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- A histone H4 lysine 20 methyltransferase couples environmental cues to sensory neuron control of developmental plasticity.
A histone H4 lysine 20 methyltransferase couples environmental cues to sensory neuron control of developmental plasticity.
Citation | “A Histone H4 Lysine 20 Methyltransferase Couples Environmental Cues To Sensory Neuron Control Of Developmental Plasticity.”. Development (Cambridge, England), pp. 1273-1282. . |
Center | University of Michigan |
Author | Colin E Delaney, Albert T Chen, Jacqueline Graniel V, Kathleen J Dumas, Patrick J Hu |
Keywords | C. elegans, Dauer, Dosage compensation, FoxO, H4K20, Insulin-like peptides |
Abstract |
Animals change developmental fates in response to external cues. In the nematode , unfavorable environmental conditions induce a state of diapause known as dauer by inhibiting the conserved DAF-2 insulin-like signaling (ILS) pathway through incompletely understood mechanisms. We have previously established a role for the dosage compensation protein DPY-21 in the control of dauer arrest and DAF-2 ILS. Here, we show that the histone H4 lysine 20 methyltransferase SET-4, which also influences dosage compensation, promotes dauer arrest in part by repressing the X-linked gene, which encodes a new agonist insulin-like peptide (ILP) expressed specifically in the paired ASI sensory neurons that are required for dauer bypass. repression in dauer-constitutive mutants requires DPY-21, SET-4 and the FoxO transcription factor DAF-16, which is the main target of DAF-2 ILS. By contrast, autosomal genes encoding major agonist ILPs that promote reproductive development are not repressed by DPY-21, SET-4 or DAF-16/FoxO. Our results implicate SET-4 as a sensory rheostat that reinforces developmental fates in response to environmental cues by modulating autocrine and paracrine DAF-2 ILS. |
Year of Publication |
2017
|
Journal |
Development (Cambridge, England)
|
Volume |
144
|
Issue |
7
|
Number of Pages |
1273-1282
|
Date Published |
12/2017
|
ISSN Number |
1477-9129
|
DOI |
10.1242/dev.145722
|
Alternate Journal |
Development
|
PMID |
28209779
|
PMCID |
PMC5399626
|
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