Pharmacologic Management
of Aggression and Irritability
Vernon M Neppe MD, PhD
EDUCATIONAL OBJECTIVES:
To educate in the area of aggression in the context
of anxiety and depression and to discuss the clinical
implications with regard to management options and problems.
ABSTRACT
Exploration of aggression spectrum concepts such as
anger, aggression, hostility, dyscontrol, rage, irritability
and impulsivity are compromised by the absence of an
adequate diagnostic and therapeutic classification,
the general equivalent use of these terms, their measuring
difficulties and their lack of research. Without a current
diagnostic framework for aggression in the Diagnostic
and Statistical Manual III revision or DSM-IV, there
are no FDA approved drugs for aggression.
Drugs such as carbamazepine have enormous potential
in the management of episodic disorders particularly
those linked with hostility. Preliminary research suggests
its use is particularly apposite in "Paroxysmal
Neurobehavioral Disorders" as a prototype organic
illness with epilepsy like phenomena. While this aggression
may occur incidentally in the context of anxiety and
depression, this is not necessarily more frequent than
other conditions.
Probably more important for anxiety and depression
is the frustration aggression context linked with adrenergic
and serotonergic elements.
Evidence exists for serotonin receptor involvement
in the aggression spectrum using animal models and human
clinical and post-mortem studies.
Beta-adrenergic blockers are useful but to a limited
degree because of side-effects in high doses in organic
populations. Biphasic effects are seen with the lipid
soluble propranolol - low doses probably relate to simple
alleviation of frustration, but, high doses seem to
have a central, possibly non-beta effect. Their action
may have links with serotonin 1A or 1B, and so may a
new unmarketed group, the Benzodioxines. Additionally,
lithium cation is commonly used in similar populations
for affective illness and aggression has serotonin 1A
agonist effects.
Animal models of aggression suggest the azapirones
are potent anti-aggressive agents. This should be via
components of their specific serotonin 1A partial agonist
effects. Irritability is an early target symptom of
response with buspirone in generalized anxiety disorder
possibly implying persistent low-dose effects.
Early preliminary open experience suggests a biphasic
dose effect for buspirone: Low doses of buspirone (15-25
mg per day) were effective after a few days in alleviating
irritability, anger and hostility without associated
significant anxiety in nine successive patients (p<
0.001, but many inpatients improve with milieu). Higher
doses such as 60-90 mg per day almost immediately greatly
relieved manic irritability, agitation, restlessness
and mood lability in ten subjects. This data requires
adequate controlled studies. If real, these two effects
can be explained in a unified seroton
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