A feasible strategy of limiting glutamate release could be the us

A feasible strategy of limiting glutamate release could be the use of ligands for metabotropic receptors, that could be safer than compounds directly affecting the machinery of release. AMPAkines, drugs potentiating the function of AMPA EGFR inhibitor receptors have also been in development for some time. Tianeptine, an antidepressant, that has been for some years in the market, has shown unique properties in the regulation of neuroplasticity, and this effect, seems

to be Inhibitors,research,lifescience,medical mediated by its modulation of the glutamatergic system.116-119 A novel approach to depression, regulation of circadian rhythms, has been the basis for the development, of an antidepressant, with an entirely new mechanism of action. Changes in the sleep-wake cycle and in the periodicity of circadian rhythm profoundly influence the state of mood. Sleep disturbances and depression/mood disorders are interlinked.120 Among the typical and recurring features of depressed individuals is insomnia Inhibitors,research,lifescience,medical with early-morning awakenings; indeed, disturbed sleep is one of the diagnostic criteria in Inhibitors,research,lifescience,medical DSM-IV. likewise, it has been shown that manipulations of circadian rhythms, such as total or REM sleep deprivation or phase

advance in the sleepwake cycle, may have therapeutic action in the treatment of depression.121 It is not clear whether sleep disturbances are part, of the clinical picture of depression or represent a causative factor; some studies have shown that changes in sleep architecture persist into the remission phase, while improvement in clinical state is frequently preceded by sleep changes.120,121 The first (and so far only) antidepressant in this class is agomelatine, an agonist, of MT1/MT2 melatonergic receptors

Inhibitors,research,lifescience,medical and antagonist of serotonin 5-HT2C receptor. Agomelatine was shown to induce synchronization of circadian rhythms and to be efficient in preclinical studies with different animal models of depression. ‘ITtic antidepressant efficacy of the drug in humans was positively tested in several Inhibitors,research,lifescience,medical clinical trials,122 and its regulation of the sleep-wake cycle has been proven.123,124 A recent study of long-term (10 months) treatment showed efficacy of agomelatine against placebo, while the percentage of patients mafosfamide reporting adverse effects was similar in the two groups.125 Furthermore, it presents clinical benefits such as respect of sexual function, absence of discontinuation symptoms, and no effect, on body weight.126,127 Agomelatine could be the first, antidepressant, with a really new mechanism of action to hit the market which will also achieve a better quality of remission by directly acting on the residual symptoms. Finally, among the novel compounds in development there are also a few monoamine-based putative antidepressants, namely agonists or antagonists of the most. ) recently characterized subtypes of serotonin receptors, 5-HT4, 5-HT6, and 5-HT7 (Table II) .

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