Three other DA systems have also been described49: (i) a periven

Three other DA systems have also been described49: (i) a periventricular system arising from the dorsal motor vagus nuclei, nucleus of the solitary tract, periaqueductal and periventricular gray, and projecting to midbrain structures including tegmentum, tectum, thalamus,

and hypothalamus; (ii) an olfactory bulb system Inhibitors,research,lifescience,medical arising from the periglomerular cells in the olfactory bulb; and (iii) an incertohypothalamic circuit from the zona incerta to the hypothalamus. DA exerts effects at DA receptors, of which several subtypes have been identified, and, Inhibitors,research,lifescience,medical similarly to 5-HT and NE, DA is taken up into the presynaptic terminal via a DA Tenatoprazole? transporter (DAT). Interestingly, DA nerve terminals in the

prefrontal cortex of humans and other primates contain no DAT, and the DA signal is inactivated by uptake into nearby NE nerve terminals by NET For this reason, NE reuptake inhibitors increase DA availability in the Inhibitors,research,lifescience,medical prefrontal cortex. Along with 5-HT and NE, DA is catabolized by MAO. DA is a precursor for NE, but its role in depression has been far less scrutinized. CSF concentrations of the major metabolite of DA-homovanillic acid (HVA) – are decreased in depressed patients,50,51 and urine levels of 3,4-dihydroxyphenylacetic acid (DOPAC; another metabolite of DA) have been shown to be decreased in depressed patients52 and potentially Inhibitors,research,lifescience,medical associated with suicidal behavior.50 There is evidence from both brain imaging Inhibitors,research,lifescience,medical studies of the DAT53 and postmortem studies54 that DA neurons are

reduced in activity in depression. Depression is highly comorbid with Parkinson’s disease, which is characterized by loss of DA Brefeldin_A cells in the substantia nigra and VTA; however, it should be noted that 5-HT and NE systems are also disrupted in Parkinson’s disease.55-57 Monoamine oxidase inhibitors (MAOIs), which have demonstrated efficacy in treating depression, decrease catabolism of all monoamines including DA. Certain medications that primarily affect the DA system, such as psychostimulants and pramipexole, also have antidepressant efficacy,58-60 particularly in bipolar depression. Future directions for monoamine systems research The monoamine deficiency hypothesis of depression has remained dominant for many years.

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