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      Ascending monoaminergic systems alterations in Alzheimer's disease. translating basic science into clinical care.

      Neuroscience and Biobehavioral Reviews
      Alzheimer Disease, metabolism, pathology, Brain, Dopamine, Humans, Neural Pathways, Neurons, Serotonin

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          Abstract

          Extensive neuropathological studies have established a compelling link between abnormalities in structure and function of subcortical monoaminergic (MA-ergic) systems and the pathophysiology of Alzheimer's disease (AD). The main cell populations of these systems including the locus coeruleus, the raphe nuclei, and the tuberomamillary nucleus undergo significant degeneration in AD, thereby depriving the hippocampal and cortical neurons from their critical modulatory influence. These studies have been complemented by genome wide association studies linking polymorphisms in key genes involved in the MA-ergic systems and particular behavioral abnormalities in AD. Importantly, several recent studies have shown that improvement of the MA-ergic systems can both restore cognitive function and reduce AD-related pathology in animal models of neurodegeneration. This review aims to explore the link between abnormalities in the MA-ergic systems and AD symptomatology as well as the therapeutic strategies targeting these systems. Furthermore, we will examine possible mechanisms behind basic vulnerability of MA-ergic neurons in AD. Published by Elsevier Ltd.

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          Author and article information

          Journal
          23707776
          10.1016/j.neubiorev.2013.05.008

          Chemistry
          Alzheimer Disease,metabolism,pathology,Brain,Dopamine,Humans,Neural Pathways,Neurons,Serotonin
          Chemistry
          Alzheimer Disease, metabolism, pathology, Brain, Dopamine, Humans, Neural Pathways, Neurons, Serotonin

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