Your search keyword '"Ono, Satoshi"' showing total 9 results

1. Atrophic gastritis and enlarged gastric folds diagnosed by double-contrast upper gastrointestinal barium X-ray radiography are useful to predict future gastric cancer development based on the 3-year prospective observation

Author

Yamamichi, Nobutake, Hirano, Chigaya, Ichinose, Masao, Takahashi, Yu, Minatsuki, Chihiro, Matsuda, Rie, Nakayama, Chiemi, Shimamoto, Takeshi, Kodashima, Shinya, Ono, Satoshi, Tsuji, Yosuke, Niimi, Keiko, Sakaguchi, Yoshiki, Kataoka, Yosuke, Saito, Itaru, Asada-Hirayama, Itsuko, Takeuchi, Chihiro, Yakabi, Seiichi, Kaikimoto, Hikaru, Matsumoto, Yuta, Yamaguchi, Daisuke, Kageyama-Yahara, Natsuko, Fujishiro, Mitsuhiro, Wada, Ryoichi, Mitsushima, Toru, and Koike, Kazuhiko

Published

2016

2. Optimal Size of Jejunal Pouch as a Reservoir after Total Gastrectomy: A Single-Center Prospective Randomized Study

Author

Tsujimoto, Hironori, Sakamoto, Naoko, Ichikura, Takashi, Hiraki, Shuichi, Yaguchi, Yoshihisa, Kumano, Isao, Matsumoto, Yusuke, Yoshida, Kazumichi, Ono, Satoshi, Yamamoto, Junji, and Hase, Kazuo

Published

2011

3. Outcomes for patients following hepatic resection of metastatic tumors from gastric cancer

Author

Tsujimoto, Hironori, Ichikura, Takashi, Ono, Satoshi, Sugasawa, Hidekazu, Hiraki, Shuichi, Sakamoto, Naoko, Yaguchi, Yoshihisa, Hatsuse, Kazuo, Yamamoto, Junji, and Hase, Kazuo

Published

2010

4. Transduced caudal‐type homeobox (CDX) 2/CDX1 can induce growth inhibition on CDX‐deficient gastric cancer by rapid intestinal differentiation.

Author

Nakayama, Chiemi, Yamamichi, Nobutake, Tomida, Shuta, Takahashi, Yu, Kageyama‐Yahara, Natsuko, Sakurai, Kouhei, Takeuchi, Chihiro, Inada, Ken‐ichi, Shiogama, Kazuya, Nagae, Genta, Ono, Satoshi, Tsuji, Yosuke, Niimi, Keiko, Fujishiro, Mitsuhiro, Aburatani, Hiroyuki, Tsutsumi, Yutaka, and Koike, Kazuhiko

Abstract

Intestinal metaplasia induced by ectopic expression of caudal‐type homeobox (CDX)2 and/or CDX1 (CDX) is frequently observed around gastric cancer (GC). Abnormal expression of CDX is also observed in GC and suggests that inappropriate gastrointestinal differentiation plays essential roles in gastric tumorigenesis, but their roles on tumorigenesis remain unelucidated. Publicly available databases show that GC patients with higher CDX expression have significantly better clinical outcomes. We introduced CDX2 and CDX1 genes separately into GC‐originated MKN7 and TMK1 cells deficient in CDX. Marked suppression of cell growth and dramatic morphological change into spindle‐shaped flat form were observed along with induction of intestinal marker genes. G0‐G1 growth arrest was accompanied by changed expression of cell cycle‐related genes but not with apoptosis or senescence. Microarray analyses additionally showed decreased expression of gastric marker genes and increased expression of stemness‐associated genes. Hierarchical clustering of 111 GC tissues and 21 non‐cancerous gastric tissues by selected 18 signature genes based on our transcriptome analyses clearly categorized the 132 tissues into non‐cancer, "CDX signature"‐positive GC, and "CDX signature"‐negative GC. Gene set enrichment analysis indicated that "CDX signature"‐positive GC has lower malignant features. Immunohistochemistry of 89 GC specimens showed that 50.6% were CDX2‐deficient, 66.3% were CDX1‐deficient, and 44.9% were concomitant CDX2/CDX1‐deficient, suggesting that potentially targetable GC cases by induced intestinal differentiation are quite common. In conclusion, exogenous expression of CDX2/CDX1 can lead to efficient growth inhibition of CDX‐deficient GC cells. It is based on rapidly induced intestinal differentiation, which may be a future therapeutic strategy. Exogenous expression of CDX2/CDX1 can lead to G0‐G1 growth arrest in CDX‐deficient gastric cancer cells, accompanied by induction of intestinal genes and decreased expression of gastric genes. Publicly available databases and hierarchical clustering of gastric tissue showed that gastric cancer with CDX expression has significantly better clinical outcomes. A novel therapy against gastric cancer based on induced intestinal differentiation may be possible in the future. [ABSTRACT FROM AUTHOR]

