1. The document summarizes different levels of organization in the nervous system from behavior and cognition down to molecules. It covers the structure and functions of neurons, glia, and the cell membrane.
2. Key aspects of neurons include the soma, dendrites, axon, synapses, and ion channels. Glia include ependymal cells, microglia, oligodendrocytes, astrocytes, and Schwann cells which support neuronal function.
3. The cell membrane maintains ion concentration gradients through ion pumps and channels. Its voltage-dependent properties allow for the propagation of action potentials along axons.
1. The document summarizes different levels of organization in the nervous system from behavior and cognition down to molecules. It covers the structure and functions of neurons, glia, and the cell membrane.
2. Key aspects of neurons include the soma, dendrites, axon, synapses, and ion channels. Glia include ependymal cells, microglia, oligodendrocytes, astrocytes, and Schwann cells which support neuronal function.
3. The cell membrane maintains ion concentration gradients through ion pumps and channels. Its voltage-dependent properties allow for the propagation of action potentials along axons.
1. The document summarizes different levels of organization in the nervous system from behavior and cognition down to molecules. It covers the structure and functions of neurons, glia, and the cell membrane.
2. Key aspects of neurons include the soma, dendrites, axon, synapses, and ion channels. Glia include ependymal cells, microglia, oligodendrocytes, astrocytes, and Schwann cells which support neuronal function.
3. The cell membrane maintains ion concentration gradients through ion pumps and channels. Its voltage-dependent properties allow for the propagation of action potentials along axons.
1. The document summarizes different levels of organization in the nervous system from behavior and cognition down to molecules. It covers the structure and functions of neurons, glia, and the cell membrane.
2. Key aspects of neurons include the soma, dendrites, axon, synapses, and ion channels. Glia include ependymal cells, microglia, oligodendrocytes, astrocytes, and Schwann cells which support neuronal function.
3. The cell membrane maintains ion concentration gradients through ion pumps and channels. Its voltage-dependent properties allow for the propagation of action potentials along axons.
Behavior and Cognition: interactions between the brain, body, and external world CNS: gross anatomy; the organization of the neural pathways, comparative neuroscience, coordination of activity across entire CNS Systems: multiple connected regions work together to support a single common function Maps: individual brain regions with consistent responses to Intracellular transport: along microtubule stimuli in the external environment; specific types of information • Retrograde: towards soma; dynein & dynactin processing • Anterograde: towards axon; kinesin Circuits/Networks: coordination of activity in small groups of connected neurons; demonstrates intricate connectivity within brain Neurons: morphology of single neuron affects how it processes electrochemical signals Synapses: site of electrochemical interactions between neurons Molecules: mediate neuronal changes and development and signal transmission
Connectivity: brain region
• Principal/projection neuron: axons extend to one or more distant brain regions • Interneuron: axons and dendrites remain in single local brain region Structure: unipolar, bipolar, multipolar Physiological responses: frequency & threshold of firing Genetic & Neurotransmitter: ion channels, receptors, etc.
