Cellular Bioelectricity

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ELEC ENG 3BB3: Cellular Bioelectricity Notes for Lecture 22 Friday, February 28, 2014

10. THE NEUROMUSCULAR JUNCTION We will look at: Structure of the neuromuscular junction Evidence for the quantal nature of transmitter release Poisson statistics for transmitter release The effect of Ca ++ and Mg ++ on transmitter release Post-junctional response to transmitter 2

Structure of the neuromuscular junction: Studying the structure and function of the neuromuscular junction is useful for understanding: some general principles of chemical synapses, and the specifics of skeletal muscle activation. 3

Structure of the neuromuscular junction (cont.): Motor nerve axons are normally myelinated, except at their terminals where they branch and synapse onto muscle fibers. The set of muscle fibers activated by a single motor neuron is known as a motor unit. 4

Structure of the neuromuscular junction (cont.): The nerve terminal contacts the muscle fiber at an end plate. The pre- and post-synaptic membranes form a specialized gutter. 5

Structure of the neuromuscular junction (cont.): The pre- and post-synaptic membrane formations are similar to nerve-to-nerve chemical synapses, except for the synaptic gutter. 6

Structure of the neuromuscular junction (cont.): Muscle fiber end-plate potentials (EPPs) are equivalent to excitatory postsynaptic potentials (EPSPs) in neurons note that they are always excitatory. 7

Structure of the neuromuscular junction (cont.): The neuromuscular junction transmitter is acetylcholine (ACh). A model of the ACh receptor is shown to the right. Channel opening requires binding of ACh with both α subunits. 8

Evidence for the quantal nature of transmitter release: In the absence of stimulation of the presynaptic nerve, miniature end-plate potentials (MEPPs) of around 0.5 mv are observed. EPPs produced by presynaptic nerve stimulation always have amplitudes that are integer multiples of the MEPP amplitude ) transmitter release is quantal 9

Poisson statistics for transmitter release: Suppose there are n presynaptic release sites and that the probability of release at any site is p, where p depends on the presynaptic transmembrane potential and the concentration of Ca ++, Mg ++ and other ions. The probability of exactly x of n releases is given by the binomial distribution: where q = 1 p. 10

Poisson statistics for transmitter release (cont.): In the case where n! 1, p 1 and x n, then the binomial distribution is well approximated by the Poisson distribution: where m = np is the mean release rate. Note that the variance in the number of events (e.g., synaptic releases) for a Poisson process is equal to the mean. 11

The effect of Ca ++ and Mg ++ on transmitter release: Decreasing the concentration of extracellular Ca ++ or elevating the concentration of Mg ++ has the effect of reducing p. The reason is that the pre-junctional nerve terminal has many voltage-gated Ca ++ channels, which facililates Ca ++ entry near the ACh release sites. It is actually binding of intracellular Ca ++ to proteins in the release site that triggers exocytosis and neurotransmitter release. Mg ++ can block the Ca ++ channel, which reduces neurotransmitter release. 12

Post-junctional response to transmitter: The postsynaptic membrane has an ACh receptor density of around 10 4 /µm 2, which is an order of magnitude greater than the density of sodium and potassium channels in squid axon. To simulate the effects of transmitter binding to the post-synaptic receptor, a parallelconductance model can be created where a mixed potassium, sodium and chloride channel is opened when ACh binds to the receptor. 13

Post-junctional response to transmitter (cont.): For the frog neuromuscular junction: g Cl ¼ 0 g Na /g K ¼ 1.29 14

Post-junctional response to transmitter (cont.): The synaptic membrane model can be simplified to a single ionic current with conductance g s and reversal potential E s. Since E s > E r, the synapse is excitatory. 15

11. SKELETAL MUSCLE We will look at: Muscle structure Excitation-contraction EMG measurement and interpretation 16

Skeletal Muscles

3.2 Muscle biomechanics Organization: skeletal muscle is made up of muscle fibers each fiber is a single cell the contraction of a fiber is achieved by the motor proteins actin & myosin (from Guyton and Hall, 10 th Edition)

Muscle structure: skeletal muscle is made up of muscle fibers each fiber is a single cell the contraction of a fiber is achieved by the motor proteins actin & myosin which form fibrils 19

Muscle structure (cont.): Each fibril is surrounded by: a sarcoplasmic reticulum (SR), which stores Ca 2+ for triggering muscle fiber contraction, and the transverse tubules system (TTS), which ensures that action potentials propagate deep into the fiber. 20

Excitation-contraction: Steps in muscle fiber contraction 1. Motor neuron action potential 2. Action potential propagation along motor axon (myelinated fiber) 3. Transmission of acetylcholine (ACh) at neuromuscular junctions (synapses) 4. Action potential generation in muscle fiber 5. Release of Ca 2+ from sarcoplasmic reticulum initiates attractive forces between actin & myosin filaments, causing them to slide alongside each other ) muscle contraction 6. Return of Ca 2+ to sarcoplasmic reticulum, ending muscle contraction 21

Excitation-contraction (cont.): The TTS and SR are crucial for synchronized contraction of all fibrils in skeletal myocytes and mammalian cardiac myocytes. (Song et al., Ann. N.Y. Acad. Sci. 2005). 22

Excitation-contraction (cont.): Organization of key channel and transporter proteins and SR structures, including the junctional SR (JSR), near the TT (Song et al., Ann. N.Y. Acad. Sci. 2005). 23

Excitation-contraction (cont.): The release of Ca 2+ to trigger contraction of fibrils is facilitated by two different types of Ca 2+ channels: 1. dihydropyridine receptors (DHPRs) or L- type Ca 2+ channels, and 2. ryanodine receptors (RyRs). 24

Excitation-contraction (cont.): L-type Ca 2+ channels are voltage-gated and appear on the TT and sarcolemmal (SL) membrane. These are opened by Na + action potentials, allowing Ca 2+ to flow into the intracellular space near the JSR. Reception of Ca 2+ by RyRs opens up Ca 2+ channels in the JSR membrane allowing release of Ca 2+ from the SR. This leads to a positive feedback loop of Ca 2+ release, triggering fibril contraction. 25

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