由性别特异性粘连蛋白表达确定的经验依赖性、性别双态突触连接性

IF 11.7 1区 综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES
Chien-Po Liao, Maryam Majeed, Oliver Hobert
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引用次数: 0

摘要

早年的生活经历会影响成年大脑随后的成熟和功能,有时甚至会以性别特异性的方式产生影响,但人们对其潜在的分子机制却知之甚少。我们在此描述了幼年经历是如何定义成年秀丽隐杆线虫神经系统中性双态突触连接的。对幼年雄性的饥饿会破坏血清素依赖性地激活痛觉感觉神经元 PHB 中的 CREB 转录因子。CREB通过一系列转录因子控制非典型粘附蛋白FMI-1/Flamingo/CELSR的表达。在胚后发育过程中,FMI-1 可促进和维持两性 PHB 与指令性中间神经元 AVA 的突触连接,但依赖于血清素的转录调控盒可拮抗雄性的 FMI-1 表达,从而在 PHB 和 AVA 之间建立起性双态连接。CREB靶标LIN-29是一个关键的调控节点,它是一种Zn指转录因子,整合了四层信息:性特异性、过去的经验、时间和细胞类型特异性。我们的研究结果提供了幼年经历如何决定性双态突触连接的机制细节。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Experience-dependent, sexually dimorphic synaptic connectivity defined by sex-specific cadherin expression
Early-life experience influences subsequent maturation and function of the adult brain, sometimes even in a sex-specific manner, but underlying molecular mechanisms are poorly understood. We describe here how juvenile experience defines sexually dimorphic synaptic connectivity in the adult Caenorhabditis elegans nervous system. Starvation of juvenile males disrupts serotonin-dependent activation of the CREB transcription factor in a nociceptive sensory neuron, PHB. CREB acts through a cascade of transcription factors to control expression of an atypical cadherin protein, FMI-1/Flamingo/CELSR. During postembryonic development, FMI-1 promotes and maintains synaptic connectivity of PHB to a command interneuron, AVA, in both sexes, but a serotonin-dependent transcriptional regulatory cassette antagonizes FMI-1 expression in males, thereby establishing sexually dimorphic connectivity between PHB and AVA. A critical regulatory node is the CREB-target LIN-29, a Zn finger transcription factor that integrates four layers of information: sexual specificity, past experience, time and cell-type specificity. Our findings provide the mechanistic details of how an early juvenile experience defines sexually dimorphic synaptic connectivity.
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来源期刊
Science Advances
Science Advances 综合性期刊-综合性期刊
CiteScore
21.40
自引率
1.50%
发文量
1937
审稿时长
29 weeks
期刊介绍: Science Advances, an open-access journal by AAAS, publishes impactful research in diverse scientific areas. It aims for fair, fast, and expert peer review, providing freely accessible research to readers. Led by distinguished scientists, the journal supports AAAS's mission by extending Science magazine's capacity to identify and promote significant advances. Evolving digital publishing technologies play a crucial role in advancing AAAS's global mission for science communication and benefitting humankind.
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