Dystrophin Is Required for Appropriate Retrograde Control of Neurotransmitter Release at the Drosophila Neuromuscular Junction

doi:10.1523/JNEUROSCI.4069-05.2006

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The Journal of Neuroscience, January 4, 2006, 26(1):333-344; doi:10.1523/JNEUROSCI.4069-05.2006

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Cellular/Molecular
Dystrophin Is Required for Appropriate Retrograde Control of Neurotransmitter Release at the Drosophila Neuromuscular Junction
Mariska C. van der Plas,¹^* Gonneke S. K. Pilgram,¹^* Jaap J. Plomp,²^,3 Anja de Jong,¹ Lee G. Fradkin,¹ and Jasprina N. Noordermeer¹
¹Laboratory of Developmental Neurobiology, ²Section of Neurophysiology, Department of Molecular and Cell Biology, and ³Department of Neurology, Leiden University Medical Center, 2300 RC Leiden, The Netherlands

Mutations in the human dystrophin gene cause the Duchenne andBecker muscular dystrophies. The Dystrophin protein providesa structural link between the muscle cytoskeleton and extracellularmatrix to maintain muscle integrity. Recently, Dystrophin hasalso been found to act as a scaffold for several signaling molecules,but the roles of dystrophin-mediated signaling pathways remainunknown. To further our understanding of this aspect of thefunction of dystrophin, we have generated Drosophila mutantsthat lack the large dystrophin isoforms and analyzed their rolein synapse function at the neuromuscular junction. In expressionand rescue studies, we show that lack of the large dystrophinisoforms in the postsynaptic muscle cell leads to elevated evokedneurotransmitter release from the presynaptic apparatus. Overallsynapse size, the size of the readily releasable vesicle poolas assessed with hypertonic shock, and the number of presynapticneurotransmitter release sites (active zones) are not changedin the mutants. Short-term synaptic facilitation of evoked transmitterrelease is decreased in the mutants, suggesting that the absenceof dystrophin results in increased probability of release. Absenceof the large dystrophin isoforms does not lead to changes inmuscle cell morphology or alterations in the postsynaptic electricalresponse to spontaneously released neurotransmitter. Therefore,postsynaptic glutamate receptor function does not appear tobe affected. Our results indicate that the postsynapticallylocalized scaffolding protein Dystrophin is required for appropriatecontrol of neuromuscular synaptic homeostasis.

Key words: Dystrophin; neuromuscular junction; neurotransmitter release; Drosophila; DGC; synaptic homeostasis

Received Sep 25, 2005; revised November 8, 2005; accepted November 9, 2005.

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