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Dive into the research topics where Hideo Yamanari is active.

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Featured researches published by Hideo Yamanari.


Clinical & Experimental Metastasis | 2000

High collagenolytic activity in spontaneously highly metastatic variants derived from a human pancreatic cancer cell line (SUIT-2) in nude mice

Norio Kitamura; Takeshi Iwamura; Hideo Yamanari; Kikuo Kawano; Michael A. Hollingsworth; Toshiaki Setoguchi

Cell lines with high metastatic capacity to the lung were established by sequential passage of a human pancreatic cancer cell line (SUIT-2) through the lung of a nude mouse, via the lateral tail vein and from a subcutaneous inoculum. Cells of the parental SUIT-2 and sublines S2-VPx (x-cycle selection from SUIT-2 cells, by Vein-Pulmonary metastasis-culture) and S2-CPx (x-cycle selection, by Cutis-Pulmonary metastasis-culture) were injected intravenously or subcutaneously into nude mice to produce experimental or spontaneous lung metastasis. The S2-VP10 cell line produced pulmonary metastases in 100% of the nude mice, when injected intravenously. It failed, however, to produce more lung colonies than its parent cell line, when injected subcutaneously. The S2-CP8 cell line produced extensive pulmonary metastases in 100% of the nude mice, when injected either intravenously or subcutaneously. This study indicates that the nude mouse provided a good model for in vivo selection of metastatic cells from SUIT-2 cells both experimentally and spontaneously, and that the SUIT-2, S2-VPx, and S2-CPx cell lines will be valuable in the study of human cancer metastasis. We previously reported high levels of ezrin expression in the S2-VP10 and S2-CP8 cell lines. Here we show that these cell lines exhibit a greater capacity to invade or attach to various extracellular matrix components than the parent SUIT-2 cells. The S2-CP8 cell lines also exhibit greater level of type-I and type-IV collagen-degrading activity than the parent SUIT-2 cell line and the S2-VP10 cell line, which shows similar collagen-degrading activity to the parent SUIT-2 cells. In RT-PCR studies, SUIT-2, S2-CP8 and S2-VP10 cell lines constitutively expressed many matrix metalloproteinases (MMP-1, MMP-2, MMP-3, MMP7, MMP-9, MMP-10 and MMP-14). These results suggest that some parameters that enhance adhesion and invasion are important to both experimental and spontaneous metastasis and the collagen degrading enzymes are predicted to play a key-role during spontaneous metastasis.


Clinical & Experimental Metastasis | 1994

Heterogeneities of attachment, chemotaxis, and protease production among clones with different metastatic potentials from a human pancreatic cancer cell line

Takeshi Iwamura; Norio Kitamura; Hideo Yamanari; Toshiaki Setoguchi

The present study extends our investigations into the metastatic heterogeneity among four clonal cell lines (S2-007:H, S2-013:M1, S2-020:M2, and S2-028:L) from a human pancreatic cancer cell line (SUIT-2), and extends our discussion the positive correlation between metastatic potential and the type I collagenase activity of the cells, focusing on their interaction with extracellular matrix. Ability to attach to the reconstituted basement membrane (Matrigel) was higher for clone H than clone L during an observation period of 30–60 min, whereas clones M1 and M2 were found to be intermediate in ability. In densitometric and radioactive studies, clone L exhibited the lowest collagenolytic activity against mouse and human type IV collagen, while clone H exhibited the highest activity in the densitometric study and clone M1 was the highest in the radioactive study. The production of urinary-type plasminogen activator was highest in clone L and lowest in clone H. On the other hand, tissue-type plasminogen activator was highest in clone M2 and low in both clones H and L. Clone M2 exhibited the highest chemotactic activity toward diluted Matrigel, whereas clone L had the lowest activity. On the whole, these clones showed heterogenous interactions with an extracellular matrix. It is suggested that the attachment activity to basement membrane and the type IV collagenolytic activity of the cells may be positively correlated with their metastatic potential, whereas the production of urinary-type plasminogen activator was negatively correlated, but confirmation of these findings awaits further study.


Surgery Today | 1996

ADENOCARCINOMA IN THE ANAL CANAL ASSOCIATED WITH A FISTULA : REPORT OF A CASE

Hideo Yamanari; Kyosuke Inada; Takeshi Iwamura; Syuichi Hokkoku; Sadao Tanaka; Minoru Fukuda; Toshiaki Setoguchi

Adenocarcinoma in the anal canal associated with an anal fistula is extremely rare, and in most cases its origin is difficult to ascertain because the primary sites have already been destroyed before any diagnosis of malignancy is able to be made. We report herein the case of a 62-year-old man found to have papillary adenocarcinoma with partial mucinous carcinoma associated with an anal fistula. The tumor was not exposed to the mucosal surface of the anal canal or rectum and an abdominoperineal resection was carried out. Macroscopic findings suggested that the tumor had developed from the anal fistula; however, the tumor showed a positive result when tested for O-acetylated sialic acids. This test also proved positive in the mucus of normal rectal mucosa, but not in the mucus of the anal glands. We speculated that the results of these tests may indicate that this tumor could have originated from the rectal mucosa, from where it migrated into the anal fistula.


