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Dive into the research topics where Kentaro Moriichi is active.

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Featured researches published by Kentaro Moriichi.


Inflammatory Bowel Diseases | 2011

Heat-killed body of lactobacillus brevis SBC8803 ameliorates intestinal injury in a murine model of colitis by enhancing the intestinal barrier function

Nobuhiro Ueno; Mikihiro Fujiya; Shuichi Segawa; Toshie Nata; Kentaro Moriichi; Hiroki Tanabe; Yusuke Mizukami; Naoyuki Kobayashi; Kazutoshi Ito; Yutaka Kohgo

Background: Probiotics have been clinically administered to improve intestinal damage in some intestinal inflammations. However, probiotic treatments are not always effective for these intestinal disorders because live bacteria must colonize and maintain their activity under unfavorable conditions in the intestinal lumen when displaying their functions. This study investigated the physiological functions of a heat‐killed body of a novel probiotic, Lactobacillus brevis SBC8803, on the protection of intestinal tissues, the regulation of cytokine production, the improvement of intestinal injury, and the survival rate of mice with dextran sodium sulfate (DSS)‐induced colitis. Methods: Heat shock protein (Hsp) induction and mitogen‐activated protein kinase (MAPK) phosphorylation in intestinal epithelia by heat‐killed L. brevis SBC8803 were examined by Western blotting. The barrier function of intestinal epithelia was measured with [3H]‐mannitol flux in the small intestine under oxidant stress. The effects of the bacteria on improving epithelial injury and cumulative survival rate were investigated with a DSS colitis model. Results: Heat‐killed L. brevis SBC8803 induced Hsps, phosphorylated p38 MAPK, regulated the expression of tumor necrosis factor alpha (TNF‐&agr;), interleukin (IL)‐1&bgr; and IL‐12, and improved the barrier function of intestinal epithelia under oxidant stress. The induction of Hsp and the protective effect were negated by p38 MAPK inhibitor. These functions relieve intestinal impairments and improve the survival rate in mice with lethal colitis. Conclusions: The administration of heat‐killed L. brevis SBC8803 helps to successfully maintain intestinal homeostasis, while also curing intestinal inflammation. A therapeutic strategy using heat‐killed bacteria is expected to be beneficial for human health even in conditions unsuitable for live probiotics because the heat‐killed body is able to exhibit its effects without the requirement of colonization. (Inflamm Bowel Dis 2011;)


Endoscopy | 2011

The diagnostic accuracy of high-resolution endoscopy, autofluorescence imaging and narrow-band imaging for differentially diagnosing colon adenoma.

Ryu Sato; Mikihiro Fujiya; Jiro Watari; Nobuhiro Ueno; Kentaro Moriichi; Shin Kashima; Shigeaki Maeda; Katuyoshi Ando; H. Kawabata; Ryuji Sugiyama; Yoshiki Nomura; Toshie Nata; Kentaro Itabashi; Yuhiei Inaba; Kotaro Okamoto; Yusuke Mizukami; Yusuke Saitoh; Yutaka Kohgo

