Publication | Closed Access
The ubiquitin–proteasome system and neurodegenerative disorders
44
Citations
44
References
2005
Year
ProteasomeProtein AggregatesSynaptic SignalingSocial SciencesNeurobiology Of DiseaseDegenerative PathologyProtein MisfoldingNeurologyUps DysfunctionNeuropathologyProtein DegradationProteomicsNeurogeneticsProtein Quality ControlMolecular NeuroscienceNeurodegenerationCell BiologyNeurodegenerative DiseasesUbiquitin–proteasome SystemCellular NeuroscienceDegenerative DiseaseNeuroscienceMedicine
As in all other mammalian tissues, the UPS (ubiquitin–proteasome system) is fundamental to normal brain function. A consistent feature of the major human neurodegenerative disorders is the accumulation of disease-related proteins, in non-native conformations, as protein aggregates within neurons or glial cells. Often the proteins in these aggregates are post-translationally conjugated with ubiquitin, suggesting a possible link between pathological protein-aggregation events in the nervous system and dysfunction of the UPS. Genetic evidence clearly demonstrates that disruption of ubiquitin-mediated processes can lead to neurodegeneration; however, the relationship between the UPS and idiopathic neurodegenerative disorders is less clear. In the latter cases, although a number of different mechanisms could potentially contribute to dysfunction of the UPS and promote the neurodegenerative process, whether UPS dysfunction is causally related to disease pathogenesis, or alternatively arises as a result of the pathological state, and indeed whether ubiquitinated inclusions are harmful or beneficial to cells, remains to be clarified.
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