Neuropeptide and serotonin co-transmission sets the activity pattern in the C. elegans egg-laying circuit

生物 血清素 神经肽 传输(电信) 秀丽隐杆线虫 动物 神经肽Y受体 解剖 细胞生物学 遗传学 受体 基因 电气工程 工程类
作者
Allison Butt,Sara Van Damme,Emerson Santiago,Andrew Olson,Isabel Beets,Michael R. Koelle
出处
期刊:Current Biology [Elsevier BV]
卷期号:34 (20): 4704-4714.e5 被引量:1
标识
DOI:10.1016/j.cub.2024.07.064
摘要

Highlights•C. elegans HSNs release NLP-3 peptides and serotonin to activate egg laying•These signals act via different receptors on the same muscles to pattern behavior•The two signals together initiate egg laying after ∼20-min inactive phases•Each signal then causes egg-laying events at different frequencies over ∼2 minSummaryNeurons typically release both a neurotransmitter and one or more neuropeptides, but how these signals are integrated within neural circuits to generate and tune behaviors remains poorly understood. We studied how the two hermaphrodite-specific neurons (HSNs) activate the egg-laying circuit of Caenorhabditis elegans by releasing both the neurotransmitter serotonin and NLP-3 neuropeptides. Egg laying occurs in a temporal pattern with approximately 2-min active phases, during which eggs are laid, separated by approximately 20-min inactive phases, during which no eggs are laid. To understand how serotonin and NLP-3 neuropeptides together help produce this behavior pattern, we identified the G-protein-coupled receptor neuropeptide receptor 36 (NPR-36) as an NLP-3 neuropeptide receptor using genetic and molecular experiments. We found that NPR-36 is expressed in, and promotes egg laying within, the egg-laying muscle cells, the same cells where two serotonin receptors also promote egg laying. During the active phase, when HSN activity is high, we found that serotonin and NLP-3 neuropeptides each have a different effect on the timing of egg laying. During the inactive phase, HSN activity is low, which may result in release of only serotonin, yet mutants lacking either serotonin or nlp-3 signaling have longer inactive phases. This suggests that NLP-3 peptide signaling may persist through the inactive phase to help serotonin signaling terminate the inactive phase. We propose a model for neural circuit function in which multiple signals with short- and long-lasting effects compete to generate and terminate persistent internal states, thus patterning a behavior over tens of minutes.
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