Your search keyword '"Matsumi, Yoshiaki"' showing total 3 results

1. Nuclear receptor gene alteration in human induced pluripotent stem cells with hepatic differentiation propensity.

Author

Itaba, Noriko, Wairagu, Peninah M., Aramaki, Natsumi, Yasui, Toshihiro, Matsumi, Yoshiaki, Kono, Yohei, Phan, Ai N.H., Otsu, Makoto, Kunisada, Takahiro, Nakamura, Yukio, Okano, Hideyuki, Jeong, Yangsik, and Shiota, Goshi

Subjects

NUCLEAR receptors (Biochemistry), INDUCED pluripotent stem cells, GENE expression, REGENERATIVE medicine, LIVER diseases, BIOLOGICAL research, CELL differentiation

Abstract

Aim Human induced pluripotent stem (hi PS) cells are an alternative cell source of regenerative medicine for liver disease. Because variations in hepatic differentiation efficacy among hi PS cells exist, it is important to select a hi PS cell line with hepatic differentiation propensity. In addition, nuclear receptors ( NR) regulate essential biological processes including differentiation and development. In this study, we identified the hi PS cell line with hepatic differentiation propensity and examined expression levels of 48 NR during this process. Methods We screened 28 hi PS cell lines, which are established from various tissues of healthy persons with various reprogramming methods, using a three-step differentiation method, and examined expression levels of 48 NR by quantitative real-time polymerase chain reaction during the differentiation process in the selected cells. Results hi PS- RIKEN- 2B and hi PS- RIKEN- 2F cells have hepatic differentiation propensity. Differentiation propensity towards endoderm was affected by donor origin but not by reprogramming methods or cell type of origins. Expression levels of NR were closely associated with those of hepatic differentiation markers. Furthermore, expression patterns of NR were categorized as five patterns. In particular, seven NR such as chicken ovalbumin upstream promoter transcription factor 1, retinoic acid receptor α, peroxisome proliferator-activated receptor-γ, progesterone receptor, photoreceptor cell-specific nuclear receptor, tailless homolog orphan receptor and glucocorticoid receptor were identified as the genes of which expression gradually goes up with differentiation. Conclusion These findings will be useful for not only elucidating mechanisms of hepatic differentiation of hi PS cells but also cell-based therapy for liver diseases. [ABSTRACT FROM AUTHOR]

Published

2014

2. c-Jun N-terminal kinase activation by oxidative stress suppresses retinoid signaling through proteasomal degradation of retinoic acid receptor α protein in hepatic cells.

Author

Hoshikawa, Yoshiko, Kanki, Keita, Ashla, An Afida, Arakaki, Yuta, Azumi, Junya, Yasui, Toshihiro, Tezuka, Yuta, Matsumi, Yoshiaki, Tsuchiya, Hiroyuki, Kurimasa, Akihiro, Hisatome, Ichiro, Hirano, Tadamichi, Fujimoto, Jiro, Kagechika, Hiroyuki, Shomori, Kohei, Ito, Hisao, and Shiota, Goshi

Abstract

We previously reported that impaired retinoid signaling causes hepatocellular carcinoma (HCC) through oxidative stress. However, the interaction between oxidative stress and retinoid signaling has not been fully understood. To address this issue, the effects of hydrogen peroxide on the transcriptional activity of RAR/RXR heterodimers, RARα and RXRα proteins and intracellular signaling pathways were examined. The transcriptional activity of RAR/RXR examined by the DR5-tk-Luc reporter assay was significantly suppressed. The RARα protein level began to decrease at 6 h after treatment and declined thereafter. However, RARα mRNA were not changed. Activation of extracellular regulated kinases (ERK), p38, c-Jun N-terminal kinase (JNK) and Akt was observed after treatment of hydrogen peroxide. SP600125, an inhibitor of JNK, reversed the RARα protein level reduced by hydrogen peroxide. Anisomycin, an activator of JNK, reduced RARα protein. Transfection of wild-type JNK-constitutive actively expressing plasmid, but not kinase-negative JNK-expressing plasmid caused reduction of RARα protein. Proteasomal degradation of RARα was observed after anisomycin treatment; however, the mutant RARα, of which phosphorylation sites are replaced with alanines, was not degradated. In hepatitis C virus (HCV)-related human liver tissues, phospho-JNK and RARα reciprocally expressed with the progression of liver disease. Finally, the staining of 8-OHdG and thioredoxin was increased with the disease progression. These data indicate that JNK activation by oxidative stress suppresses retinoid signaling through proteasomal degradation of RARα, suggesting that a vicious cycle between aberrant retinoid signaling and oxidative stress accelerates hepatocarcinogenesis. ( Cancer Sci 2011; 102: 934-941) [ABSTRACT FROM AUTHOR]

Published

2011

3. Iron state in association with retinoid metabolism in non-alcoholic fatty liver disease.

Author

Tsuchiya, Hiroyuki, Ashla, An Afida, Hoshikawa, Yoshiko, Matsumi, Yoshiaki, Kanki, Keita, Enjoji, Munechika, Momosaki, Seiya, Nakamuta, Makoto, Taketomi, Akinobu, Maehara, Yoshihiko, Shomori, Kohei, Kurimasa, Akihiro, Hisatome, Ichiro, Ito, Hisao, and Shiota, Goshi

Subjects

RETINOIDS, METABOLISM, FATTY liver, REACTIVE oxygen species, CYTOCHROMES, TRETINOIN, GENE expression

Abstract

We have recently reported that hyperdynamic state of retinoid metabolism, which may lead to the shortage of retinoid, is observed in patients with non-alcoholic fatty liver disease (NAFLD). Hepatic iron overload, which causes production of reactive oxygen species (ROS), is also frequently seen in NAFLD patients. The aim of the study is to examine iron state and retinoid metabolic state simultaneously, and to clarify the relationship between two disorders. Thirty-six persons, comprising 17 patients with simple steatosis (SS), 11 with NASH, and 8 normal controls (N), were examined on hepatic expression of iron metabolism-related genes including hemojuvelin (HJV), hepcidin (HEPC), transferrin receptor 1 and 2 (TfR1, TfR2), ferroportin (FPN), neogenin (NEO) and ferritin heavy chain (FtH) and hepatic iron contents in addition to expression 51 genes which is involved in retinoid metabolism and antioxidative action. In patients with NAFLD, expression of HJV, TfR2, FPN, TfR1, FtH, SOD and catalase was increased, compared with that in N. In addition, hepatic iron content, which was increased in NASH, was correlated with expression level of TfR2. Expression of cellular retinoid binding protein ( CRBP1), alcohol dehydrogenase 1 ( ADH1) and cytochrome P450 26A1( CYP26A1) was significantly correlated with that of HJV, TfR2 and FPN, respectively. The results of the present study suggest that the reasons responsible for iron accumulation in NASH in the present study may partly be due to enhanced expression of TfRs, especially TfR2, and hyperdynamic state of retinoid metabolism is closely related to iron metabolism in the disease. [ABSTRACT FROM AUTHOR]

Published

2010