Published

2018

5. CD47 is an adverse prognostic factor and a therapeutic target in gastric cancer.

Author

Yoshida, Kazumichi, Tsujimoto, Hironori, Matsumura, Kouji, Kinoshita, Manabu, Takahata, Risa, Matsumoto, Yusuke, Hiraki, Shuichi, Ono, Satoshi, Seki, Shuhji, Yamamoto, Junji, and Hase, Kazuo

Subjects

STOMACH cancer, MEMBRANE proteins, GLYCOPROTEINS, IMMUNOHISTOCHEMISTRY, FLOW cytometry, PHAGOCYTOSIS, IMMUNODEFICIENCY

Abstract

CD47 is an antiphagocytic molecule that acts via ligation to signal regulatory protein alpha on phagocytes; its enhanced expression and therapeutic targeting have recently been reported for several malignancies. However, CD47 expression in gastric cancer is not well documented. Immunohistochemical expression of CD47 in surgical specimens was investigated. Expression of CD47 and CD44, a known gastric cancer stem cell marker, were investigated in gastric cancer cell lines by flow cytometry. MKN45 and MKN74 gastric cancer cells were sorted by fluorescence-activated cell sorting according to CD44 and CD47 expression levels, and their in vitro proliferation, spheroid-forming capacity, and in vivo tumorigenicity were studied. In vitro phagocytosis of cancer cells by human macrophages in the presence of a CD47 blocking monoclonal antibody (B6H12) and the survival of immunodeficient mice intraperitoneally engrafted with MKN45 cells and B6H12 were compared to experiments using control antibodies. Immunohistochemistry of the clinical specimens indicated that CD47 was positive in 57 out of 115 cases, and its positivity was an independent adverse prognostic factor. Approximately 90% of the MKN45 and MKN74 cells expressed CD47 and CD44. CD47hi gastric cancer cells showed significantly higher proliferation and spheroid colony formation than CD47lo, and CD44hi CD47hi cells showed the highest proliferation in vitro and tumorigenicity in vivo. B6H12 significantly enhanced in vitro phagocytosis of cancer cells by human macrophages and prolonged the survival of intraperitoneal cancer dissemination in mice compared to control antibodies. In conclusion, CD47 is an adverse prognostic factor and promising therapeutic target in gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2015

6. Photodynamic therapy using nanoparticle loaded with indocyanine green for experimental peritoneal dissemination of gastric cancer.

Author

Tsujimoto, Hironori, Morimoto, Yuji, Takahata, Risa, Nomura, Shinsuke, Yoshida, Kazumichi, Horiguchi, Hiroyuki, Hiraki, Shuichi, Ono, Satoshi, Miyazaki, Hiromi, Saito, Daizo, Hara, Isao, Ozeki, Eiichi, Yamamoto, Junji, and Hase, Kazuo

