 2021年4月

　詳細を見る

記述言語：日本語
急性肝障害に伴う膵酵素上昇

黒川美穂, 森田祐輔, 井本効志, 鈴木秀生, 田代茂樹, 桑野哲史, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2021年2月

　詳細を見る

記述言語：日本語
MC4R欠損マウスを用いた閉経後女性におけるNASH発症メカニズムの解析

鈴木秀生, 豊田優貴, 大角真央, 日置智惟, 倉重智之, 井本効志, 黒川美穂, 田代茂樹, 桑野哲史, 田中正剛, 國府島庸之, 加藤正樹, 小川佳宏

日本消化器病学会雑誌 2020年7月

　詳細を見る

記述言語：日本語
APAP肝障害マウスモデルにおけるPirfenidoneによる肝障害抑制効果の検討

田代茂樹, 豊田優貴, 大角真央, 日置智惟, 倉重智之, 井本効志, 黒川美穂, 鈴木秀生, 桑野哲史, 田中正剛, 國府島庸之, 加藤正樹, 小川佳宏

日本消化器病学会雑誌 2020年7月

　詳細を見る

記述言語：日本語
膵機能低下に伴う肝脂肪化症例の臨床的特徴と遺伝子発現変化

田中正剛, 国府島庸之, 黒川美穂, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 豊田優貴, 日置智惟, 倉重智之, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
MC4R欠損マウスを用いた閉経後女性におけるNASH発症メカニズムの解析

鈴木秀生, 黒川美穂, 井本効志, 田代茂樹, 合谷孟, 桑野哲史, 田中正剛, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
NAFLDにおける組織学的肝内微小構造形成に関わる臨床的特徴と遺伝子発現変化

田中正剛, 国府島庸之, 黒川美穂, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 豊田優貴, 日置智惟, 倉重智之, 加藤正樹, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
免疫チェックポイント阻害剤による肝障害の臨床的特徴

日置智惟, 豊田優貴, 倉重智之, 井本効志, 黒川美穂, 鈴木秀生, 田代茂樹, 桑野哲史, 田中正剛, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
好中球リンパ球比を用いた非アルコール性脂肪性肝疾患(NAFLD)患者における発癌高リスク群の囲い込み

井本効志, 国府島庸之, 日置智惟, 倉重智之, 黒川美穂, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 加藤正樹, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
急性肝障害における超音波造影剤による血行動態評価の有用性

倉重智之, 豊田優貴, 日置智惟, 井本効志, 黒川美穂, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2020年4月

　詳細を見る

記述言語：日本語
肝細胞癌との鑑別が困難であったFallot四徴症修復術後に発症した肝原発悪性リンパ腫の一例

垰田あかり, 井本効志, 倉重智之, 正月泰士, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 加藤正樹, 小川佳宏

日本消化器病学会九州支部例会・日本消化器内視鏡学会九州支部例会プログラム・抄録集 2019年5月

　詳細を見る

記述言語：日本語
閉経後女性における脂肪肝発症メカニズムの解析とその臨床的特徴の検討

鈴木秀生, 国府島庸之, 倉重智之, 正月泰士, 井本効志, 田代茂樹, 桑野哲史, 田中正剛, 加藤正樹, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
APAP肝障害マウスモデルにおけるPirfenidoneによる肝障害抑制効果の検討

田代茂樹, 加藤正樹, 倉重智之, 正月泰士, 井本効志, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
NAFLDにおけるSteatosis、Inflammation、Ballooning、Mallory-Denk body、Fibrosisの各因子と関連する臨床的特徴と遺伝子発現変化

国府島庸之, 倉重智之, 正月泰士, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 加藤正樹, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
分子標的薬と免疫チェックポイント阻害薬による肝障害(症例報告も可) 当院における免疫チェックポイント阻害剤での肝障害の臨床的特徴

井本効志, 国府島庸之, 加藤正樹

肝臓 2019年4月

　詳細を見る

記述言語：日本語
当院におけるFib-4 index上昇患者の臨床的特徴についての検討

倉重智之, 加藤正樹, 正月泰士, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
急性肝障害における類洞内皮細胞障害と類洞内過凝固の関与の検討

正月泰士, 加藤正樹, 倉重智之, 井本効志, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 国府島庸之, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
急性肝障害に合併する腎障害の臨床的特徴

井本効志, 倉重智之, 正月泰士, 田代茂樹, 鈴木秀生, 桑野哲史, 田中正剛, 加藤正樹, 国府島庸之, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
急性肝障害に対する肝類洞血流障害に注目した治療戦略

