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120 results on '"Hsu, C.W."'

1. Genome-wide screening reveals the genetic basis of mammalian embryonic eye development

Author

Chee, J.M., Lanoue, L., Clary, D., Higgins, K., Bower, L., Flenniken, A., Guo, R., Adams, D.J., Bosch, F., Braun, R.E., Brown, S.D.M., Chin, H.J.G., Dickinson, M.E., Hsu, C.W., Dobbie, M., Gao, X., Galande, S., Grobler, A., Heaney, J.D., Herault, Y., de Angelis, M.H., Mammano, F., Nutter, L.M.J, Parkinson, H., Qin, C., Shiroishi, T., Sedlacek, R., Seong, J.K., Xu, Y., Brooks, B., McKerlie, C., Lloyd, K.C.K., Westerberg, H., and Moshiri, A.

Subjects
Cancer Research, Technology Platforms
Abstract

BACKGROUND: Microphthalmia, anophthalmia, and coloboma (MAC) spectrum disease encompasses a group of eye malformations which play a role in childhood visual impairment. Although the predominant cause of eye malformations is known to be heritable in nature, with 80% of cases displaying loss-of-function mutations in the ocular developmental genes OTX2 or SOX2, the genetic abnormalities underlying the remaining cases of MAC are incompletely understood. This study intended to identify the novel genes and pathways required for early eye development. Additionally, pathways involved in eye formation during embryogenesis are also incompletely understood. This study aims to identify the novel genes and pathways required for early eye development through systematic forward screening of the mammalian genome. RESULTS: Query of the International Mouse Phenotyping Consortium (IMPC) database (data release 17.0, August 01, 2022) identified 74 unique knockout lines (genes) with genetically associated eye defects in mouse embryos. The vast majority of eye abnormalities were small or absent eyes, findings most relevant to MAC spectrum disease in humans. A literature search showed that 27 of the 74 lines had previously published knockout mouse models, of which only 15 had ocular defects identified in the original publications. These 12 previously published gene knockouts with no reported ocular abnormalities and the 47 unpublished knockouts with ocular abnormalities identified by the IMPC represent 59 genes not previously associated with early eye development in mice. Of these 59, we identified 19 genes with a reported human eye phenotype. Overall, mining of the IMPC data yielded 40 previously unimplicated genes linked to mammalian eye development. Bioinformatic analysis showed that several of the IMPC genes colocalized to several protein anabolic and pluripotency pathways in early eye development. Of note, our analysis suggests that the serine-glycine pathway producing glycine, a mitochondrial one-carbon donator to folate one-carbon metabolism (FOCM), is essential for eye formation. CONCLUSIONS: Using genome-wide phenotype screening of single-gene knockout mouse lines, STRING analysis, and bioinformatic methods, this study identified genes heretofore unassociated with MAC phenotypes providing models to research novel molecular and cellular mechanisms involved in eye development. These findings have the potential to hasten the diagnosis and treatment of this congenital blinding disease.

Published
2023

2. Protocol for fast scRNA-seq raw data processing using scKB and non-arbitrary quality control with COPILOT

Author

Hsu, C.W., Shahan, R., Nolan, T.M., Benfey, P.N., and Ohler, U.

Subjects
Cancer Research
Abstract

We describe a protocol to perform fast and non-arbitrary quality control of single-cell RNA sequencing (scRNA-seq) raw data using scKB and COPILOT. scKB is a wrapper script of kallisto and bustools for accelerated alignment and transcript count matrix generation, which runs significantly faster than the popular tool Cell Ranger. COPILOT then offers non-arbitrary background noise removal by comparing distributions of low-quality and high-quality cells. Together, this protocol streamlines the processing workflow and provides an easy entry for new scRNA-seq users. For complete details on the use and execution of this protocol, please refer to Shahan et al. (2022).

Published
2022

5. A single-cell Arabidopsis root atlas reveals developmental trajectories in wild-type and cell identity mutants

Author

Shahan, R., Hsu, C.W., Nolan, T.M., Cole, B.J., Taylor, I.W., Greenstreet, L., Zhang, S., Afanassiev, A., Vlot, A.H.C., Schiebinger, G., Benfey, P.N., and Ohler, U.