Oncology | 2004

Establishment and Characterization of a Novel Human Pancreatic Cancer Cell Line (SUIT-4) Metastasizing to Lymph Nodes and Lungs in Nude Mice

Kikuo Kawano; Takeshi Iwamura; Hideo Yamanari; Yasuhisa Seo; Tatsuo Suganuma; Kazuo Chijiiwa

A new tumor cell line (SUIT-4) derived from ascites of a patient with carcinoma of the pancreas has been established in tissue culture and in nude mice, and maintained for over 7 years. In tissue culture, the cells grew as a confluent monolayer with piling up of cells in some areas. The population doubling time during the exponential phase of the cell growth was 43.9 h in vitro. Chromosome count ranged from 63 to 68 with a modal number of 67. Subcutaneous injection of cultured cells into the flanks of nude mice resulted in tumor formation with a doubling time of 88.8 h. Histopathologically, xenografts in nude mice were moderately differentiated tubular adenocarcinoma, and the tumor cells showed spontaneous metastasis to the regional lymph nodes in 6 of 21 nude mice and to the lung in 4 of 21. Transmission electron microphotographs confirmed the ductal cell origin of the carcinoma and revealed that the cells had abundant mitochondria and lysosomes. SUIT-4 cells released carcinoembryonic antigen (3.08 × 102 ng/1 × 106 cells/24 h) and carbohydrate antigen 19-9 (4.75 × 104 U/1 × 106 cells/24 h) during exponential cell growth in vitro. Reverse transcriptase-polymerase chain reaction studies revealed that SUIT-4 cells expressed matrix metalloproteinases 1, 3, 7, 10 and 14.


Cancer Research | 1997

P-selectin Expression in a Metastatic Pancreatic Tumor Cell Line (SUIT-2)

Takeshi Iwamura; Thomas C. Caffrey; Norio Kitamura; Hideo Yamanari; Toshiaki Setoguchi; Michael A. Hollingsworth


Experimental Cell Research | 1994

Extracellular Matrix Components Regulating Glandular Differentiation and the Formation of Basal Lamina of a Human Pancreatic Cancer Cell Line in Vitro

Hideo Yamanari; Tatsuo Suganuma; Takeshi Iwamura; Norio Kitamura; Toshiaki Setoguchi


Nihon Rinsho Geka Gakkai Zasshi (journal of Japan Surgical Association) | 2003

A CASE OF ECTOPIC ANISAKIASIS ASSOCIATED WITH EARLY GASTRIC CANCER

Toshinori Sakurai; Ichiro Niina; Mayumi Fujiwara; Hideo Yamanari; Toshio Shimayama; Kazuo Chijiiwa


Nihon Rinsho Geka Gakkai Zasshi (journal of Japan Surgical Association) | 2002

A CASE OF TRANSVERSE COLON VOLVULUS OCCURRED AFTER A SIGMOIDECTOMY

Toshinori Sakurai; Mikio Kanemaru; Hideo Yamanari; Yoichiro Mori; Toshio Shimayama; Kazuo Chijiiwa


Jpn J Gastroenterol Surg, Nihon Shokaki Geka Gakkai zasshi | 2002

A Case of Transverse Colon Volvulus

Hideo Yamanari; Toshio Shimayama; Toshinori Sakurai; Mikio Kanemaru; Youichirou Mori


Oncology | 2004

Contents Vol. 66, 2004

Francesco Parmeggiani; Ciro Costagliola; Sergio D’Angelo; Carlo Incorvaia; Paolo Perri; Adolfo Sebastiani; Wen-Ying Lee; Wu-Chou Su; Pin-Wen Lin; How-Ran Guo; Tsai-Wang Chang; Helen H.W. Chen; Young Ho Yun; Tito R. Mendoza; Dae Seog Heo; Taiwoo Yoo; Bong Yul Heo; Hyeoun-Ae Park; Ho Cheol Shin; Xin Shelley Wang; Charles S. Cleeland; Wenshu Sun; Jiro Fujimoto; Teruhiko Tamaya; Kikuo Kawano; Takeshi Iwamura; Yasuhisa Seo; Tatsuo Suganuma; Kohei Murata; Eiji Miyoshi

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Charles S. Cleeland

University of Texas MD Anderson Cancer Center

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