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Titlebook: Cerebellar Degenerations: Clinical Neurobiology; Andreas Plaitakis Book 1992 Springer-Verlag US 1992 anatomy.cortex.neurobiology.neurophys

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楼主: Dangle
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Physiology of the Cerebellumthe cerebellum in the coordination of movements, and Flourens (1842) and Luciani (1891) established functional compensation as a characteristic feature of cerebellar action. Sherrington (1897), Löwenthal and Horseley (1897), Fodera (1923), and Pollock and Davis (1923) recognized inhibition as another characteristic feature of cerebellar action.
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https://doi.org/10.1007/978-3-658-35802-0ith anoxia, stroke, hypoglycemia, epilepsy, and several degenerative diseases (Huntington’s chorea, olivopontocerebellar atrophy, OPCA amyotrophic lateral sclerosis) may be at least partially produced by excessive activation of excitatory amino acid receptors [2–4].
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https://doi.org/10.1007/978-3-658-35929-4hy can be found in combination with atrophic lesions of the basal ganglia, brain stem, spinal cord, and/or cerebral cortex. Such disorders may be best categorized under ., although some authors will use this term only when they refer to disorders with coexisting progressive autonomic failure.
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Objektbasierte Programmierung mit Gosuggested that the cerebellum is involved in motor control. Such ablation techniques, along with the subsequently developed stimulation methods, have served as basic experimental tools for understanding the cerebellar physiology for almost two centuries.
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https://doi.org/10.1007/978-3-658-35724-5ble differences exist between, e.g., amphibia and mammals) is beyond any question, studies over the last 40 years make it clear that the mammalian cerebellum receives (and sends) fibers to several regions of the brain and thus is able to influence many regions and systems within the central nervous
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Participatory Forms and Formats,so been documented (see Section 5.2.1). The inhibitory interneurones, and basket, stellate, and Golgi cells also seem to operate primarily with GABA. However, it has been proposed that taurine (Tau) may be associated with some of the inhibitory cerebellar neurones (see Section 5.2.2). It seems that
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https://doi.org/10.1007/978-3-658-35802-0 [2–6] and PDHC occurring at high levels in neuronal perikarya [7]. Both regional and cellular differences in the distribution of these mitochondrial enzymes are believed partially to reflect the contrasting involvement of GDH and PDHC in the metabolism of transmitters, glutamate, and acetylcholine
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