Excitatory postsynaptic potential
[Image:Synapse diag6.png|thumb|300px| This single EPSP does not sufficiently depolarize the membrane to generate an action potential.]
[Image:Synapse diag5.png|thumb|300px|The summation of these three EPSPs generates an action potential.]
In neuroscience, an excitatory postsynaptic potential is a postsynaptic potential that makes the postsynaptic neuron more likely to fire an action potential. This temporary depolarization of postsynaptic membrane potential, caused by the flow of positively charged ions into the postsynaptic cell, is a result of opening ligand-gated [ion channel]s. These are the opposite of inhibitory postsynaptic potentials, which usually result from the flow of negative ions into the cell or positive ions out of the cell. EPSPs can also result from a decrease in outgoing positive charges, while IPSPs are sometimes caused by an increase in positive charge outflow. The flow of ions that causes an EPSP is an excitatory postsynaptic current.
EPSPs, like IPSPs, are graded. When multiple EPSPs occur on a single patch of postsynaptic membrane, their combined effect is the sum of the individual EPSPs. Larger EPSPs result in greater membrane depolarization and thus increase the likelihood that the postsynaptic cell reaches the threshold for firing an action potential.
EPSPs in living cells are caused chemically. When an active presynaptic cell releases neurotransmitters into the synapse, some of them bind to receptors on the postsynaptic cell. Many of these receptors contain an ion channel capable of passing positively charged ions either into or out of the cell. At excitatory synapses, the ion channel typically allows sodium into the cell, generating an excitatory postsynaptic current. This depolarizing current causes an increase in membrane potential, the EPSP.
Excitatory molecules
The neurotransmitter most often associated with EPSPs is the amino acid glutamate, and is the main excitatory neurotransmitter in the central nervous system of vertebrates. Its ubiquity at excitatory synapses has led to it being called the excitatory neurotransmitter. In some invertebrates, glutamate is the main excitatory transmitter at the neuromuscular junction. In the neuromuscular junction of vertebrates, EPP are mediated by the neurotransmitter acetylcholine, which is one of the primary transmitters in the central nervous system of invertebrates.At the same time, GABA is the most common neurotransmitter associated with IPSPs in the brain.
However, classifying neurotransmitters as such is technically incorrect, as there are several other synaptic factors that help determine a neurotransmitter's excitatory or inhibitory effects.
Miniature EPSPs and quantal analysis
The release of neurotransmitter vesicles from the presynaptic cell is probabilistic. In fact, even without stimulation of the presynaptic cell, a single vesicle will occasionally be released into the synapse, generating miniature EPSPs. Bernard Katz pioneered the study of these mEPSPs at the neuromuscular junction in 1951, revealing the quantal nature of synaptic transmission. Quantal size can then be defined as the synaptic response to the release of neurotransmitter from a single vesicle, while quantal content is the number of effective vesicles released in response to a nerve impulse. Quantal analysis refers to the methods used to deduce, for a particular synapse, how many quanta of transmitter are released and what the average effect of each quantum is on the target cell, measured in terms of amount of ions flowing or change in the membrane potential.