Pharmacology of appetite suppression
by
Halford JC, Blundell JE
Department of Psychology,
Eleanor Rathbone Building,
University of Liverpool, UK.
Prog Drug Res 2000; 54:25-58
ABSTRACT
Despite a rising worldwide epidemic of obesity there
is currently only a very small number of anti-obesity drugs available to
manage the problem. Large numbers of differing pharmacological agents reliably
produce a reduction in food intake when administered acutely to animals,
and when administered chronically they result in a significant decrease
in body mass. Behavioural analysis of drug-induced anorexia in animals demonstrates
that various compounds profoundly effect feeding behaviour in differing
ways. This indicates the variety of mechanisms by which pharmacological
agents can induce changes in food intake, body weight and eventually body
composition. Some of the same drugs produce decreases in food intake and
weight loss in humans. Some of these drugs do so by modifying the functioning
of the appetite system as measured by subjective changes in feelings of
hunger and fullness (indices of satiety). Such drugs can be considered as
"appetite suppressants" with clinical potential as anti-obesity agents.
Other drugs induce changes in food intake and body weight through various
physiological mechanisms inducing feelings of nausea or even by side effect
related malaise. Of the drugs considered suitable candidates for appetite
suppressants are agents which act via peripherally satiety peptide systems
(such as CCK, Bombesin/GRP, Enterostatin and GLP-1), or alter the CNS levels
of various hypothalamic neuropeptides (NPY, Galanin, Orexin and Melanocortins)
or levels of the key CNS appetite monoamine neurotransmitters such as serotonin
(5-HT) and noradrenaline (NA). Recently, the hormone leptin has been regarded
as a hormonal signal linking adipose tissue status with a number of key
central nervous system circuits. The peptide itself stimulates leptin receptors
and it links with POMC and MC-4 receptors. These receptors may also provide
drug targets for the control of appetite. Any changes induced by a potential
appetite suppressant should be considered in terms of the (i) psychological
experience and behavioural expression of appetite, (ii) metabolism and peripheral
physiology, and (iii) functioning of CNS neural pathways. In humans, modulation
of appetite may involve changes in total caloric consumption, subjective
changes in feelings of hunger and fullness, preferences for specific food
items, and general macronutrient preferences. These may be expressed behaviourally
as changes in meal patterns, snacking behaviour and food choice. Within
the next 20 years it is certain that clinicians will have a new range of
anti-obesity compounds available to choose from. Such novel compounds may
act on a single component of the appetite system or target a combination
of these components detailed in this review. Such compounds used in combination
with lifestyle changes and dietary intervention may be useful in dealing
with the rising world epidemic of obesity.
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Ephedra and the FDA
Drugs to treat obesity
Appetite suppressants
Phendimetrazine (Bontril, Obex)
Refs
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