桑野哲史, 国府島庸之, 倉重智之, 正月泰士, 井本効志, 田代茂樹, 鈴木秀生, 田中正剛, 加藤正樹, 小川佳宏

肝臓 2019年4月

　詳細を見る

記述言語：日本語
肝細胞癌十二指腸浸潤に対するソラフェニブ治療後に生じた肝十二指腸瘻を内視鏡的に閉鎖しえた一例

井本効志, 国府島庸之, 倉重智之, 正月泰士, 田代茂樹, 鈴木秀生, 桑野哲史, 加藤正樹, 小川佳宏

肝臓 2019年3月

　詳細を見る

記述言語：日本語

症例は79歳女性。肝細胞癌術後およびC型肝硬変SVR後で当院通院中であった。2017年10月黒色便を主訴に受診し、精査の結果肝細胞癌の再発とその十二指腸浸潤部からの腫瘍出血と診断された。浸潤部からの出血は自然止血した。動脈塞栓術や外科的治療の適応は乏しいと判断され、ソラフェニブ400mg/dayを開始した。2018年1月に腹部CTおよび上部消化管内視鏡検査では、再発癌部は縮小し十二指腸浸潤部には肝十二指腸瘻が出現していた。瘻孔閉鎖のためポリグリコール酸シートとフィブリン糊による内視鏡的瘻孔閉鎖処置を行い、さらに瘻孔周囲をアルゴンプラズマ凝固にて焼灼した。瘻孔は縮小傾向を示しソラフェニブ治療を継続したところ、同年5月には瘻孔は閉鎖した。十二指腸浸潤を伴う肝細胞癌の縮小とともに生じた肝十二指腸瘻を、内視鏡的に閉鎖しえた症例を経験したので報告する。(著者抄録)
当院での免疫チェックポイント阻害剤による肝障害の臨床的特徴

井本効志, 国府島庸之, 加藤正樹

日本消化器病学会雑誌 2018年10月

　詳細を見る

記述言語：日本語
肥満合併症としての肝疾患-NASHと肝細胞癌をどう捉えるか- NASH病態進展・肝細胞癌発症における代謝異常

国府島庸之, 鈴木秀生, 黒川美穂, 井本効志, 倉重智之, 正月泰士, 田代茂樹, 桑野哲史, 大橋朋子, 加藤正樹, 小川佳宏

肥満研究 2018年9月

　詳細を見る

記述言語：日本語
当院での免疫チェックポイント阻害剤による肝障害の臨床的特徴

井本効志, 国府島庸之, 加藤正樹

肝臓 2018年9月

　詳細を見る

記述言語：日本語
腹部超音波を用いた急性肝障害症例における門脈血流と肝硬度の経時的変化の検討

森田祐輔, 井本効志, 黒川美穂, 鈴木秀生, 桑野哲史, 国府島庸之, 山崎晃裕, 大橋朋子, 加藤正樹, 小川佳宏

肝臓 2018年4月

　詳細を見る

記述言語：日本語
NAFLD患者における肥満と体組成の関与

黒川美穂, 森田祐輔, 井本効志, 鈴木秀生, 桑野哲史, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2018年4月

　詳細を見る

記述言語：日本語
急性発症型自己免疫性肝炎の臨床的特徴の検討

井本効志, 国府島庸之, 加藤正樹

肝臓 2018年4月

　詳細を見る

記述言語：日本語
急性肝障害における類洞血流障害の関与

桑野哲史, 井本効志, 黒川美穂, 森田祐輔, 鈴木秀生, 國府島庸之, 加藤正樹, 小川佳宏

肝臓 2018年4月

　詳細を見る

記述言語：日本語
高度肝障害を伴った急性発症still病4例の検討

黒川美穂, 井本効志, 森田祐輔, 鈴木秀生, 桑野哲史, 国府島庸之, 加藤正樹, 小川佳宏

肝臓 2017年11月

　詳細を見る

記述言語：日本語
急性発症型自己免疫性肝炎の臨床的特徴

井本効志, 黒川美穂, 森田祐輔, 鈴木秀生, 桑野哲史, 國府島庸之, 加藤正樹, 小川佳宏

肝臓 2017年11月

　詳細を見る

記述言語：日本語
内臓脂肪蓄積と異所性脂肪/臓器連関 NAFLD病態進展における体組成・体脂肪分布の関与

国府島庸之, 黒川美穂, 井上千絵子, 森田祐輔, 井本効志, 鈴木秀生, 桑野哲史, 山崎晃裕, 大橋朋子, 牧俊允, 木村真一郎, 前田泰孝, 園田紀之, 加藤正樹, 小川佳宏

肥満研究 2017年9月

　詳細を見る

記述言語：日本語
B型肝細胞癌術後経過中に認められた異時性肝内胆管癌の1例

井本効志, 高見裕子, 立石昌樹, 龍知記, 和田幸之, 才津秀樹

肝臓 2011年11月

　詳細を見る

記述言語：日本語

▼全件表示

所属学協会

日本内科学会
日本消化器病学会
日本肝臓学会

共同研究・競争的資金等の研究課題

フォンタン関連肝疾患における肝線維化の病態解明

研究課題/領域番号：23K19591 2023年 - 2024年

日本学術振興会科学研究費助成事業研究活動スタート支援

　詳細を見る

担当区分：研究代表者資金種別：科研費