Abstract

Although there have been multiple advances in the development of novel anticancer agents and operative procedures, prognosis of patients with advanced gastric cancer remains poor, especially in patients with peritoneal metastasis. In this study, we established nanoparticles loaded with indocyanine green ( ICG) derivatives: ICG loaded lactosomes ( ICGm) and investigated the diagnostic and therapeutic value of photodynamic therapy ( PDT) using ICGm for experimental peritoneal dissemination of gastric cancer. Experimental peritoneal disseminated xenografts of human gastric cancer were established in nude mice. Three weeks after intraperitoneal injection of the cancer cells, either ICGm ( ICGm-treated mice) or ICG solution ( ICG-treated mice) was injected through the tail vein. Forty-eight hours after injection of the photosensitizer, in vivo and ex vivo imaging was carried out. For PDT, 48 h after injection of the photosensitizer, other mice were irradiated through the abdominal wall, and the body weight and survival rate were monitored. In vivo imaging revealed that peritoneal tumors were visualized through the abdominal wall in ICGm-treated mice, whereas only non-specific fluorescence was observed in ICG-treated mice. The PDT reduced the total weight of the disseminated nodules and significantly improved weight loss and survival rate in ICGm-treated mice. In conclusion, ICGm can be used as a novel diagnostic and therapeutic nanodevice in peritoneal dissemination of gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2014

7. Cathepsin E Is a Marker of Gastric Differentiation and Signet-Ring Cell Carcinoma of Stomach: A Novel Suggestion on Gastric Tumorigenesis.

Author

Konno-Shimizu, Maki, Yamamichi, Nobutake, Inada, Ken-ichi, Kageyama-Yahara, Natsuko, Shiogama, Kazuya, Takahashi, Yu, Asada-Hirayama, Itsuko, Yamamichi-Nishina, Mitsue, Nakayama, Chiemi, Ono, Satoshi, Kodashima, Shinya, Fujishiro, Mitsuhiro, Tsutsumi, Yutaka, Ichinose, Masao, and Koike, Kazuhiko

Subjects

CATHEPSINS, STOMACH cancer, ADENOCARCINOMA, CELL lines, GASTROINTESTINAL tumors, GASTROENTEROLOGY, CELL differentiation

Abstract

Gastric cancer (GC) presents various histological features, though the mechanism underlying its diversity is seldom elucidated. It is mainly classified into well differentiated tubular adenocarcinoma (tub1), moderately differentiated tubular adenocarcinoma (tub2), poorly differentiated adenocarcinoma (por), signet-ring cell carcinoma (sig), mucinous adenocarcinoma (muc), and papillary adenocarcinoma (pap). By screening, we found cathepsin E (CTSE) expresses universally in sig-type, occasionally in por-type, and rarely in tub1/tub2-type GC cell lines. In surgically-resected specimens, CTSE was immunostained in 50/51 sig-type (98.0%), 3/10 tub1-type (30.0%), 7/18 tub2-type (38.9%), 15/26 por-type (57.7%), 4/10 pap-type (40.0%), and 0/3 muc-type (0.0%) GC. In endoscopically-resected specimens, 6/7 sig-type (85.7%), 7/52 tub1-type (13.7%), 5/12 tub2-type (41.7%), 2/7 pap-type (28.6%) GC and 0/6 adenoma (0.0%) expressed CTSE. For non-malignant tissues, CTSE is universally expressed in normal fundic, pyloric, and cardiac glands of stomach, but hardly in other digestive organs. In the precancerous intestinal metaplasia of stomach, CTSE is mostly observed in mixed gastric-and-intestinal type and deficient in solely-intestinal type. CTSE expression is positively correlated with gastric marker MUC5AC (p<0.0001) and negatively correlated with intestinal marker MUC2 (p = 0.0019). For sig-type GC, in both tumors and background mucosa, expression of MUC5AC and CTSE is high whereas that of MUC2 is low, indicating that sig-type GC reflects the features of background mucosa. For gastric adenoma and tub1/tub2-type GC, more undifferentiated tumors tend to show higher expression of CTSE with MUC5AC and lower expression of MUC2 in tumors, but they tend to present lower expression of CTSE, MUC5AC and MUC2 in background mucosa. These suggest that more malignant gastric adenocarcinoma with stronger gastric and weaker intestinal properties tend to arise from background mucosa with decreased both gastric and intestinal features. In conclusion, CTSE is a marker of both gastric differentiation and signet-ring cell carcinoma, which should shed light on the mechanism of gastric tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2013

