Your search keyword '"Minekawa R"' showing total 2 results

1. Involvement of Sp-1 in the Regulation of the Id-1 Gene during Trophoblast Cell Differentiation.

Author

Takeda, T., Sakata, M., Isobe, A., Yamamoto, T., Nishimoto, F., Minekawa, R., Hayashi, M., Okamoto, Y., Desprez, P.-Y., Tasaka, K., and Murata, Y.

Subjects

CELL differentiation, CHORIOCARCINOMA, STEM cells, ELECTROPHORESIS, ELECTROCHEMISTRY

Abstract

Abstract: Id-1, a member of the helix-loop-helix transcription factor family, inhibits the differentiation of Rcho-1 cells, which were derived from rat choriocarcinoma and consist of trophoblast stem cells. Id-1 is expressed at a high level in undifferentiated trophoblast stem cells and then down-regulated during early differentiation, and is thought to be a key regulator in the trophoblast giant-cell differentiation pathway. In this study, we analyzed the signaling mechanism regulating the high expression levels of Id-1 in undifferentiated Rcho-1 cells. Promoter deletion analysis revealed that a 31-bp sequence (Box-2 region), located between −200 and −169bp in the Id-1 promoter is necessary for the promoter activity. Electrophoretic mobility shift assays and DNA affinity precipitation assays showed that Box-2-binding activity was decreased during differentiation and that Sp-1 protein bound to this sequence. The protein level of Sp-1 was decreased during the differentiation. These results suggest that the Sp-1 protein level may regulate the Box-2-binding activity and the trophoblast giant-cell differentiation. [Copyright &y& Elsevier]

Published

2007

2. STAT3-mediated constitutive expression of SOCS3 in an undifferentiated rat trophoblast-like cell line.

Author

Isobe, A., Takeda, T., Sakata, M., Yamamoto, T., Minekawa, R., Hayashi, M., Auernhammer, C.J., Tasaka, K., and Murata, Y.

Subjects

TROPHOBLAST, CELL differentiation, LABORATORY rats, STEM cells, PHOSPHORYLATION

Abstract

In the trophoblast, constitutive expression of SOCS3 is important for the negative regulation of trophoblast giant cell differentiation. In this study, we analyzed the signaling pathway regulating the constitutive SOCS3 expression in undifferentiated Rcho-1 cells, which were derived from rat choriocarcinoma and consist of trophoblast stem cells that are capable of differentiating to trophoblast giant cells in vitro. PD98059, an MEK inhibitor, repressed the SOCS3 expression but AG490, a JAK2 inhibitor, did not. Promoter deletion analysis revealed that the STAT response element (SRE) in the SOCS3 promoter is necessary for the promoter activity. Overexpression of STAT3 increased the SOCS3 promoter activity, whereas expression of dominant-negative STAT3 reduced it. Constitutive STAT3 tyrosine phosphorylation that was not inhibited by either AG490 or PD98059 was demonstrated. Electrophoretic mobility shift assays showed the existence of a protein that bound to SRE and was supershifted with STAT3 antibody. This binding reaction was inhibited by neither AG490 nor PD98059. These findings imply that the ERK/MAPK pathway and STAT3 are involved in the constitutive activation of SOCS3 in undifferentiated Rcho-1 cells. Moreover, they indicate that the constitutive STAT3 tyrosine phosphorylation and the DNA binding activity of STAT3 do not depend on the ERK/MAPK or JAK kinase pathway. These results suggest that a trophoblast-specific STAT3 activation pathway is important for the regulation of giant cell differentiation. [ABSTRACT FROM AUTHOR]

Published

2006