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胚胎运动神经元轴突和树突靶向需要Imp和Chinmo。

Imp and Chinmo are required for embryonic motor neuron axon and dendrite targeting.

作者信息

Fisher Katherine H, Lai Sen-Lin, Doe Chris Q

机构信息

Institute of Neuroscience, Howard Hughes Medical Institute, University of Oregon, Eugene, OR 97403, USA.

出版信息

Biol Open. 2025 Jul 15;14(7). doi: 10.1242/bio.062105. Epub 2025 Jul 25.

Abstract

Neural progenitors generate distinct neuronal populations over time. Drosophila larval neural progenitors, neuroblasts (NBs), generate neuronal diversity by expressing temporal gradients of transcription factors and RNA-binding proteins, including early factors Imp and Chinmo and late factors Syp, Mamo, and Broad. These factors have been well characterized in the larval central nervous system (CNS), yet nothing is known about their expression or function in the embryonic CNS. We show that embryonic Imp is expressed in a low-to-high temporal gradient, the opposite of the larval Imp gradient. Embryonic Chinmo is expressed in all post-mitotic neurons, but not in a gradient, while the late larval factors Mamo, E93, Syp, and Broad show little embryonic expression. We show that Imp is required for Chinmo expression in postmitotic neurons, and loss of Chinmo - but not Imp - derepresses Syp. Finally, we tested whether Imp and Chinmo are required for motor neuron molecular identity or morphology. Although neither is required to specify temporal or molecular neuronal identity, both are required for axon targeting to the correct body wall muscle, and downregulating dendrite outgrowth. We conclude that temporal factors are regulated differently in embryos and larvae, and that Imp and Chinmo are required for proper neuronal axon and dendrite projections.

摘要

随着时间的推移,神经祖细胞会产生不同的神经元群体。果蝇幼虫神经祖细胞,即成神经细胞(NBs),通过表达转录因子和RNA结合蛋白的时间梯度来产生神经元多样性,这些因子包括早期因子Imp和Chinmo以及晚期因子Syp、Mamo和Broad。这些因子在幼虫中枢神经系统(CNS)中已得到充分表征,但它们在胚胎中枢神经系统中的表达或功能尚不清楚。我们发现胚胎期的Imp以从低到高的时间梯度表达,这与幼虫期Imp的梯度相反。胚胎期的Chinmo在所有有丝分裂后的神经元中表达,但不是以梯度形式表达,而幼虫晚期因子Mamo、E93、Syp和Broad在胚胎期几乎不表达。我们发现Imp是有丝分裂后神经元中Chinmo表达所必需的,Chinmo的缺失——而不是Imp的缺失——会解除对Syp的抑制。最后,我们测试了Imp和Chinmo是否是运动神经元分子身份或形态所必需的。虽然两者都不是确定时间或分子神经元身份所必需的,但两者都是轴突靶向正确体壁肌肉以及下调树突生长所必需的。我们得出结论,时间因子在胚胎和幼虫中的调控方式不同,并且Imp和Chinmo是神经元轴突和树突正确投射所必需的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3cd5/12352280/ecd0f4df9fa5/biolopen-14-062105-g1.jpg

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