Takashi Hamazaki scite author profile

The Greenhouse Gases Observing Satellite (GOSAT) monitors carbon dioxide (CO(2)) and methane (CH(4)) globally from space using two instruments. The Thermal and Near Infrared Sensor for Carbon Observation Fourier-Transform Spectrometer (TANSO-FTS) detects gas absorption spectra of the solar short wave infrared (SWIR) reflected on the Earth's surface as well as of the thermal infrared radiated from the ground and the atmosphere. TANSO-FTS is capable of detecting three narrow bands (0.76, 1.6, and 2.0 microm) and a wide band (5.5-14.3 microm) with 0.2 cm(-1) spectral resolution (interval). The TANSO Cloud and Aerosol Imager (TANSO-CAI) is an ultraviolet (UV), visible, near infrared, and SWIR radiometer designed to detect cloud and aerosol interference and to provide the data for their correction. GOSAT is placed in a sun-synchronous orbit 666 km at 13:00 local time, with an inclination angle of 98 degrees . A brief overview of the GOSAT project, scientific requirements, instrument designs, hardware performance, on-orbit operation, and data processing is provided.

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Induction of Cytoplasmic Rods and Rings Structures by Inhibition of the CTP and GTP Synthetic Pathway in Mammalian Cells

Carcamo

et al. 2011

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BackgroundCytoplasmic filamentous rods and rings (RR) structures were identified using human autoantibodies as probes. In the present study, the formation of these conserved structures in mammalian cells and functions linked to these structures were examined.Methodology/Principal FindingsDistinct cytoplasmic rods (∼3–10 µm in length) and rings (∼2–5 µm in diameter) in HEp-2 cells were initially observed in immunofluorescence using human autoantibodies. Co-localization studies revealed that, although RR had filament-like features, they were not enriched in actin, tubulin, or vimentin, and not associated with centrosomes or other known cytoplasmic structures. Further independent studies revealed that two key enzymes in the nucleotide synthetic pathway cytidine triphosphate synthase 1 (CTPS1) and inosine monophosphate dehydrogenase 2 (IMPDH2) were highly enriched in RR. CTPS1 enzyme inhibitors 6-diazo-5-oxo-L-norleucine and Acivicin as well as the IMPDH2 inhibitor Ribavirin exhibited dose-dependent induction of RR in >95% of cells in all cancer cell lines tested as well as mouse primary cells. RR formation by lower concentration of Ribavirin was enhanced in IMPDH2-knockdown HeLa cells whereas it was inhibited in GFP-IMPDH2 overexpressed HeLa cells. Interestingly, RR were detected readily in untreated mouse embryonic stem cells (>95%); upon retinoic acid differentiation, RR disassembled in these cells but reformed when treated with Acivicin.Conclusions/SignificanceRR formation represented response to disturbances in the CTP or GTP synthetic pathways in cancer cell lines and mouse primary cells and RR are the convergence physical structures in these pathways. The availability of specific markers for these conserved structures and the ability to induce formation in vitro will allow further investigations in structure and function of RR in many biological systems in health and diseases.

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A Heterogeneous Expression Pattern for Nanog in Embryonic Stem Cells

et al. 2007

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Nanog is a critical homeodomain factor responsible for maintaining embryonic stem (ES) cell self-renewal and pluripotency. Of interest, Nanog expression is not homogeneous in the conventional culture of murine ES cells. A Nanog-high population expresses markers for pluripotent ES cells, whereas a Nanog-low population expresses markers for primitive endoderm, such as Gata6. Since the inner cell mass of early blastocysts has recently been reported to be heterogeneous in terms of Nanog and Gata6 expression, ES cells appear to closely resemble the developing stage from which they originate. We further demonstrate that Nanog can directly repress Gata6 expression through its binding to the proximal promoter region of the Gata6 gene and that overexpression of Nanog reduces heterogeneity during ES cell maintenance. Interestingly, Nanog heterogeneity does not correlate with the heterogeneous expression of stage-specific embryonic antigen-1, suggesting that multiple but overlapping levels of heterogeneity may exist in ES cells. These findings provide insight into the factors that control ES cell self-renewal and the earliest lineage commitment to primitive endoderm while also suggesting methods to promote homogeneity during ES cell maintenance.

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