Agmatine: an endogenous ligand at
imidazoline receptors is a novel
neurotransmitter
by
Reis DJ, Regunathan S
Division of Neurobiology,
Cornell University Medical College,
New York, New
York 10021, USA.
djreis@mail.med.cornell.edu
Ann N Y Acad Sci 1999 Jun 21; 881:65-80
ABSTRACT
Agmatine, an amine and organic cation, is an endogenous ligand at alpha
2-adrenergic and imidazoline (I-) receptors, to which it binds with high
affinity. In addition, agmatine has properties of an endogenous
neurotransmitter. Thus, agmatine (a) is locally synthesized in brain by a
specific enzyme, arginine decarboxylase; (b) is stored in a large number of
neurons with selective distribution in the CNS; (c) is associated with small
vesicles in axon terminals that, at least in hippocampus, make synaptic
asymmetric (excitatory) synapses on pyramidal cells; (d) is released from
synaptosomes in a Ca(2+)-dependent manner; (e) can be enzymatically degraded by
agmatinase in synaptosomes; (f) can be inactivated by selective reuptake; (g)
blocks the ligand-gated NMDA receptor channel at sites distinct from
ligand-binding and polyamine sites; and (h) has systemic actions when
administered intraventricularly. Additionally, (i) agmatine is a precursor of
brain putrescine and, hence, of higher polyamines, and (j) it competitively
inhibits the activity of all isozymes of nitric oxide synthase. Agmatine meets
most criteria to establish it as a novel neurotransmitter/neuromodulator in the
CNS. However, agmatine differs from forms of clonidine displacing system with
respect to distribution, bioactivity, and capacity to interact with antibodies
raised to imidazoline-like drugs. Thus, there are multiple endogenous ligands of
the imidazoline receptors, one of which is agmatine.
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