Subjects
Cancer Research
Abstract

In all multicellular organisms, transcriptional networks orchestrate organ development. The Arabidopsis root, with its simple structure and indeterminate growth, is an ideal model for investigating the spatiotemporal transcriptional signatures underlying developmental trajectories. To map gene expression dynamics across root cell types and developmental time, we built a comprehensive, organ-scale atlas at single-cell resolution. In addition to estimating developmental progressions in pseudotime, we employed the mathematical concept of optimal transport to infer developmental trajectories and identify their underlying regulators. To demonstrate the utility of the atlas to interpret new datasets, we profiled mutants for two key transcriptional regulators at single-cell resolution, shortroot and scarecrow. We report transcriptomic and in vivo evidence for tissue trans-differentiation underlying a mixed cell identity phenotype in scarecrow. Our results support the atlas as a rich community resource for unraveling the transcriptional programs that specify and maintain cell identity to regulate spatiotemporal organ development.

Published
2022

10. A single cell Arabidopsis root atlas reveals developmental trajectories in wild type and cell identity mutants

Author

Shahan, R., Hsu, C.W., Nolan, T.M., Cole, B.J., Taylor, I.W., Vlot, A.H.C., Benfey, P.N., and Ohler, U.

Subjects
Cancer Research
Abstract

Cell fate acquisition is a fundamental developmental process in all multicellular organisms. Yet, much is unknown regarding how a cell traverses the pathway from stem cell to terminal differentiation. Advances in single cell genomics1 hold promise for unraveling developmental mechanisms2–3 in tissues4, organs5–6, and organisms7–8. However, lineage tracing can be challenging for some tissues9 and integration of high-quality datasets is often necessary to detect rare cell populations and developmental states10,11. Here, we harmonized single cell mRNA sequencing data from over 110,000 cells to construct a comprehensive atlas for a stereotypically developing organ with indeterminate growth, the Arabidopsis root. To test the utility of the atlas to interpret new datasets, we profiled mutants for two key transcriptional regulators at single cell resolution, shortroot and scarecrow. Although both transcription factors are required for early specification of cell identity12, our results suggest the existence of an alternative pathway acting in mature cells to specify endodermal identity, for which SHORTROOT is required. Uncovering the architecture of this pathway will provide insight into specification and stabilization of the endodermis, a tissue analogous to the mammalian epithelium. Thus, the atlas is a pivotal advance for unraveling the transcriptional programs that specify and maintain cell identity to regulate organ development in space and time.

Published
2020

11. Origin and transformation of light hydrocarbons ascending at an active pockmark on Vestnesa Ridge, Arctic Ocean

Author

Pape, T., Bünz, S., Hong, W.‐L., Torres, M. E., Riedel, Michael, Panieri, G., Lepland, A., Hsu, C.W., Wintersteller, P., Wallmann, Klaus, Schmidt, Christopher, Yao, H., Bohrmann, Gerhard, Pape, T., Bünz, S., Hong, W.‐L., Torres, M. E., Riedel, Michael, Panieri, G., Lepland, A., Hsu, C.W., Wintersteller, P., Wallmann, Klaus, Schmidt, Christopher, Yao, H., and Bohrmann, Gerhard

Published
2020
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12. Differentially transcribed genes in skeletal muscle of Duroc and Taoyuan pigs

Author

Lin, C.S. and Hsu, C.W.

Subjects
Swine -- Comparative analysis, Swine -- Physiological aspects, Genetic research -- Comparative analysis, Genetic research -- Physiological aspects, DNA microarrays -- Comparative analysis, DNA microarrays -- Physiological aspects, Zoology and wildlife conservation
Abstract

