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38 results on '"Pei-Hsuan Chu"'

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1. 3D-Suspension culture platform for high throughput screening of neurotoxic chemicals using LUHMES dopaminergic neurons

2. Artificial intelligence-assisted fast screening cervical high grade squamous intraepithelial lesion and squamous cell carcinoma diagnosis and treatment planning

3. Scalable generation of sensory neurons from human pluripotent stem cells

4. Efficient and safe single-cell cloning of human pluripotent stem cells using the CEPT cocktail

5. SEQUIN is an R/Shiny framework for rapid and reproducible analysis of RNA-seq data

6. A Versatile Polypharmacology Platform Promotes Cytoprotection and Viability of Human Pluripotent and Differentiated Cells

7. The MT1G Gene in LUHMES Neurons Is a Sensitive Biomarker of Neurotoxicity

8. Stem Cell-Derived Endothelial Cell Model that Responds to Tobacco Smoke Like Primary Endothelial Cells

9. A Comprehensive Roadmap of Human Placental Development in vitro

10. Scalable Generation of Pseudo-Unipolar Sensory Neurons from Human Pluripotent Stem Cells

11. Enhancing the Fitness of Embryoid Bodies and Organoids by Chemical Cytoprotection

12. SEQUIN: rapid and reproducible analysis of RNA-seq data in R/Shiny

13. Directed Differentiation of Human Pluripotent Stem Cells into Radial Glia and Astrocytes Bypasses Neurogenesis

14. Human Pluripotent Stem Cells for High-Throughput Drug Screening and Characterization of Small Molecules

16. In Vitro Exposure Systems and Dosimetry Assessment Tools for Inhaled Tobacco Products: Workshop Proceedings, Conclusions and Paths Forward for In Vitro Model Use

17. A Versatile Polypharmacology Platform Promotes Cytoprotection and Viability of Human Pluripotent and Differentiated Cells

18. Comprehensive Analyses and Prioritization of Tox21 10K Chemicals Affecting Mitochondrial Function by in-Depth Mechanistic Studies

19. Engineered kinase activation reveals unique morphodynamic phenotypes and associated trafficking for Src family isoforms

20. Dissecting motility signaling through activation of specific Src-effector complexes

21. Engineering extrinsic disorder to control protein activity in living cells

22. Identification of an HptB-mediated multi-step phosphorelay in Pseudomonas aeruginosa PAO1

24. USER-FRIENDLY TOOLS FOR QUANTIFYING THE DYNAMICS OF CELLULAR MORPHOLOGY AND INTRACELLULAR PROTEIN CLUSTERS

25. Comprehensive Analyses and Prioritization of Tox21 10K Chemicals Affecting Mitochondrial Function by in-Depth Mechanistic Studies.

26. Generation of a Light Inhibited Src Kinase through Insertion of LOV into the Catalytic Domain

27. An optogenetic tool for the activation of endogenous diaphanous-related formins induces thickening of stress fibers without an increase in contractility: Photo-activation of Diaphanous-related Formins

28. Purified vitamin K epoxide reductase alone is sufficient for conversion of vitamin K epoxide to vitamin K and vitamin K to vitamin KH2

29. Erratum: Corrigendum: Dissecting motility signaling through activation of specific Src-effector complexes

30. Engineered Manipulation of Signaling Networks: Control of Kinase Activation and Interactions Dissects Parallel Src Pathways

31. New Tools for Activation of Src Family Isoforms In Vivo Demonstrate Specific Roles for Each Isoform in Cell Motility

32. Enrichment of superoxide dismutase 2 in glioblastoma confers to acquisition of temozolomide resistance that is associated with tumor-initiating cell subsets

33. Purification of a Single Peptide with Vitamin K Epoxide to Vitamin K and Vitamin K to Vitamin KH2 Activity

34. Photo‐Curable Ion‐Enhanced Fluorinated Elastomers for Pressure‐Sensitive Textiles

35. Purified vitamin K epoxide reductase alone is sufficient for conversion of vitamin K epoxide to vitamin K and vitamin K to vitamin KH2.

36. Purified vitamin K epoxide reductase alone is sufficient for conversion of vitamin K epoxide to vitamin K and vitamin K to vitamin KH2.

37. Inhibition of nitric oxide production reverses diabetes-induced Kupffer cell activation and Klebsiella pneumonia liver translocation.

38. Engineering extrinsic disorder to control protein activity in living cells.

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