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1. Metabolically driven maturation of human-induced-pluripotent-stem-cell-derived cardiac microtissues on microfluidic chips

2. Stem cell-based vascularization of microphysiological systems

3. Isochoric supercooled preservation and revival of human cardiac microtissues

4. Maladaptive Contractility of 3D Human Cardiac Microtissues to Mechanical Nonuniformity

5. A combined hiPSC-derived endothelial cell and in vitro microfluidic platform for assessing biomaterial-based angiogenesis

6. Contractile deficits in engineered cardiac microtissues as a result of MYBPC3 deficiency and mechanical overload.

7. Quantitatively characterizing drug‐induced arrhythmic contractile motions of human stem cell‐derived cardiomyocytes

8. Multivalent conjugates of basic fibroblast growth factor enhance in vitro proliferation and migration of endothelial cells

9. Generation of spatial-patterned early-developing cardiac organoids using human pluripotent stem cells

10. WAT-on-a-chip: a physiologically relevant microfluidic system incorporating white adipose tissue.

11. Multivalent hyaluronic acid bioconjugates improve sFlt-1 activity in vitro

12. Miniaturized iPS-Cell-Derived Cardiac Muscles for Physiologically Relevant Drug Response Analyses.

13. In vitro cardiac tissue models: Current status and future prospects

14. Self-organizing human cardiac microchambers mediated by geometric confinement.

15. Automated Video-Based Analysis of Contractility and Calcium Flux in Human-Induced Pluripotent Stem Cell-Derived Cardiomyocytes Cultured over Different Spatial Scales

16. Human iPSC-based cardiac microphysiological system for drug screening applications.

17. Calcium transients closely reflect prolonged action potentials in iPSC models of inherited cardiac arrhythmia.

18. Three-dimensional filamentous human diseased cardiac tissue model

19. Human induced pluripotent stem cell-based microphysiological tissue models of myocardium and liver for drug development

20. Multivalent ligands control stem cell behaviour in vitro and in vivo

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