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1. Optimized Sawhorse Waveform for the Measurement of Oxytocin Release in Zebrafish.

2. Regenerated interneurons integrate into locomotor circuitry following spinal cord injury.

3. Hypothalamic Dopamine Neurons Control Sensorimotor Behavior by Modulating Brainstem Premotor Nuclei in Zebrafish.

4. Zebrafish oxytocin neurons drive nocifensive behavior via brainstem premotor targets.

5. The Midline Axon Crossing Decision Is Regulated through an Activity-Dependent Mechanism by the NMDA Receptor.

6. Gaze-Stabilizing Central Vestibular Neurons Project Asymmetrically to Extraocular Motoneuron Pools.

7. Motor Behavior Mediated by Continuously Generated Dopaminergic Neurons in the Zebrafish Hypothalamus Recovers after Cell Ablation.

8. Transgenic FingRs for Live Mapping of Synaptic Dynamics in Genetically-Defined Neurons.

9. Hypothalamic radial glia function as self-renewing neural progenitors in the absence of Wnt/β-catenin signaling.

10. Specialized insulin is used for chemical warfare by fish-hunting cone snails.

11. Simultaneous mapping of membrane voltage and calcium in zebrafish heart in vivo reveals chamber-specific developmental transitions in ionic currents.

12. Bright and fast multicoloured voltage reporters via electrochromic FRET.

13. Optical recording of action potentials in mammalian neurons using a microbial rhodopsin.

14. Electrical spiking in Escherichia coli probed with a fluorescent voltage-indicating protein.

15. The coreceptor CD2 uses plasma membrane microdomains to transduce signals in T cells.

16. Escape behavior elicited by single, channelrhodopsin-2-evoked spikes in zebrafish somatosensory neurons.

17. Single-molecule imaging of fluorescent proteins.

18. Mechanisms for segregating T cell receptor and adhesion molecules during immunological synapse formation in Jurkat T cells.

19. Making microtubules and mitotic spindles in cells without functional centrosomes.

20. Selected line difference in sensitivity to a GABAergic neurosteroid during ethanol withdrawal.

21. Single-molecule microscopy reveals plasma membrane microdomains created by protein-protein networks that exclude or trap signaling molecules in T cells.

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