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Dive into the research topics where Etsuko Hattori is active.

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Featured researches published by Etsuko Hattori.


Biochemical and Biophysical Research Communications | 2003

Differentiation of bone marrow cells into cells that express liver-specific genes in vitro: implication of the Notch signals in differentiation

Kazuo Okumoto; Takafumi Saito; Etsuko Hattori; Junitsu Ito; Tohru Adachi; Tadashi Takeda; Kazuhiko Sugahara; Hisayoshi Watanabe; Koji Saito; Hitoshi Togashi; Sumio Kawata

Bone marrow (BM) stem cells have been shown to differentiate into liver cells. It remains difficult to sort and culture BM stem cells, and the gene expression of liver-specific proteins in these cells has not been fully investigated. We used a negative selective magnetic cell separation system to obtain stem cell-enriched BM cells. The cells obtained were cultured with hepatocytes or with hepatocyte growth factor (HGF), and the differentiation of BM cells into cells expressing liver-specific genes, hepatocyte nuclear factor (HNF) 1alpha, cytokeratin (CK) 8, alpha-fetoprotein (AFP), and albumin was investigated by the reverse transcription-polymerase chain reaction. We also investigated the gene expressions of Notch receptor-1 (Notch-1) and its ligand Jagged-1 in BM cell differentiation. Sorted BM cells showed positive for Sca-1 (Ataxin-1) by immunofluorescence staining. Fluorescence activated cell sorter analysis showed that 32.6% of sorted BM cells had a high level of expression of the hematopoietic stem cell marker CD90 (Thy-1). When cultured with hepatocytes, these cells expressed the liver-specific genes HNF1alpha and CK8 on culture day 3, AFP and albumin on culture day 7. When cultured with HGF (20ng/ml), the cells expressed HNF1alpha on day 3 and CK8 on day 7. Gene expressions of Notch-1 and Jagged-1 were detected in cultured BM cells on day 3. These results suggest that the negative selective magnetic cell separation system is useful for the rapid preparation of stem cell-enriched BM cells, and that the Notch signaling pathway plays a role in BM cell differentiation into a hepatocyte lineage in vitro.


Liver International | 2004

Possible contribution of circulating transforming growth factor-beta1 to immunity and prognosis in unresectable hepatocellular carcinoma.

Kazuo Okumoto; Etsuko Hattori; Kazuko Tamura; Shinichi Kiso; Hisayoshi Watanabe; Koji Saito; Takafumi Saito; Hitoshi Togashi; Sumio Kawata

Transforming growth factor‐β1 (TGF‐β1) has been implicated in tumor progression. The relationship of this cytokine as measured in plasma to anti‐tumor immunity and prognosis was investigated.


Journal of Gastroenterology | 2006

Characteristics of rat bone marrow cells differentiated into a liver cell lineage and dynamics of the transplanted cells in the injured liver

Kazuo Okumoto; Takafumi Saito; Hiroaki Haga; Etsuko Hattori; Rika Ishii; Tetsuru Karasawa; Akihiko Suzuki; Keiko Misawa; Mai Sanjo; Junitsu Ito; Kazuhiko Sugahara; Koji Saito; Hitoshi Togashi; Sumio Kawata

BackgroundBone marrow cells (BMCs) have been shown to differentiate into a liver cell lineage, but little is known about their dynamics following transplantation. BMCs were cultured to investigate the expression of liver-specific genes in vitro and transplanted into in vivo liver-injury models to elucidate their dynamics in the liver.MethodsThe mRNA expression of various liver-specific genes in BMCs cocultured with hepatocytes was analyzed using reverse transcription-polymerase chain reaction. BMCs from transgenic rats expressing green fiuorescent protein were transplanted into the spleen of rat liver-injury models induced with 2-acetylaminofiuorene (2-AAF) or carbon tetrachloride (CCl4). BMCs were also transplanted directly into livers treated with CCl4 to determine which route is better for transplantation.ResultsBMCs differentiated into a liver cell lineage in vitro and expressed mRNAs consistent with mature hepatocytes, including albumin. The transplanted BMCs were found in the liver in the CCl4-induced injury model, but not in the 2-AAF-induced model. The hepatocyte growth factor and fibroblast growth factor mRNA levels in the liver were significantly higher in the CCl4-induced model than in the 2-AAF-induced model. Migration of BMCs to the liver was more effective following injection into the liver, rather than into the spleen.ConclusionsCultured BMCs differentiated into a liver cell lineage are a potential source for cell transplantation. Transplantation is successful in the severely injured liver with a high level of expression of mRNAs for growth factors. Injection of BMCs directly into the liver is the preferred route of administration.


