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Bi / CNS 150 Lecture 10 Synaptic inhibition; cable properties of neurons;

Bi / CNS 150 Lecture 10 Synaptic inhibition; cable properties of neurons; electrical integration in cerebellum Monday, October 19, 2015 Henry Lester. Chapter 2 (p. 22-30); Chapter 10 (223-234). The pentameric GABA A and glycine receptors look like ACh receptors;

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Bi / CNS 150 Lecture 10 Synaptic inhibition; cable properties of neurons;

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  1. Bi / CNS 150 Lecture 10 Synaptic inhibition; cable properties of neurons; electrical integration in cerebellum Monday, October 19, 2015 Henry Lester Chapter 2 (p. 22-30); Chapter 10 (223-234)

  2. The pentameric GABAA and glycine receptors look like ACh receptors; but they are permeable to anions (mostly Cl-, of course) 1. -amino-butyric acid (GABA) is the principal inhibitory transmitter in the brain. 2. Glycine is the dominant inhibitory transmitter in the spinal cord & hindbrain. GABAA receptors are more variable than glycine receptors in subunit composition and therefore in kinetic behavior. . . Cation channels become anion channels with only one amino acid change per subunit, in this approximate location Like a previous lecture

  3. Crystal structure of GABAA Receptor (Miller et al, 2014) • Homomer of 5 GABAAβ3 subunits • Overall structure similar to nicotinic receptor

  4. A Synapse “pushes” the Membrane Potential Toward the Reversal Potential (Erev) for the synaptic Channels ACh and glutamate receptors flux Na+ and K+, (and in some cases Ca2+), and Erev ~ 0 mV. At GABAA and glycine receptors, Erev is near ECl ~ -70 mV Membrane potential +80 +60 ENa +40 At Erev , the current through open receptors is zero. Positive to Erev, current flows outward Negative to Erev, current flows inward +20 -5 -20 Resting potential -50 -80 EK -100 Like Figure 10-11

  5. Pharmacology of GABAA Receptors: activators Benzodiazepines (= BZ below): Valium (diazepam), (Ambien, Lunesta are analogs) More on neuropharmacology: Bi 155, January 2017 The natural ligand binds at subunit interfeces (like ACh at ACh receptors) phenobarbital site is unceratin

  6. GABAA and Glycine blockers bind either at the agonist site or in the channel Strychnine (glycine receptor) Bicuculline (GABAA receptor Agonist site Picrotoxin (GABAA & glycine receptors)

  7. How does the receptor transduce binding into channel gating? (prev. lecture) CLOSED OPEN . . . Both ideas are also in play for GABA or glycine receptors Swivel? Miyazawa, Nature 2003 Twist? Corringer, J Physiol 2010

  8. We have Completed our Survey of Synaptic Receptors Most ^ A. ACh, Serotonin 5-HT3, GABA, (invert. GluCl, dopamine, tyrosine) receptor-channels Figure 10-7

  9. direction of information flow Postsynaptic Presynaptic neuron neuron little hill (base) (apex) Parts of two generalized CNS neurons Inhibitory terminal Excitatory terminal axon presynaptic terminal node of Ranvier initial myelin segment axon hillock cell body (soma) apical dendrites basal dendrites presynaptic terminal nucleus postsynaptic dendrite synaptic cleft Like Figure 2-1 (rotated)

  10. 10% of the neurons in the CNS are cerebellar granule cells The cerebellum: a famous circuit in neuroscience. In today’s lecture, it exemplifies pre- and postsynaptic structures. Molecular layer Purkinje cell layer Ganule cell layer White matter Figure 42-4

  11. A plurality of synapses in the CNS (> 1013 ) occur between parallel fiber axons and Purkinje cell dendritic spines Molecular layer Like Figure 42-5 500 nm

  12. Types of synapses (Don’t mind the Type I, Type II stuff) Figure 10-3

  13. Types of synaptic integration 1. Temporal A. Molecular lifetimes B. Capacitive filtering 2. Spatial 3. Excitatory-inhibitory

