Synapse

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This article describes in detail the chemical synapses and not electrical synapses. Chemical synapses are the ones found between axon terminals and dendrites of neurons (pre/post synaptic membranes are not in contact), whereas electrical synapses are the ones where the pre- and post-synaptic membranes are in contact and the current is passed through gap junctions (such as in cardiomyocytes).

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edit edit Electrical Synapses

The simplest way for one neuron to pass its signal to another is by direct electrical coupling through low resistance pathways of gap junctions. Such electrical synapses transmit without delay and in both directions, but the integration properties of such synapses are very limited. In nonneuronal elements the gap junction coupling is present among myocardial cells, intestinal smooth muscle cells, hepatocytes, etc.

edit edit Chemical Synapses

Chemical Synapse Overview

edit edit Structure

Chemical synapses, in contrast to electrical synapses, provide a wider spectrum of possibilities for adjustment and control of the signal transmission. The principles of chemical communication at a synapse are the same as those of chemical communication by water-soluble hormones. The proximity between the 2 ends of the synapse is main reason why the neurotransmitters released are much less diluted leading to a very effective transmission. Due to the inherent organization of the chemical synapse, conduction is one way, but with a certain delay.

When a neuron makes a chemical synapse with another neuron, the presynaptic nerve terminal characteristically broadens to form a terminal bouton. The number of these terminals range from 10000 to 200000 laying over the dendrites (80-85%) and the rest over the soma (5-20%). Areas of high electron density adjacent to the plasma membranes in the region of synaptic contact are visible in EM (symmetrical and asymmetrical synapses, Gray I and Gray II synapses).

edit edit Function

Membrane potential changes of the presynaptic terminal (e.g., action potential) cause the release of a neurotransmitter by exocytosis, due to the activation of Ca2+-VGCs. The inflowing calcium ions bind on special protein molecules on the inside surface of the membrane, called released sites, which causes them to open and release the vesicles. Each vesicle can release from 2000 to 10000 molecules of neurotransmitter. After the release, each of them is recycled and refilled with new neurotransmitter substance. For the synthesis of the neurotransmitter and its packaging into vesicles, ATP is used (which is provided by the numerous mitochondria in the vicinity of the presynaptic membrane).

The neurotransmitter diffuses across the synaptic cleft (about 50 nm) and binds to a specific membrane protein (receptor). Post-synaptic membranes have receptor proteins. These proteins have:

The termination, in other words the removal of the neurotransmitter from the receptor, can occur by at least one of the following ways:

  1. By breaking away from the receptor due to thermally-induced oscillations that originate from the neurotransmitter itself and the receptor. This will allow the enzymes (such as acetylcholinesterase) to breakdown the neurotransmitter in the synaptic cleft or be up-taken in the presynaptic membrane by a reuptake pump.
  2. Various enzymes present within the subsynaptic membrane may inactivate/metabolize the neurotransmitter.


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