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Biogenic amine theory of depression

Strong support for the biogenic amine theory of depression is provided by the powerful antidepressant effect of inhibitors of monoamine oxidase. An example is pargyline (Fig. 30-33), which forms a covalent... [Pg.1809]

This data, coupled with numerous positive outcome studies of the effectiveness of antidepressants, has led to the development of the monoamine (or biogenic amine) hypothesis of depression. The theory holds that depressive symptoms are ushered in by a malfunction of either norepinephrine (NE) or serotonin (5-HT) neurons, which play critical roles in the functioning of the limbic system and the adjacent hypothalamus. The basic neuronal malfunction is felt to be identical for either NE or 5-HT neurons, thus what follows (a description of the pathophysiology of NE neurons) can also be seen to occur in individuals in whom 5-HT neurons are affected. For reasons that are not well understood, patients with major depression (with vegetative symptoms) appear to suffer from either NE or 5-HT dysfunction, but probably not both simultaneously (although some exceptions exist). [Pg.69]


See other pages where Biogenic amine theory of depression is mentioned: [Pg.219]    [Pg.220]    [Pg.219]    [Pg.220]    [Pg.219]    [Pg.220]    [Pg.219]    [Pg.220]    [Pg.130]    [Pg.414]    [Pg.36]   
See also in sourсe #XX -- [ Pg.220 , Pg.221 , Pg.222 ]

See also in sourсe #XX -- [ Pg.220 , Pg.221 , Pg.222 ]




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