BACKGROUND AND STUDY AIMS Conventional colonoscopy can result in unnecessary biopsy or endoscopic resection due to its inability to distinguish adenomas from hyperplastic polyps. This study therefore evaluated the efficacy of high-resolution endoscopy (HRE), autofluorescence imaging (AFI), and narrow-band imaging (NBI) in discriminating colon adenoma from hyperplastic polyps. PATIENTS AND METHODS This was a prospective multicenter study in patients undergoing AFI and NBI examinations. HRE, AFI, and NBI images were classified into two groups based on morphological characteristics, the predominant color intensities, and the visibility of meshed capillary vessels, respectively. Each of the endoscopic photographs were independently evaluated by a single endoscopist. The images were then assessed by three specialists and three residents, the latter having performed < 500 colonoscopies and < 30 NBI and AFI examinations. Diagnostic test statistics were calculated to compare the accuracy in differentiating colon adenoma from hyperplastic polyps for each method. RESULTS A total of 183 patients were enrolled in the study and 339 adenomas and 85 hyperplastic polyps were identified. AFI and NBI could distinguish adenoma from hyperplastic polyps with an accuracy of 84.9 % and 88.4 %, respectively, whereas HRE exhibited an accuracy of 75.9 %. In the 358 lesions in which the AFI diagnosis was consistent with that of NBI, the accuracy, sensitivity, and specificity were high, at 91.9 %, 92.7 %, and 92.9 %, respectively. During the study comparing specialists and residents, AFI and NBI dramatically improved the diagnostic accuracy of residents from 69.1 % to 86.1 % and 84.7 %, respectively. CONCLUSIONS Both AFI and NBI are considered to be feasible tools that can discriminate colon adenoma from hyperplastic polyps, and their use may be particularly beneficial for less-experienced endoscopists.


Journal of Gene Medicine | 2013

MicroRNA‐146b improves intestinal injury in mouse colitis by activating nuclear factor‐κB and improving epithelial barrier function

Toshie Nata; Mikihiro Fujiya; Nobohiro Ueno; Kentaro Moriichi; Hiroaki Konishi; Hiroki Tanabe; Takaaki Ohtake; Katsuya Ikuta; Yutaka Kohgo

The precise role of microRNAs in inflammatory disease is not clear. The present study investigated the effect of microRNA (miR‐146b) with respect to improving intestinal inflammation.


Oncogene | 2014

microRNA-18a induces apoptosis in colon cancer cells via the autophagolysosomal degradation of oncogenic heterogeneous nuclear ribonucleoprotein A1.

Mikihiro Fujiya; Hiroaki Konishi; Mohamed Kamel Mk; Nobuhiro Ueno; Yuhei Inaba; Kentaro Moriichi; Hiroki Tanabe; Katsuya Ikuta; Takaaki Ohtake; Yutaka Kohgo

It is well known that microRNAs (miRs) are abnormally expressed in various cancers and target the messenger RNAs (mRNAs) of cancer-associated genes. While (miRs) are abnormally expressed in various cancers, whether miRs directly target oncogenic proteins is unknown. The present study investigated the inhibitory effects of miR-18a on colon cancer progression, which was considered to be mediated through its direct binding and degradation of heterogeneous nuclear ribonucleoprotein A1 (hnRNP A1). An MTT assay and xenograft model demonstrated that the transfection of miR-18a induced apoptosis in SW620 cells. A binding assay revealed direct binding between miR-18a and hnRNP A1 in the cytoplasm of SW620 cells, which inhibited the oncogenic functions of hnRNP A1. A competitor RNA, which included the complementary sequence of the region of the miR-18a-hnRNP A1 binding site, repressed the effects of miR-18a on the induction of cancer cell apoptosis. In vitro single and in vivo double isotope assays demonstrated that miR-18a induced the degradation of hnRNP A1. An immunocytochemical study of hnRNP A1 and LC3-II and the inhibition of autophagy by 3-methyladenine and ATG7, p62 and BAG3 siRNA showed that miR-18a and hnRNP A1 formed a complex that was degraded through the autophagolysosomal pathway. This is the first report showing a novel function of a miR in the autophagolysosomal degradation of an oncogenic protein resulting from the creation of a complex consisting of the miR and a RNA-binding protein, which suppressed cancer progression.


