Mui Luong scite author profile

One hundred eighty-four serum samples from patients with ovarian cancer (n ‫؍‬ 109), patients with benign tumors (n ‫؍‬ 19), and healthy donors (n ‫؍‬ 56) were analyzed on strong anion-exchange surfaces using surface-enhanced laser desorption͞ionization )], 6 of 6 low malignant potential, 5 of the 6 benign tumors, and 9 of 10 normal patient samples. In conclusion, we have discovered three ovarian cancer biomarker protein panels that, when used together, effectively distinguished serum samples from healthy controls and patients with either benign or malignant ovarian neoplasia.

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BMP signaling is required for cell cleavage in preimplantation-mouse embryos

Mochel

Luong

Chiang

et al. 2015

Developmental Biology

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The mechanisms regulating cell division during development of the mouse pre-implantation embryo are poorly understood. We have investigated whether bone morphogenetic protein (BMP) signaling is involved in controlling cell cycle during mouse pre-implantation development. We mapped and quantitated the dynamic activities of BMP signaling through high-resolution immunofluorescence imaging combined with a 3D segmentation method. Immunostaining for phosphorylated Smad1/5/8 shows that BMP signaling is activated in mouse embryos as early as the 4-cell stage, and becomes spatially restricted by late blastocyst stage. Perturbation of BMP signaling in preimplantation mouse embryos, whether by treatment with a small molecule inhibitor, with Noggin protein, or by over-expression of a dominant-negative BMP receptor, indicates that BMPs regulate cell cleavage up to the morula stage. These results indicate that BMP signaling is active during mouse pre-implantation development and is required for cell cleavage in preimplantation mouse embryos.

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Bmp Indicator Mice Reveal Dynamic Regulation of Transcriptional Response

et al. 2012

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Cellular responses to Bmp ligands are regulated at multiple levels, both extracellularly and intracellularly. Therefore, the presence of these growth factors is not an accurate indicator of Bmp signaling activity. While a common approach to detect Bmp signaling activity is to determine the presence of phosphorylated forms of Smad1, 5 and 8 by immunostaining, this approach is time consuming and not quantitative. In order to provide a simpler readout system to examine the presence of Bmp signaling in developing animals, we developed BRE-gal mouse embryonic stem cells and a transgenic mouse line that specifically respond to Bmp ligand stimulation. Our reporter identifies specific transcriptional responses that are mediated by Smad1 and Smad4 with the Schnurri transcription factor complex binding to a conserved Bmp-Responsive Element (BRE), originally identified among Drosophila, Xenopus and human Bmp targets. Our BRE-gal mES cells specifically respond to Bmp ligands at concentrations as low as 5 ng/ml; and BRE-gal reporter mice, derived from the BRE-gal mES cells, show dynamic activity in many cellular sites, including extraembryonic structures and mammary glands, thereby making this a useful scientific tool.

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Stochastic response of mES cells toward BMP signaling is improved under dynamic microfluidic conditions

Luong¹,

Sun²,

Shin³

et al. 2009

Developmental Biology

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Applications of Deep Sequencing to Developmental Systems

Leventhal

Blitz

Luong

et al. 2015

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Mui Luong

Identification of biomarkers for ovarian cancer using strong anion-exchange ProteinChips: Potential use in diagnosis and prognosis

BMP signaling is required for cell cleavage in preimplantation-mouse embryos

Bmp Indicator Mice Reveal Dynamic Regulation of Transcriptional Response

Stochastic response of mES cells toward BMP signaling is improved under dynamic microfluidic conditions

Applications of Deep Sequencing to Developmental Systems

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