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Kpc-1 3'UTR 促进机械敏感性神经元树突分支所必需的 mRNA 的树突运输和翻译效率,该神经元对雄性求爱至关重要。

The kpc-1 3'UTR facilitates dendritic transport and translation efficiency of mRNAs for dendrite arborization of a mechanosensory neuron important for male courtship.

机构信息

Department of Biological Sciences, University of Illinois at Chicago, Chicago, Illinois, United States of America.

School of Life Science and Technology, ShanghaiTech University, Shanghai, China.

出版信息

PLoS Genet. 2024 Aug 7;20(8):e1011362. doi: 10.1371/journal.pgen.1011362. eCollection 2024 Aug.

Abstract

A recently reported Schizophrenia-associated genetic variant in the 3'UTR of the human furin gene, a homolog of C. elegans kpc-1, highlights an important role of the furin 3'UTR in neuronal development. We isolate three kpc-1 mutants that display abnormal dendrite arborization in PVD neurons and defective male mating behaviors. We show that the kpc-1 3'UTR participates in dendrite branching and self-avoidance. The kpc-1 3'UTR facilitates mRNA localization to branching points and contact points between sibling dendrites and promotes translation efficiency. A predicted secondary structural motif in the kpc-1 3'UTR is required for dendrite self-avoidance. Animals with over-expression of DMA-1, a PVD dendrite receptor, exhibit similar dendrite branching and self-avoidance defects that are suppressed with kpc-1 over-expression. Our results support a model in which KPC-1 proteins are synthesized at branching points and contact points to locally down-regulate DMA-1 receptors to promote dendrite branching and self-avoidance of a mechanosensory neuron important for male courtship.

摘要

最近报道了人类弗林蛋白酶基因 3'UTR 中的一个与精神分裂症相关的遗传变异,该基因与秀丽隐杆线虫的 kpc-1 同源,这突显了弗林蛋白酶 3'UTR 在神经元发育中的重要作用。我们分离出三个 kpc-1 突变体,它们在 PVD 神经元中表现出异常的树突分支,并表现出雄性交配行为缺陷。我们表明,kpc-1 3'UTR 参与树突分支和自我回避。kpc-1 3'UTR 促进 mRNA 定位到树突分支点和兄弟姐妹树突之间的接触点,并提高翻译效率。kpc-1 3'UTR 中的一个预测的二级结构模体是树突自我回避所必需的。过表达 PVD 树突受体 DMA-1 的动物表现出类似的树突分支和自我回避缺陷,这些缺陷可以通过过表达 kpc-1 来抑制。我们的结果支持这样一种模型,即 KPC-1 蛋白在分支点和接触点合成,以局部下调 DMA-1 受体,从而促进对雄性求偶至关重要的机械敏感神经元的树突分支和自我回避。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c2e/11333003/4f74fcdb121e/pgen.1011362.g001.jpg

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