  14. Previous lecture all molecules begin here at t= 0 units: s-1 State 1 State 2 Synaptic integration 1A. Molecular lifetimes k21 open closed Concentration of acetylcholine at NMJ (because of acetylcholinesterase, turnover time ~ 100 μs) high 0 Number of open channels ms

  15. At the nerve-muscle synapse, acetylcholinesterase is present at densities of > 1000 / μm2 near each synapse, high enough to destroy each transmitter molecule as it leaves a receptor What causes the ~ δ-function of glutamate & GABA at CNS synapses? Na+-coupled transporters for glutamate & GABA are present at densities of > 1000 / μm2 near each synapse, probably high enough to sequester each transmitter molecule as it leaves a receptor (more on this topic, later today) Figure 4-17

  16. Synaptic Integration 1B. Capacitive filtering Figure 9-6

  17. 1B. Temporal Summation 2. Spatial summation Recording Recording Axon Axon Synaptic Current Synaptic Potential Long time constant (100 ms) Short time constant (20 ms) Synaptic Current Synaptic Potential Long length constant (1 mm) Short length constant (0.33 mm) ~ 100 pA Vm 2 mV 25 ms Vm Improved from Figure 10-14

  18. 1. If dendrites were passive, they would act like leaky cables . . . Excitatory synapses V V EPSP measured in dendrite EPSP measured in soma Gulledge & Stuart (2005) J. Neurobiol 64:75,

  19. . . . and passively integrate inputs . . . V V V Δt = 0 Δt = 0 Δt = 5 ms Prolonged rising phase Simultaneous, colocalized EPSPs (two individual trials) Nearly simultaneous, colocalized EPSPs (two individual trials) Simultaneous, Spatially distinct EPSPs Inspect the simulation, and run the movie, at http://www.neuron.yale.edu/neuron/static/about/stylmn.html Gulledge & Stuart (2005) J. Neurobiol 64:75,

  20. . . . but two-photon microscopes allow researchers to visualize patch-clamped dendrites in living animals . . . Gulledge & Stuart (2005) J. Neurobiol 64:75,

  21. 25 μm . . . dendrites are not passive. They have Na channels Now break the patch, to fill the cell with dye: immunocytochemistry * = axon hillock Averaged traces Whitaker, Brain Res, 2001 Magee & Johnston, J Physiol (1995)

  22. brain slice . . . voltage-gated Na+ and Ca2+ channels in dendrites lead to partial “backpropagation” of action potentials, implying that parts of cells can process signals semi-independently. Stay tuned! Gulledge & Stuart (2005) J. Neurobiol 64:75,

  23. Excitatory-inhibitory integration: • The “veto principle” of inhibitory transmission Inhibitory synapses work best when they are “near“ the excitatory event they will inhibit. “Near” means < one cable length. A. Inhibitory synapses on dendrites do a good job of inhibiting EPSPs on nearby spines B. Inhibitory synapses on cell bodies and initial segments do a good job of inhibiting spikes

  24. “Veto” inhibition at the axon initial segment: Schematic of a GABAergic “chandelier cell” in human cerebral cortex Inhibitory Chandelier Cell Ch terminals Ch. axon Pyramidal Cells Ch terminals from Felipe et al, Brain (1999) 122, 1807

  25. Now we localize the inhibitory “vetos” of cerebellar Purkinje cells by “pinceaux” (paintbrushes) of basket cells Molecular layer Purkinje cell layer Ganule cell layer White matter Figure 42-4

  26. How to localize and quantify inhibitory synapses NH2 A fusion protein: GABA transporter (GAT1)-GFP

  27. cerebellum

  28. <Immunocytochemistry For GABA transporter Molecular layer (basket cells stain) Purkinje cell layer “pinceux” (paintbrushes) stain heavily Granule cell layer

  29. mGAT1 GFP knock-in fluorescence > <Immunocytochemistry For GABA transporter Molecular layer (basket cells stain) Purkinje cell layer “pinceaux” stain heavily, showing soma-hillock “veto” Granule cell layer

  30. GAT1-GFP expression in cerebellum: basket cell terminals in molecular layer, Showing dendritic “veto” GABA transporter density is ~1000/(μm2) 50 mm

  31. HAL’s Office Hours, as usual Mon 1:15-2 Red Door End of Lecture 10

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