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Review Harmaline Tremor: Underlying Mechanisms in a Potential Animal Model of Essential Tremor

Title: Review Harmaline Tremor: Underlying Mechanisms in a Potential Animal Model of Essential Tremor
Authors: Adrian Handforth
Contributors: The Pennsylvania State University CiteSeerX Archives
Source: http://www.tremorjournal.org/index.php/tremor/article/download/92/pdf/.
Collection: CiteSeerX
Subject Terms: Tremor; harmaline; harmine; inferior olive; cerebellum; animal model
Description: Background: Harmaline and harmine are tremorigenic b-carbolines that, on administration to experimental animals, induce an acute postural and kinetic tremor of axial and truncal musculature. This drug-induced action tremor has been proposed as a model of essential tremor. Here we review what is known about harmaline tremor. Methods: Using the terms harmaline and harmine on PubMed, we searched for papers describing the effects of these b-carbolines on mammalian tissue, animals, or humans. Results: Investigations over four decades have shown that harmaline induces rhythmic burst-firing activity in the medial and dorsal accessory inferior olivary nuclei that is transmitted via climbing fibers to Purkinje cells and to the deep cerebellar nuclei, then to brainstem and spinal cord motoneurons. The critical structures required for tremor expression are the inferior olive, climbing fibers, and the deep cerebellar nuclei; Purkinje cells are not required. Enhanced synaptic norepinephrine or blockade of ionic glutamate receptors suppresses tremor, whereas enhanced synaptic serotonin exacerbates tremor. Benzodiazepines and muscimol suppress tremor. Alcohol suppresses harmaline tremor but exacerbates harmaline-associated neural damage. Recent investigations on the mechanism of harmaline tremor have focused on the T-type calcium channel. Discussion: Like essential tremor, harmaline tremor involves the cerebellum, and classic medications for essential tremor have been found to suppress harmaline tremor, leading to utilization of the harmaline model for preclinical testing of antitremor drugs. Limitations are that the model is acute, unlike essential tremor, and
Document Type: text
Language: English
Relation: http://citeseerx.ist.psu.edu/viewdoc/summary?doi=10.1.1.678.9319; http://www.tremorjournal.org/index.php/tremor/article/download/92/pdf/
Availability: http://citeseerx.ist.psu.edu/viewdoc/summary?doi=10.1.1.678.9319; http://www.tremorjournal.org/index.php/tremor/article/download/92/pdf/
Rights: Metadata may be used without restrictions as long as the oai identifier remains attached to it.
Accession Number: edsbas.5F5625B4
Database: BASE