The objective of this study was to compare gene transcription profiles of LM between two pig breeds, Duroc and Taoyuan, which display dramatically different postnatal muscle growth. We isolated LM from neonatal pigs, and the Duroc muscle length and mass were greater (P < 0.01) than for Taoyuan pigs; however, insignificant differences in the muscle fiber area and the percentage of fiber types were found. A human high-density complementary DNA (cDNA) microarray consisting of 9,182 probes was used to compare gene transcription profiles of LM between the two breeds. The results showed that the transcription level of 73 genes and 44 genes in Duroc LM were upregulated and down-regulated by at least 1.75-fold (P < 0.05) compared with Taoyuan, respectively. The strongly upregulated genes in Duroc pigs included those encoding the complex of myofibrillar proteins (e.g., myosin light and heavy chains, and troponin), ribosomal proteins, transcription regulatory proteins (e.g., skeletal muscle LIM protein 1 [SLIM1] and high-mobility group proteins), and energy metabolic enzymes (e.g., electron-transferring flavo-protein dehydrogenase, NADH dehydrogenase, malate dehydrogenase, and ATP synthases). The highly transcribed genes that encode energy metabolic enzymes indicate a more glycolytic metabolism in Duroc LM, thereby favoring carbohydrates rather than lipids for use as energy substrates in this tissue. The over-transcribed genes that encode skeletal muscle-predominant proteins or transcription regulators that control myo-genesis and/or muscle growth suggest a general mechanism for the observed higher rate of postnatal muscle growth in Duroc pigs. The transcription of one such gene, SLIM1, was more highly transcribed (P < 0.01) in Duroc LM at birth and at postnatal d 7 than in Taoyuan. The transcription of SLIM1 increased (P < 0.05) in Duroc LM from neonate through 7 d of age, whereas its transcription remained essentially constant in Taoyuan during this period. These results suggest that SLIM1 may be useful for the development of markers associated with the postnatal muscle growth of pigs. Key Words: Gene Transcription, Microarray, Neonate, Pig, Skeletal Muscle, Skeletal Muscle LIM Protein 1

Published
2005

20. Development of vortical structure over delta wing with leading-edge flap

Author

Kuo, Cheng-Hsiung and Hsu, C.W.

Subjects
Wings (Animal) -- Research, Leading edges (Aerodynamics) -- Research, Flaps (Airplanes) -- Research, Aerospace and defense industries, Business, Science and technology
Abstract

The flow structure over a delta wing with a leading-edge flap is largely dependent on the flap deflection angle and angle of attack when the flap is statically deflected on the windward side. The vortex breakdown location can be substantially delayed when the oscillating leading-edge flap has a time scale of almost one convection time scale. The vortex breakdown location is not delayed so effectively when the convection time scale is much longer than the oscillating leading-edge flap time scale. There is a phase shift in the development of vortex breakdown due to the vortical structures' mutual interaction over the wing surface.

Published
1997

21. Effect of Ag segregation on reversal behavior of [(FePt).sub.77] [Ag.sub.23] alloy thin films

Author

Chen, S.K., Hsu, C.W., Yuan, F.T., Hsiao, S.N., Chang, H.W., Sun, A.C., Liao, W.M., Wei, D.H., Lee, H.Y., Huang, H.W., Hsu, Y.W., and Yao, Y.D.

Subjects
Dielectric films -- Analysis, Thin films -- Analysis, Magnetic fields -- Analysis, Segregation -- Analysis, Business, Electronics, Electronics and electrical industries
Abstract

Effect of Ag segregation on magnetic and structural properties of [(FePt).sub.77] [Ag.sub.23] single-layer films were studied. Thin films were first sputtered on the heated glass substrates and cooled to room temperature, a post annealing at temperatures ([T.sub.p]) from 200 [degrees]C to 400 [degrees]C for 60 min was then applied. [L1.sub.0] structure formed as substrate temperature ([T.sub.s]) equals to 600 [degrees]C and 700 [degrees]C. For those ordered films, Ag was observed to precipitate as particles on the film surface and grow with the increasing [T.sub.s]. After post annealing at 400 [degrees]C for 60 min, those silver particles dissolved into the film, leading to changes in reversal behavior. The optimum condition is obtained in the [T.sub.s] = 600 [degrees]C, [T.sub.p] = 400 [degrees]C sample. Drastic reduction in coercive squareness ratio (from >0.8 to 0.41) and enhanced coercivity (from 4.7 to 6.4 kOe) indicate the reversal behavior alters from cooperative to independent. Negative [delta]M curve suggests that this independent rotation results from the reduction of exchange interactions. Index Terms--Coercivity enhancement, domain structure, FePt, reversal behavior, segregation, thin film.

