Actin-myosin Interaction And Its Regulation - Encyclopedia Britannica

Release of acetylcholine from the nerve terminal

The vesicles cluster close to specialized regions of the nerve terminal membrane called active zones. Freeze-fracture electron microscopy reveals an orderly array of small particles (about 10 nm in diameter) within these active zones, which are believed to represent voltage-gated calcium channels. The channels are opened by depolarization (an increase in membrane potential) of the nerve terminal membrane and selectively allow the passage of calcium ions.

The nerve impulse is a wave of depolarization traveling along the axon of the motor nerve such that the resting membrane potential of about −70 millivolt is reversed, becoming briefly positive. At the nerve terminal, the nerve impulse causes voltage-gated calcium channels at the active zones to open until depolarization subsides. This allows calcium ions to enter the nerve terminal along their concentration gradient. The region of raised calcium concentration within the nerve terminal is localized close to the active zones and, by a process that is not yet understood, causes vesicles in this region to fuse with the nerve terminal membrane and to open outward (exocytosis), thereby discharging their contents into the synaptic cleft. A nerve impulse causes the release of about 50–100 vesicles of acetylcholine in humans and somewhat more in some other species.

At high rates of stimulation, sufficient to cause a smooth contraction (tetanus) of the muscle, the quantity of transmitter released per impulse declines for the first few impulses (synaptic depression), which may be due to a reduction in the number of vesicles ready for release.

Following the voltage-dependent influx of calcium into the nerve terminal, it is necessary for calcium to be removed to prevent continuous discharge of neurotransmitter. Mechanisms underlying this process are likely to involve sodium-calcium exchange across the nerve terminal membrane and possibly calcium uptake by mitochondria.

Acetylcholine is released from the nerve terminal by two other processes, independently of the nerve impulse. Neither of these processes leads to muscle contraction. The first occurs spontaneously when individual vesicles randomly fuse with the nerve terminal membrane and discharge their contents, generating a small potential change (about 0.5–1 millivolt), the miniature end plate potential. This potential is below the threshold at which an action potential is triggered in the muscle cell and thus does not lead to muscle contraction. The frequency of such events varies; in humans they occur at each end plate about once every five seconds. The second process of acetylcholine release occurs as a continuous “molecular leakage” of neurotransmitter from the nerve terminal rather than from vesicles. The overall amount released in resting muscle by this means greatly exceeds the spontaneous release of individual vesicles.

The acetylcholine molecules diffuse across the synaptic cleft and react with the acetylcholine receptors. The number of available acetylcholine binding sites greatly exceeds the number of acetylcholine molecules released. Acetylcholine is either rapidly broken down by the enzyme acetylcholinesterase, which is anchored in the basement membrane, or diffuses out of the primary cleft, thus preventing constant stimulation of acetylcholine receptors. Drugs that inactivate acetylcholinesterase and thereby prolong the presence of acetylcholine in the cleft can lead to repetitive firing of the muscle cell in response to a single nerve stimulus.