Your search keyword '"Je-Young Ryu"' showing total 3 results

1. Chimeric analysis of EGFP and DsRed2 transgenic mice demonstrates polyclonal maintenance of pancreatic acini

Author

Yoh-ichi Tagawa, Kenichi Harimoto, Je-Young Ryu, and Antoni Siswanto

Subjects

Genetically modified mouse, Green Fluorescent Proteins, Mice, Transgenic, Enteroendocrine cell, Biology, Green fluorescent protein, Islets of Langerhans, Mice, Acinus, Genetics, medicine, Animals, Progenitor cell, Mice, Inbred BALB C, geography, geography.geographical_feature_category, Chimera, Stem Cells, fungi, Pancreatic Ducts, Embryo, Islet, Molecular biology, Pancreas, Exocrine, Mice, Inbred C57BL, Blastocyst, medicine.anatomical_structure, Polyclonal antibodies, biology.protein, Animal Science and Zoology, Agronomy and Crop Science, Biotechnology

Abstract

The pancreatic islet is an assembly of specific endocrine cells. There are many conflicting reports regarding whether the acinus develops from single or multiple progenitor cells. This study investigated the development and maintenance clonality of the pancreatic acinus and duct using a chimeric analysis with EGFP and DsRed2 transgenic mice. Chimeric mice (G-R mice) were obtained by the aggregation method, using 8-cell stage embryos from EGFP and DsRed2 transgenic mice. The islets from the G-R mice were chimeric and mosaic, consisting of either EGFP- or DsRed2-positive populations, as in previous reports. On the other hand, most acini developed from either EGFP or DsRed2 origin, but some were chimeric. Interestingly, these chimeric acini were clearly separated into two-color regions and were not mosaic. Some large intralobular pancreatic ducts consisting of more than 10 cells were found to be chimeric, but no small ducts made up of less than 9 cells were chimeric. Our histological observations suggest that the pancreatic acinus polyclonally and directionally is maintained by multiple progenitor cells. Pancreatic large ducts also seem to develop polyclonally and might result from the assembly of small ducts that develop from a single origin. These findings provide useful information for further understanding pancreatic maintenance.

Published

2012

2. Nrk, an X-linked Protein Kinase in the Germinal Center Kinase Family, Is Required for Placental Development and Fetoplacental Induction of Labor

Author

Shinya Yamanaka, Kanako Nakao-Wakabayashi, Naoki Okamoto, Naomi Kitamura, Masayuki Komada, Je-Young Ryu, Kimitoshi Denda, Tomoko Ichisaka, and Yoh-ichi Tagawa

Subjects

Male, X Chromosome, Placenta, Uterus, Serine threonine protein kinase, Pregnancy Proteins, Protein Serine-Threonine Kinases, Biology, Biochemistry, X-inactivation, Andrology, Mice, Pregnancy, medicine, Animals, Placental Circulation, Yolk sac, Molecular Biology, Alleles, Crosses, Genetic, reproductive and urinary physiology, Fetus, Labor, Obstetric, Amnion, urogenital system, Intracellular Signaling Peptides and Proteins, Cell Biology, equipment and supplies, Mice, Mutant Strains, medicine.anatomical_structure, embryonic structures, Immunology, Pregnancy, Animal, Female, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, Developmental Biology

Abstract

The complete mechanism of labor induction in eutherian mammals remains unclear. Although important roles for the fetus and placenta in triggering labor have been proposed, no gene has been shown to be required in the fetus/placenta for labor induction. Here we show that Nrk, an X-linked gene encoding a Ser/Thr kinase of the germinal center kinase family, is essential in the fetus/placenta for labor in mice. Nrk was specifically expressed in the spongiotrophoblast layer, a fetus-derived region of the placenta, and Nrk disruption caused dysregulated overgrowth of the layer. Due to preferential inactivation of the paternally derived X chromosome in placenta, Nrk heterozygous mutant placentas exhibited a similar defect to that in Nrk-null tissues when the wild-type allele was paternally derived. However, the phenotype was weaker than in Nrk-null placentas due to leaky Nrk expression from the inactivated X chromosome. Crossing of Nrk-null females to wild-type and Nrk-null males, as well as uterine transfer of Nrk-null fetuses to wild-type females, revealed that pregnant mice exhibit a severe defect in delivery when all fetuses/placentas are Nrk-null. In addition, Nrk was not expressed in female reproductive tissues such as the uterus and ovary, as well as the fetal amnion and yolk sac, in pregnant mice. Progesterone and estrogen levels in the maternal circulation and placenta, which control the timing of labor, were unaffected upon Nrk disruption. We thus provide evidence for a novel labor-inducing fetoplacental signal that depends on the X chromosome and possibly arises from the placenta.

Published

2011

3. Nrk, an X-Iinked Protein Kinase in the Germinal Center Kinase Family, Is Required for Placental Development and Fetoplacental Induction of Labor.

Author

Denda, Kimitoshi, Nakao-Wakabayashi, Kanako, Okamoto, Naoki, Kitamura, Naomi, Je-Young Ryu, Tagawa, Yoh-ichi, Ichisaka, Tomoko, Yamanaka, Shinya, and Komada, Masayuki

Subjects

*MAMMALS, *FETUS, *PLACENTA, *LABOR (Obstetrics), *PROTEIN kinases

Abstract

The complete mechanism of labor induction in eutherian mammals remains unclear. Although important roles for the fetus and placenta in triggering labor have been proposed, no gene has been shown to be required in the fetus/placenta for labor induction. Here we show that Nrk, an X-linked gene encoding a Ser/Thr kinase of the germinal center kinase family, is essential in the fetus/placenta for labor in mice. Nrk was specifically expressed in the spongiotrophoblast layer, a fetus-derived region of the placenta, and Nrk disruption caused dysregulated overgrowth of the layer. Due to preferential inactivation of the paternally derived X chromosome in placenta, Nrk heterozygous mutant placentas exhibited a similar defect to that in Nrk-null tissues when the wild-type allele was paternally derived. However, the phenotype was weaker than in Nrk-null placentas due to leaky Nrk expression from the inactivated X chromosome. Crossing of Nrk-null females to wild-type and Nrk-null males, as well as uterine transfer of Nrk-null fetuses to wild-type females, revealed that pregnant mice exhibit a severe defect in delivery when all fetuses/placentas are Nrk-null. In addition, Nrk was not expressed in female reproductive tissues such as the uterus and ovary, as well as the fetal amnion and yolk sac, in pregnant mice. Progesterone and estrogen levels in the maternal circulation and placenta, which control the timing of labor, were unaffected upon Nrk disruption. We thus provide evidence for a novel labor-inducing fetoplacental signal that depends on the X chromosome and possibly arises from the placenta. [ABSTRACT FROM AUTHOR]

Published

2011