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Developmental decline in neuronal regeneration by the progressive change of two intrinsic timers.


ABSTRACT: Like mammalian neurons, Caenorhabditis elegans neurons lose axon regeneration ability as they age, but it is not known why. Here, we report that let-7 contributes to a developmental decline in anterior ventral microtubule (AVM) axon regeneration. In older AVM axons, let-7 inhibits regeneration by down-regulating LIN-41, an important AVM axon regeneration-promoting factor. Whereas let-7 inhibits lin-41 expression in older neurons through the lin-41 3' untranslated region, lin-41 inhibits let-7 expression in younger neurons through Argonaute ALG-1. This reciprocal inhibition ensures that axon regeneration is inhibited only in older neurons. These findings show that a let-7-lin-41 regulatory circuit, which was previously shown to control timing of events in mitotic stem cell lineages, is reutilized in postmitotic neurons to control postdifferentiation events.

SUBMITTER: Zou Y 

PROVIDER: S-EPMC4074024 | biostudies-literature | 2013 Apr

REPOSITORIES: biostudies-literature

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Developmental decline in neuronal regeneration by the progressive change of two intrinsic timers.

Zou Yan Y   Chiu Hui H   Zinovyeva Anna A   Ambros Victor V   Chuang Chiou-Fen CF   Chang Chieh C  

Science (New York, N.Y.) 20130401 6130


Like mammalian neurons, Caenorhabditis elegans neurons lose axon regeneration ability as they age, but it is not known why. Here, we report that let-7 contributes to a developmental decline in anterior ventral microtubule (AVM) axon regeneration. In older AVM axons, let-7 inhibits regeneration by down-regulating LIN-41, an important AVM axon regeneration-promoting factor. Whereas let-7 inhibits lin-41 expression in older neurons through the lin-41 3' untranslated region, lin-41 inhibits let-7 ex  ...[more]

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