Literature DB >> 18715893

Dendrite elongation and dendritic branching are affected separately by different forms of intrinsic motoneuron excitability.

Carsten Duch1, Fernando Vonhoff, Stefanie Ryglewski.   

Abstract

Dendrites are the fundamental determinant of neuronal wiring. Consequently dendritic defects are associated with numerous neurological diseases and mental retardation. Neuronal activity can have profound effects on dendritic structure, but the mechanisms controlling distinct aspects of dendritic architecture are not fully understood. We use the Drosophila genetic model system to test the effects of altered intrinsic excitability on postembryonic dendritic architecture development. Targeted dominant negative knock-downs of potassium channel subunits allow for selectively increasing the intrinsic excitability of a selected subset of motoneurons, whereas targeted expression of a genetically modified noninactivating potassium channel decrease intrinsic excitability in vivo. Both manipulations cause significant dendritic overgrowth, but by different mechanisms. Increased excitability causes increased dendritic branch formation, whereas decreased excitability causes increased dendritic branch elongation. Therefore dendritic branching and branch elongation are controlled by separate mechanisms that can be addressed selectively in vivo by different manipulations of neuronal intrinsic excitability.

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Year:  2008        PMID: 18715893     DOI: 10.1152/jn.90758.2008

Source DB:  PubMed          Journal:  J Neurophysiol        ISSN: 0022-3077            Impact factor:   2.714


  30 in total

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5.  Dendrites are dispensable for basic motoneuron function but essential for fine tuning of behavior.

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6.  Relating ion channel expression, bifurcation structure, and diverse firing patterns in a model of an identified motor neuron.

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7.  Tiling among stereotyped dendritic branches in an identified Drosophila motoneuron.

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8.  MECP2 impairs neuronal structure by regulating KIBRA.

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