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Glial-derived prodegenerative signaling in the Drosophila neuromuscular system.


ABSTRACT: We provide evidence for a prodegenerative, glial-derived signaling framework in the Drosophila neuromuscular system that includes caspase and mitochondria-dependent signaling. We demonstrate that Drosophila TNF-? (eiger) is expressed in a subset of peripheral glia, and the TNF-? receptor (TNFR), Wengen, is expressed in motoneurons. NMJ degeneration caused by disruption of the spectrin/ankyrin skeleton is suppressed by an eiger mutation or by eiger knockdown within a subset of peripheral glia. Loss of wengen in motoneurons causes a similar suppression providing evidence for glial-derived prodegenerative TNF-? signaling. Neither JNK nor NF?? is required for prodegenerative signaling. However, we provide evidence for the involvement of both an initiator and effector caspase, Dronc and Dcp-1, and mitochondrial-dependent signaling. Mutations that deplete the axon and nerve terminal of mitochondria suppress degeneration as do mutations in Drosophila Bcl-2 (debcl), a mitochondria-associated protein, and Apaf-1 (dark), which links mitochondrial signaling with caspase activity in other systems.

SUBMITTER: Keller LC 

PROVIDER: S-EPMC3313621 | biostudies-literature | 2011 Dec

REPOSITORIES: biostudies-literature

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Glial-derived prodegenerative signaling in the Drosophila neuromuscular system.

Keller Lani C LC   Cheng Ling L   Locke Cody J CJ   Müller Martin M   Fetter Richard D RD   Davis Graeme W GW  

Neuron 20111201 5


We provide evidence for a prodegenerative, glial-derived signaling framework in the Drosophila neuromuscular system that includes caspase and mitochondria-dependent signaling. We demonstrate that Drosophila TNF-α (eiger) is expressed in a subset of peripheral glia, and the TNF-α receptor (TNFR), Wengen, is expressed in motoneurons. NMJ degeneration caused by disruption of the spectrin/ankyrin skeleton is suppressed by an eiger mutation or by eiger knockdown within a subset of peripheral glia. Lo  ...[more]

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