14,110 research outputs found
Measurement-induced nonlocality in arbitrary dimensions in terms of the inverse approximate joint diagonalization
Here we focus on the measurement induced nonlocality and present a
redefinition in terms of the skew information subject to a broken observable.
It is shown that the obtained quantity possesses an obvious operational
meaning, can tackle the noncontractivity of the measurement induced nonlocality
and has analytic expressions for many quantum states. Most importantly, an
inverse approximate joint diagonalization algorithm, due to its simplicity,
high efficiency, stability, and state independence, is presented to provide
almost analytic expressions for any quantum state, which can also shed light on
other aspects in physics
GPER-induced signaling is essential for the survival of breast cancer stem cells.
G protein-coupled estrogen receptor-1 (GPER), a member of the G protein-coupled receptor (GPCR) superfamily, mediates estrogen-induced proliferation of normal and malignant breast epithelial cells. However, its role in breast cancer stem cells (BCSCs) remains unclear. Here we showed greater expression of GPER in BCSCs than non-BCSCs of three patient-derived xenografts of ER- /PR+ breast cancers. GPER silencing reduced stemness features of BCSCs as reflected by reduced mammosphere forming capacity in vitro, and tumor growth in vivo with decreased BCSC populations. Comparative phosphoproteomics revealed greater GPER-mediated PKA/BAD signaling in BCSCs. Activation of GPER by its ligands, including tamoxifen (TMX), induced phosphorylation of PKA and BAD-Ser118 to sustain BCSC characteristics. Transfection with a dominant-negative mutant BAD (Ser118Ala) led to reduced cell survival. Taken together, GPER and its downstream signaling play a key role in maintaining the stemness of BCSCs, suggesting that GPER is a potential therapeutic target for eradicating BCSCs
The Information Of The Milky Way From 2MASS Whole Sky Star Count: The Bimodal Color Distributions
The J-Ks color distribution (CD) with a bin size of 0.05 magnitude for the
entire Milky Way has been carried out by using the Two Micron All Sky Survey
Point Source Catalog (2MASS PSC). The CDs are bimodal, which has a red peak at
0.8 < J-Ks < 0.85 and a blue peak at 0.3 < J-Ks < 0.4. The colors of the red
peak are more or less the same for the whole sky, but that of the blue peak
depend on Galactic latitude, (J-Ks ~ 0.35 at low Galactic latitudes and 0.35 <
J-Ks < 0.4 for other sky areas). The blue peak dominates the bimodal CDs at low
Galactic latitudes and becomes comparable with the red peak in other sky
regions. In order to explain the bimodal distribution and the global trend
shown by the all sky 2MASS CDs, we assemble an empirical HR diagram, which is
composed by observational-based near infrared HR diagrams and color magnitude
diagrams, and incorporate a Milky Way model. In the empirical HR diagram, the
main sequence stars turnoff the thin disk is relatively bluer, (J-Ks)0 = 0.31,
when we compare with the thick disk which is (J-Ks)0 = 0.39. The age of the
thin/thick disk is roughly estimated to be around 4-5/8-9 Gyr according to the
color-age relation of the main sequence turnoff. In general, the 2MASS CDs can
be treated as a tool to census the age of stellar population of the Milky Way
in a statistical manner and to our knowledge this is a first attempt to measure
the age.Comment: Accepted by ApJ on Sept. 11 201
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Functional Effects of let-7g Expression in Colon Cancer Metastasis.
MicroRNA regulation is crucial for gene expression and cell functions. It has been linked to tumorigenesis, development and metastasis in colorectal cancer (CRC). Recently, the let-7 family has been identified as a tumor suppressor in different types of cancers. However, the function of the let-7 family in CRC metastasis has not been fully investigated. Here, we focused on analyzing the role of let-7g in CRC. The Cancer Genome Atlas (TCGA) genomic datasets of CRC and detailed data from a Taiwanese CRC cohort were applied to study the expression pattern of let-7g. In addition, in vitro as well as in vivo studies have been performed to uncover the effects of let-7g on CRC. We found that the expression of let-7g was significantly lower in CRC specimens. Our results further supported the inhibitory effects of let-7g on CRC cell migration, invasion and extracellular calcium influx through store-operated calcium channels. We report a critical role for let-7g in the pathogenesis of CRC and suggest let-7g as a potential therapeutic target for CRC treatment
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