American Journal of Clinical Pathology | 2008

Clinicopathologic Implications of Genetic Instability in Intestinal-Type Gastric Cancer and Intestinal Metaplasia as a Precancerous Lesion Proof of Field Cancerization in the Stomach

Amen Hamdy Zaky; Jiro Watari; Hiroki Tanabe; Ryu Sato; Kentaro Moriichi; Atsumi Tanaka; Atsuo Maemoto; Mikihiro Fujiya; Toshifumi Ashida; Yutaka Kohgo

To clarify field cancerization in the stomach by genetic alterations, we studied 83 cases of intestinal-type gastric cancer (GC) and paired intestinal metaplasia (IM) distant from GC and 39 cases of chronic gastritis with IM (CG-IM) for genetic instability (GIN). Microsatellite instability (MSI) and loss of heterozygosity (LOH) were evaluated at 5 microsatellite loci. The incidence of GIN was 21% (8/39) in CG-IM, 48% (40/83) in GC-IM, and 65% (54/83) in GC and showed a significant difference among these 3 categories. By tumor location, MSI showed the highest incidence in GC and GC-IM with the tumor located in the upper third of the stomach. GIN in GC and GC-IM significantly increased with the progression of tumor invasion from mucosal to advanced cancer. GIN, especially LOH, was more frequently detected in cases with vs without lymphatic or vascular invasion and lymph node involvement in GC and GC-IM. The GIN of GC and GC-IM was significantly similar in relation to clinicopathologic features. Biologic detection of GIN in IM may be a surrogate marker for GC risk and for clinical evaluation of malignant potential. The condition is consistent with the hypothesis of field cancerization in the stomach.


BMC Gastroenterology | 2012

Back-to-Back Comparison of Auto-Fluorescence Imaging (AFI) Versus High Resolution White Light Colonoscopy for Adenoma Detection

Kentaro Moriichi; Mikihiro Fujiya; Ryu Sato; Jiro Watari; Yoshiki Nomura; Toshie Nata; Nobuhiro Ueno; Shigeaki Maeda; Shin Kashima; Kentaro Itabashi; Chisato Ishikawa; Yuhei Inaba; Takahiro Ito; Kotaro Okamoto; Hiroki Tanabe; Yusuke Mizukami; Yusuke Saitoh; Yutaka Kohgo

BackgroundSome patients under close colonoscopic surveillance still develop colorectal cancer, thus suggesting the overlook of colorectal adenoma by endoscopists. AFI detects colorectal adenoma as a clear magenta, therefore the efficacy of AFI is expected to improve the detection ability of colorectal adenoma. The aim of this study is to determine the efficacy of AFI in detecting colorectal adenoma.MethodsThis study enrolled 88 patients who underwent colonoscopy at Asahikawa Medical University and Kushiro Medical Association Hospital. A randomly selected colonoscopist first observed the sigmoid colon and rectum with conventional high resolution endosopy (HRE). Then the colonoscopist changed the mode to AFI and handed to the scope to another colonoscopist who knew no information about the HRE. Then the second colonoscopist observed the sigmoid colon and rectum. Each colonoscopist separately recorded the findings. The detection rate, miss rate and procedural time were assessed in prospective manner.ResultsThe detection rate of flat and depressed adenoma, but not elevated adenoma, by AFI is significantly higher than that by HRE. In less-experienced endoscopists, AFI dramatically increased the detection rate (30.3%) and reduced miss rate (0%) of colorectal adenoma in comparison to those of HRE (7.7%, 50.0%), but not for experienced endoscopists. The procedural time of HRE was significantly shorter than that of AFI.ConclusionsAFI increased the detection rate and reduced the miss rate of flat and depressed adenomas. These advantages of AFI were limited to less-experienced endoscopists because experienced endoscopists exhibited a substantially high detection rate for colorectal adenoma with HRE.