Published
2007

22. Ordering enhancement of FePt thin films by introducing Mo layers

Author

Hsiao, S.N., Chen, S.K., Yuan, F.T., Huang, H.W., Hsu, C.W., Yao, Y.D., and Lee, H.Y.

Subjects
Dielectric films -- Research, Dielectric films -- Design and construction, Thin films -- Research, Thin films -- Design and construction, Magnetrons -- Usage, Business, Electronics, Electronics and electrical industries
Abstract

Single-layer FePt, bilayer Mo/FePt and FePt/Mo, and trilayer Mo/FePt/Mo samples were prepared by rf magnetron sputtering. Each layer of FePt and Mo in the studied samples is 20 nm in thickness. Samples were deposited onto corning 1737 glass substrate at room temperature, then annealed at 350[degrees]C and 400[degrees]C for a period of 10-120 min. Coercivities of the Mo-layer introduced samples were higher than those of single-layer FePt. X-ray diffraction data also indicate higher degree of ordering for Mo-layer introduced samples. We suggest that the incoherent FePt/Mo interface may induce extra nucleation sites for ordering transformation, thus lower the threshold of ordering temperature. Index Terms--Coercivity enhancement, FePt/Mo bilayer films, FePt/Mo interface, ordering enhancement.

Published
2007

23. Prevention of Postdental Procedure Bacteremia: A Network Meta-analysis

Author

Zeng, B.S., primary, Lin, S.Y., additional, Tu, Y.K., additional, Wu, Y.C., additional, Stubbs, B., additional, Liang, C.S., additional, Yeh, T.C., additional, Chen, T.Y., additional, Carvalho, A.F., additional, Lin, P.Y., additional, Lei, W.T., additional, Hsu, C.W., additional, Chen, Y.W., additional, Tseng, P.T., additional, and Chen, C.H., additional

Published
2019
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24. The effect of GePt underlayer on the [L1.sub.0] ordering FePt thin films

Author

Hsu, C.J., Tsai, J.L., Hsu, C.W., Chen, S.K., and Chang, W.C.

Subjects
Electromagnetism -- Research, Dielectric films -- Research, Thin films -- Research, Business, Electronics, Electronics and electrical industries
Abstract

We have explored the effect of GePt underlayer deposition temperature on [L1.sub.0] ordered FePt films. As the deposition temperature of GePt increased from room temperature (RT) to 800 [degrees]C, the coercively ([H.sub.c]) of the (GePt/FePt) bilayer increased from 1.1 to 9.1 kOe, which indicated the [Ge.sup.2] [Pt.sub.3] phase formed at higher deposition temperature and promoted the [L1.sub.o] ordered FePt phase formation. Under the similar process, the single layer FePt coercively was 6.9 kOe. The interlayer diffusion between GePt and FePt cannot be avoided when the GePt underlayer deposited at RT. An interesting island-like microstructure was observed when GePt underlayer deposited at higher temperature. Index Terms--Coercivity, [L1.sub.0] ordered FePt.

Published
2006

38. Optical characterization of individual quantum dots

Author

Holtz, P.O., primary, Hsu, C.W., additional, Larsson, L.A., additional, Karlsson, K.F., additional, Dufåker, D., additional, Lundskog, A., additional, Forsberg, U., additional, Janzen, E., additional, Moskalenko, E.S., additional, Dimastrodonato, V., additional, Mereni, L., additional, and Pelucchi, E., additional

Published
2012
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46. 919 ENTECAVIR (ETV) THERAPY IN CHRONIC HEPATITIS B PATIENTS PREVIOUSLY TREATED WITH ADEFOVIR (ADV) WITH INCOMPLETE RESPONSE ON-TREATMENT OR RELAPSE OFF-TREATMENT

Author

Lai, C.L., primary, Elion, R., additional, Sherman, M., additional, Hann, H.W., additional, Tyrell, D.L., additional, Hsu, C.W., additional, Tan, C.K., additional, Peng, C.Y., additional, Leung, N., additional, Mercarni, K., additional, Zhang, H., additional, Iloeje, U.H., additional, and Kreter, B., additional

Published
2009
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