II. Soma III. Glia
Nissl stain: rough endoplasmic reticulum Gap junctions: direct connection of cytosol between two cells via Golgi stain: entire neuron ion channels Microtubule Associated Protein (MAP) tau: stains soma, dendrites, and axon red; MAP2 stains soma and dendrites 1. Ependymal cells: produces cerebral-spinal fluid (CSF) only green • Choroid plexus: lining made of ependymal cells found in ventricles and canal of spinal cord Reticular theory: nervous system is continuous • Tight junctions form blood-CSF barrier Neuron doctrine: neurites end freely in nervous system; • CSF cushions skull & circulates nutrients & waste communication through contact (contiguous) exchanged with cells and blood Law of dynamic polarization: propagation of nerve impulses is 2. Microglia: processes extend from soma; secretes immune unidirectional, towards dendrites and soma and away from axon response molecules and engulf damaged tissues in response to injury (ATP-sufficient); removal of neurites (pruning for Protein synthesis: 2º alpha helix & beta sheet, 3º polypeptide adaptation to changing environment) or entire neurons subunit folds due to residue group interactions; exon, intron, 3. Myelin sheath: spiral wrapping that insulates axon promoter: DNA à mRNA • Oligodendrocytes: can wrap axons from multiple neurons in Ribosomes: proteins synthesized by free ribosomes remain in CNS cells; for insertion in cell membrane or out of cell if synthesized • Schwann cells: wrap only one axon in PNS by ribosomes on rough ER 4. Astrocytes: communicate via gap junctions Smooth endoplasmic reticulum: protein folding, regulation of • Blood-brain barrier: formed by endothelial cells of Ca2+ capillaries, pericytes, and astrocytes that limits permeability Golgi apparatus: modifies post-translational proteins to of substances from bloodstream to brain determine their final destinations o Astrocytes’ end-feet wrap around capillaries Cytoskeleton: microtubule (tubulin), neurofilament, • Tripartite synapse: astrocytes surround pre-/postsynaptic microfilament (actin) neuron o Segregate neighboring neuron spatially via isolation of chemical release Axon collaterals: branches along axon o Increase in Ca2+ in microdomains (which can eventually Axon terminal: abundance of ATP, no microtubules spread further) in response to NT release due to NT Dendritic spines: highly specialized protrusions influence receptors dendritic strength o Neurotransmitter reuptake & gliotransmitter release that affects transmission o Release factors that can influence the development (e.g. • Ligand-gated/ionotropic receptor: neurotransmitter binding silent synapses) or modification of synapses (including to protein removal by microglia, increasing NT receptors); can • Voltage-gated: membrane potential threshold; may require influence transmission without initiating structural NT changes (e.g. higher NT release) • Phagocytosis: direct (silent synapses) and indirect (signals Investigating selective permeability: microglia) • Chemical: toxins selectively block specific ion channels • Genetic: mutations affect protein structure • Electrophysiological: changes in voltage across cell membrane • X-ray crystallography: maps out amino acids necessary
Na+/K+ pump: uses ATP to create concentration gradient; 3 Na+
out and 2 K+ in Ca2+ pump: Ca2+ binds to Plasma Membrane Ca2+ ATP-ase, which uses ATP to throw Ca2+ out of cell Na+/Ca2+ exchanger: uses energy produced by 3 Na+ flowing down [Na+] gradient into cell to pump 1 Ca2+ out of cell
IV. Membrane Potential
Ohm’s Law: I = gV = V/R Capacitor: stores electrical energy • Membrane acts like a capacitor: intracellular cations are attracted to extracellular anions due to potential difference, but there is no open channel (net difference occur at surfaces) Depolarization: decrease in potential difference across membrane; Vm becomes less negative Hyperkalemia: too high [K+]o which cause muscle weakness and irregular heartbeat; high [K+]o leads to depolarization, lowering ion driving force of Na+ K+ spatial buffering: high [K+]o flows through K+ channels on astrocytes, which release to other microdomains with less [K+]o • Blood-brain barrier limits [K+] flow into serum
Equilibrium potential: electric potential difference that exactly
counterbalances ion concentration gradient when membrane is permeable to only one single ion Ion driving force: difference between actual membrane potential and Eion drives Vm towards Eion once the membrane is permeable to the ion; magnitude of force proportional to magnitude of the difference !" !"# ! Nernst Equation: 𝐸!"# = ln ( ) !" !"# ! !" !!"! !"! ! !!!! ! ! ! Goldman-Hodgkin-Katz: 𝑉! !"#$ = ln ( ) ! !!"! !"! ! !!!! ! ! ! • PK = 40PNa at resting potential
Transmembrane ion channel: different properties of R-groups
and size of pore formed by polypeptide subunits determine ion channels’ permeability to selective ions; hydrophobic parts keep channel suspended in membrane; 4-6 subunits • If mutation happens: R-groups affect 3º structure due to hydrophobic/hydrophilic interactions with other amino acids on the same polypeptide chain à structure of polypeptide subunits is changed à shape of pore no longer fits ion à channel is no longer permeable to that ion Ion channel gating: selective opening and closing