Nature Communications | 2016

Probiotic-derived ferrichrome inhibits colon cancer progression via JNK-mediated apoptosis

Hiroaki Konishi; Mikihiro Fujiya; Hiroki Tanaka; Nobuhiro Ueno; Kentaro Moriichi; Junpei Sasajima; Katsuya Ikuta; Hiroaki Akutsu; Hiroki Tanabe; Yutaka Kohgo

Previous reports have suggested that some probiotics inhibit tumorigenesis and cancer progression. However, the molecules involved have not yet been identified. Here, we show that the culture supernatant of Lactobacillus casei ATCC334 has a strong tumour-suppressive effect on colon cancer cells. Using mass spectrometry, we identify ferrichrome as a tumour-suppressive molecule produced by L. casei ATCC334. The tumour-suppressive effect of ferrichrome is greater than that of cisplatin and 5-fluorouracil, and ferrichrome has less of an effect on non-cancerous intestinal cells than either of those agents. A transcriptome analysis reveals that ferrichrome treatment induces apoptosis, which is mediated by the activation of c-jun N-terminal kinase (JNK). Western blotting indicates that the induction of apoptosis by ferrichrome is reduced by the inhibition of the JNK signalling pathway. This we demonstrate that probiotic-derived ferrichrome exerts a tumour-suppressive effect via the JNK signalling pathway.


Gastrointestinal Endoscopy | 2008

Transnasal ultrathin endoscopy for placement of a long intestinal tube in patients with intestinal obstruction.

Ryu Sato; Jiro Watari; Hiroki Tanabe; Mikihiro Fujiya; Nobuhiro Ueno; Youkou Konno; Chisato Ishikawa; Takahiro Ito; Kentaro Moriichi; Kotaro Okamoto; Atsuo Maemoto; Kenji Chisaka; Yohei Kitano; Kakuya Matsumoto; Toshifumi Ashida; Toru Kono; Yutaka Kohgo

BACKGROUND The technical difficulties related to the insertion of a long intestinal tube into the jejunum under fluoroscopy present a considerable problem in patients with an intestinal obstruction. OBJECTIVE To evaluate the usefulness of endoscopic long intestinal-tube placement with the ultrathin esophagogastroduodenoscope (UT-EGD). DESIGN A prospective randomized clinical trial was conducted. PATIENTS Twenty-eight consecutive patients who presented with an intestinal obstruction were included in the study. INTERVENTION The UT-EGD was inserted nasally into at least the second portion of the duodenum or beyond. After a guidewire was introduced through the working channel, with fluoroscopic guidance, the UT-EGD itself was carefully removed with the guidewire left in place. Next, a hydrophilic intestinal tube was advanced over the guidewire into the jejunum, and then the guidewire was removed. MAIN OUTCOME MEASUREMENTS Primary end points are the total procedure time, the radiation exposure time, and the rate of complications, all compared with the conventional method. RESULTS The mean (+/-SD) total procedure time was 18.7 +/- 8.4 minutes for the UT-EGD method and 39.5 +/- 15.0 minutes for the conventional method, with a significant time difference between the 2 methods (P < .0005). The mean (+/-SD) radiation exposure time was also shorter with the UT-EGD method (11.1 +/- 6.0 minutes) than with the conventional method (30.3 +/- 13.7 minutes) (P < .0005). There were no complications, except for mild nasal bleeding with each method. CONCLUSIONS The UT-EGD method has definite advantages in the placement of a long intestinal tube for patients with an intestinal obstruction in comparison with the conventional method.


Journal of Clinical Pathology | 2006

K‐ras mutations and cell kinetics in Helicobacter pylori associated gastric intestinal metaplasia: a comparison before and after eradication in patients with chronic gastritis and gastric cancer

Jiro Watari; Atsumi Tanaka; Hiroki Tanabe; Ryu Sato; Kentaro Moriichi; Amen Hamdy Zaky; Kotaro Okamoto; Atsuo Maemoto; Mikihiro Fujiya; Toshifumi Ashida; Kiron M. Das; Yutaka Kohgo

