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1. Optogenetics enables real-time spatiotemporal control over spiral wave dynamics in an excitable cardiac system

2. Paradoxical Onset of Arrhythmic Waves from Depolarized Areas in Cardiac Tissue Due to Curvature-Dependent Instability

3. The Effects of Repetitive Use and Pathological Remodeling on Channelrhodopsin Function in Cardiomyocytes

4. 'Trapped reentry' as a dormant source of acute focal arrhythmia and fractionated atrial electrograms under sinus rhythm

5. 1275First evidence of 'trapped reentry' as dormant source of acute atrial fibrillation and fractionated atrial electrograms under sinus rhythm

6. Dynamic Loading of Human Engineered Heart Tissue Enhances Contractile Function and Drives Desmosome-linked Disease Phenotype

8. Optogenetics enables real-time spatiotemporal control over spiral wave dynamics in an excitable cardiac system

9. Response by Feola et al to Letter Regarding Article, 'Localized Optogenetic Targeting of Rotors in Atrial Cardiomyocyte Monolayers'

10. Paradoxical onset of arrhythmic waves from depolarized areas in cardiac tissue due to curvature-dependent instability

11. Localized Optogenetic Targeting of Rotors in Atrial Cardiomyocyte Monolayers

12. Excitation wave propagation in a patterned multidomain cardiac tissue

13. Optogenetic manipulation of anatomical re-entry by light-guided generation of a reversible local conduction block

14. Optogenetic Engineering of Atrial Cardiomyocytes

15. Functional analysis of the engineered cardiac tissue grown on recombinant spidroin fiber meshes

17. Arrhythmogenic role of the border between two areas of cardiac cell alignment

18. 29-02: Optogenetic termination of anatomical reentry in rat myocardial slices

20. Dynamic loading of human engineered heart tissue enhances contractile function and drives a desmosome-linked disease phenotype

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