The Nervous System 195Glycine is a neurotransmitter in the spinal cord, brain stem,
and retina, whereas GABA is more widespread in the CNS.
In the spinal cord, GABA and glycine have important roles in
both sensory and motor transmission. However, glycine is par-
ticularly important in the spinal control of skeletal movements
(chapter 12; see figs. 12.29 and 12.30). Flexion of an arm, for
example, involves stimulation of the flexor muscles by motor
neurons in the spinal cord. The motor neurons that innervate
the antagonistic extensor muscles are inhibited by IPSPs pro-
duced by glycine released from other neurons. The importance
of the inhibitory actions of glycine is revealed by the deadly
effects of strychnine, a poison that causes spastic paralysis by
specifically blocking the glycine receptor proteins. Animals
poisoned with strychnine die from asphyxiation because they
are unable to relax the diaphragm.
GABA is the most prevalent neurotransmitter in the
brain; in fact, as many as one-third of all the neurons in the
brain use GABA as a neurotransmitter. Like glycine, GABA
is inhibitory—it hyperpolarizes the postsynaptic membrane
by opening Cl^2 channels. Also, the effects of GABA, like
those of glycine, are involved in motor control. For example,
large neurons called Purkinje cells mediate the motor func-
tions of the cerebellum by producing IPSPs in their post-
synaptic neurons. A deficiency of GABA-releasing neurons
is responsible for uncontrolled movements in people with
Huntington’s disease. Huntington’s disease is a neurodegen-
erative disorder caused by a defect in the huntingtin gene
(chapter 3, section 3.4).exit of K^1 ) through NMDA channels in the dendrites of the
postsynaptic neuron.
Inhibitory Neurotransmitters
There are two inhibitory neurotransmitters in the CNS: GABA
( gamma-aminobutyric acid ), a derivative of glutamic acid,
and glycine. The glycine and GABA receptors are ligand-gated
ion channels that, like the nicotinic ACh receptor, open when
the receptor binds to its neurotransmitter ligand. When GABA
and glycine bind to their respective receptors, they open chan-
nels for Cl^2 that hyperpolarize the postsynaptic membrane and
produce an IPSP ( fig. 7.32 ).
Because active transport carriers keep the concentration of
Cl^2 lower inside than outside of mature neurons, Cl^2 will dif-
fuse into the postsynaptic neuron. This is true as long as the post-
synaptic membrane potential is less negative (more depolarized)
than the chloride equilibrium potential (chapter 6, section 6.4).
This may not be the case at rest, because the chloride equilib-
rium potential may be close to the resting membrane potential.
However, if an excitatory neurotransmitter partially depolarizes
the membrane, the movement of Cl^2 through its open chan-
nels is promoted. When this occurs, the hyperpolarizing effects
of Cl^2 entering the cell make it more difficult for the postsyn-
aptic neuron to reach the threshold depolarization required to
stimulate action potentials. Thus, the opening of Cl^2 channels
by an inhibitory neurotransmitter renders excitatory input less
effective.
Figure 7.32 GABA receptors contain a chloride channel. When GABA (gamma-aminobutyric acid) binds to its receptor, a
chloride ion (Cl^2 ) channel opens through the receptor. This permits the inward diffusion of Cl^2 , resulting in hyperpolarization, or
an IPSP.
- Channel closed
until receptor binds
to GABA - Channel closed
until receptor binds
to GABA
3. Diffusion of Cl–^
into cell causes
hyperpolarization (IPSP)
2. GABA receptor
binds to GABA, Cl–
channel opens
GABAGABA
Channel receptors
closedPlasma
membraneChloride ion (Cl–)