Background:Helicobacter pylori related gastric intestinal metaplasia (IM) is considered to be a precancerous lesion. Aims: To identify the effects of H pylori eradication on K-ras mutations, cell kinetics in IM and histological changes in patients with and without gastric cancers in a one-year prospective study. Methods: Patients included group A (n = 39), chronic gastritis, and group B (n = 53), intestinal-type early gastric cancer patients who had all undergone endoscopic mucosal resection (n = 25) or surgical resection (n = 28). K-ras codon 12 mutations in IM were examined, followed by DNA sequencing analysis. Proliferating and apoptotic cells were detected with anti-Ki-67 antibody and using the TUNEL method, respectively. Results: The incidence of K-ras mutations in the cancer was only 3.8%. The mutant K-ras in IM was observed more frequently in group A (46.2%) than in group B patients (1.9%) (p<0.005). After eradication, the K-ras mutations significantly declined to 12.8% in group A (p<0.005). The mutation pattern of K-ras codon 12 before eradication was that GGT was mainly changed to AGT (50%) in group A. AGT transformation was not affected by treatment. Apoptosis in IM showed an increase after H pylori eradication in both groups (p<0.05 in group A) although no histological improvement in IM was observed. The monocyte score was significantly higher in group A than in group B (p<0.05); the score improved significantly after eradication. Conclusions: K-ras mutations in IM do not always play a role in gastric carcinogenesis but cell kinetics, especially apoptosis, in IM may contribute to it. There are early events in K-ras mutations which are influenced by H pylori infection; some mutations may also be selected by eradication. These unstable K-ras mutations in IM may be related to lymphocyte infiltration caused by H pylori infection.


International Journal of Colorectal Disease | 2012

Autofluorescence imaging and the quantitative intensity of fluorescence for evaluating the dysplastic grade of colonic neoplasms

Kentaro Moriichi; Mikihiro Fujiya; Ryu Sato; Toshie Nata; Yoshiki Nomura; Nobuhiro Ueno; Chisato Ishikawa; Yuhei Inaba; Takahiro Ito; Kotaro Okamoto; Hiroki Tanabe; Yusuke Mizukami; Jiro Watari; Yusuke Saitoh; Yutaka Kohgo

Background and aimsAutofluorescence imaging (AFI) is a novel technology which can capture fluorescence emitted from intestinal tissues. While AFI is useful for detecting colorectal neoplasms, it is unclear whether AFI can facilitate the diagnosis by differentiating the extent of dysplasia of colorectal neoplasms. This study investigated the efficacy of AFI in discriminating high-grade from low-grade adenoma.Materials and methodsSixty-seven patients who underwent colonoscopy with AFI were enrolled in this study. The AFI images obtained from 158 lesions in these patients were visually classified into four categories, namely, green (G), green with magenta spots (GM), magenta with green spots (MG), and magenta (M), according to their color intensities, immediately after the examination. The AFI images of the lesions were quantified using an image-analytical software program (F index). Either the F index or the visual assessment was prospectively compared with the dysplastic grade.ResultsThe F index of the high-grade adenomas was significantly lower than that of the low-grade adenomas, hyperplasia, and normal mucosa (p < 0.05). The incidence of the lesions classified into the M classification for high-grade adenomas (55.6%) was significantly higher than that of either low-grade adenomas (20.8%) or hyperplasia (0%). No correlation was observed between the F index or the visual classification and the tumor shape. The F index was not influenced by the size of the lesion, while the size was significantly associated with the visual classification of AFI.ConclusionsAFI, particularly the F index, is considered to be a useful procedure for estimating the dysplastic grade of colonic adenomas.

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Mikihiro Fujiya

Asahikawa Medical University

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Yutaka Kohgo

Asahikawa Medical College

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Nobuhiro Ueno

Asahikawa Medical University

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Hiroki Tanabe

Asahikawa Medical University

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Yuhei Inaba

Asahikawa Medical University

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Shin Kashima

Asahikawa Medical University

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Takahiro Ito

Asahikawa Medical University

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Jiro Watari

Hyogo College of Medicine

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Yoshiki Nomura

Asahikawa Medical University

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Kotaro Okamoto

Asahikawa Medical College

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