Journal of Gastroenterology and Hepatology | 2007

Serum levels of stem cell factor and thrombopoietin are markedly decreased in fulminant hepatic failure patients with a poor prognosis.

Kazuo Okumoto; Takafumi Saito; Motoyuki Onodera; Ayuka Sakamoto; Mamiko Tanaka; Etsuko Hattori; Hiroaki Haga; Jun–Itsu Ito; Kazuhiko Sugahara; Koji Saito; Hitoshi Togashi; Sumio Kawata

Background and Aim:  Hematopoietic growth factors including stem cell factor (SCF), thrombopoietin (TPO) and granulocyte colony stimulating factor (G‐CSF) have a potential role in inducing bone marrow hematopoietic stem cells to move into the circulation, and the association of these factors with liver regeneration has received a lot of attention recently. The aim of this study was to determine the serum levels of such factors in patients with acute liver injury.


Hepatology Research | 2010

Expression of the RNA‐binding protein Musashi1 in adult liver stem‐like cells

Etsuko Hattori; Hong-Jin Shu; Takafumi Saito; Kazuo Okumoto; Hiroaki Haga; Junji Yokozawa; Junitsu Ito; Hisayoshi Watanabe; Koji Saito; Hitoshi Togashi; Sumio Kawata

Aim:  Musashi1 is an RNA‐binding protein that regulates the Notch signaling pathway in stem cells. Our previous study revealed that Musashi1 is expressed in early hepatocytes during liver development in the mouse. However, whether this unique protein is expressed with Notch signaling markers in adult liver stem‐like cells remains unknown.


Biochemical and Biophysical Research Communications | 2004

Genetic variations in humans associated with differences in the course of hepatitis C

Takafumi Saito; Guijin Ji; Haruhide Shinzawa; Kazuo Okumoto; Etsuko Hattori; Tohru Adachi; Tadashi Takeda; Kazuhiko Sugahara; Junitsu Ito; Hisayoshi Watanabe; Koji Saito; Hitoshi Togashi; Keisuke Ishii; Tadashi Matsuura; Kiyoshi Inageda; Masaaki Muramatsu; Sumio Kawata


Journal of Medical Virology | 2003

Spontaneous elimination of serum hepatitis C virus (HCV) RNA in chronic HCV carriers: a population-based cohort study.

Hisayoshi Watanabe; Takafumi Saito; Haruhide Shinzawa; Kazuo Okumoto; Etsuko Hattori; Tohru Adachi; Tadashi Takeda; Kazuhiko Sugahara; Junitsu Ito; Koji Saito; Hitoshi Togashi; Ryosuke Suzuki; Masahiro Hayashi; Tatsuo Miyamura; Yoshiharu Matsuura; Sumio Kawata


Hepatology Research | 2003

Possible contribution of circulating interleukin-10 (IL-10) to anti-tumor immunity and prognosis in patients with unresectable hepatocellular carcinoma.

Etsuko Hattori; Kazuo Okumoto; Tohru Adachi; Tadashi Takeda; Junitsu Ito; Kazuhiko Sugahara; Hisayoshi Watanabe; Koji Saito; Takafumi Saito; Hitoshi Togashi; Sumio Kawata


Hepatology | 2003

Separate analysis of asialoglycoprotein receptors in the right and left hepatic lobes using 99mTc-GSA SPECT

Kazuhiko Sugahara; Hitoshi Togashi; Kazuei Takahashi; Yuya Onodera; Mai Sanjo; Keiko Misawa; Akihiko Suzuki; Tohru Adachi; Junitsu Ito; Kazuo Okumoto; Etsuko Hattori; Tadashi Takeda; Hisayoshi Watanabe; Koji Saito; Takafumi Saito; Yukio Sugai; Sumio Kawata


Journal of Hepatology | 2005

Differentiation of rat bone marrow cells cultured on artificial basement membrane containing extracellular matrix into a liver cell lineage

Kazuo Okumoto; Takafumi Saito; Etsuko Hattori; Junitsu Ito; Akihiko Suzuki; Keiko Misawa; Rika Ishii; Tetsuru Karasawa; Hiroaki Haga; Mai Sanjo; Tadashi Takeda; Kazuhiko Sugahara; Koji Saito; Hitoshi Togashi; Sumio Kawata

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