8. Serum granulysin level as a novel prognostic marker in patients with gastric carcinoma.

Author

Saigusa, Susumu, Ichikura, Takashi, Tsujimoto, Hironori, Sugasawa, Hidekazu, Majima, Takashi, Kawarabayashi, Nobuaki, Chochi, Kentaro, Ono, Satoshi, Kinoshita, Manabu, Seki, Shuhji, Ogawa, Kazuyuki, and Mochizuki, Hidetaka

Subjects

CELLULAR immunity, IMMUNE response, CYTOKINES, GASTRIC diseases, CANCER patients, PROGNOSIS

Abstract

Background: Granulysin is a cytolytic molecule present in human cytotoxic T cells and natural killer cell granules, and plays a key role in the cell-mediated immunity against tumor and infection. However, few studies have estimated serum granulysin concentrations in patients with solid or hematological malignancies. Methods: Peripheral blood samples were taken from patients with gastric carcinoma preoperatively and from healthy volunteers. Serum and tumor tissue granulysin concentrations were measured using a granulysin-specific ELISA kit in order to assess its prognostic value. Results: Both serum and tumor tissue granulysin concentrations were higher in patients with stage II or III gastric cancer and lower in patients with stage IV disease as compared to healthy controls. The low preoperative granulysin levels were associated with more frequent hepatic and peritoneal metastases, and with a poor outcome of the curative gastrectomy. Conclusions: Preoperative serum granulysin levels reflect the status of cell-mediated immunity in patients with gastric carcinoma. It has significance as a prognostic determinant following a curative resection. [ABSTRACT FROM AUTHOR]

Published

2007

9. Rebamipide induces dendritic cell recruitment to N-methyl-N′-nitro-N-nitrosoguanidine (MNNG)-exposed rat gastric mucosa based on IL-1β upregulation

Author

Yamamichi, Nobutake, Oka, Masashi, Inada, Ken-ichi, Konno-Shimizu, Maki, Kageyama-Yahara, Natsuko, Tamai, Hideyuki, Kato, Jun, Fujishiro, Mitsuhiro, Kodashima, Shinya, Niimi, Keiko, Ono, Satoshi, Tsutsumi, Yutaka, Ichinose, Masao, and Koike, Kazuhiko

Subjects

*DENDRITIC cells, *METHYL groups, *NITROSOGUANIDINE, *LABORATORY rats, *GASTRIC mucosa, *INTERLEUKIN-1, *TUMOR necrosis factors

Abstract

Abstract: Rebamipide is usually used for mucosal protection, healing of gastric ulcers, treatment of gastritis, etc., but its effects on gastric malignancy have not been elucidated. Using Lewis and Buffalo rat strains treated with peroral administration of N-methyl-N′-nitro-N-nitrosoguanidine (MNNG), we evaluated the effect of rebamipide on the induction of tumor-suppressive dendritic cells, which are known to be heterogeneous antigen-presenting cells of bone marrow origin and are critical for the initiation of primary T-cell responses. Using CD68 as a marker for dendritic cells, the stomach pyloric mucosae of Lewis and Buffalo rats were immunohistochemically analyzed in the presence or absence of rebamipide and MNNG. After a 14-day treatment of rebamipide alone, no significant change in number of CD68-expressing cells was detected in either rat strain. However, after concurrent exposure to MNNG for 14days, treatment with rebamipide slightly increased CD68-positive cells in the Lewis strain, and significantly increased them in the Buffalo strain. Analysis of two chemotactic factors of dendritic cells, IL-1β and TNF-α, in the gastric cancer cells showed that expression of IL-1β, but not TNF-α, was induced by rebamipide in a dose-dependent manner. A luciferase promoter assay using gastric SH-10-TC cells demonstrated that an element mediating rebamipide action exists in the IL-1β gene promoter region. In conclusion, rebamipide has potential tumor-suppressive effects on gastric tumorigenesis via the recruitment of dendritic cells, based on the upregulation of the IL-1β gene in gastric epithelial cells. [Copyright &y& Elsevier]

Published

2012