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蛋白聚糖介导的信号素在轴突导向中的分子机制。

Molecular mechanisms of proteoglycan-mediated semaphorin signaling in axon guidance.

机构信息

Department of Cell Biology, Faculty of Science, Charles University, Prague 128 43, Czechia.

Laboratory of Structural Neurobiology, Institute of Molecular Genetics of the Czech Academy of Sciences, Prague 142 20, Czechia.

出版信息

Proc Natl Acad Sci U S A. 2024 Jul 30;121(31):e2402755121. doi: 10.1073/pnas.2402755121. Epub 2024 Jul 23.

Abstract

The precise assembly of a functional nervous system relies on axon guidance cues. Beyond engaging their cognate receptors and initiating signaling cascades that modulate cytoskeletal dynamics, guidance cues also bind components of the extracellular matrix, notably proteoglycans, yet the role and mechanisms of these interactions remain poorly understood. We found that secreted semaphorins bind specifically to glycosaminoglycan (GAG) chains of proteoglycans, showing a preference based on the degree of sulfation. Structural analysis of Sema2b unveiled multiple GAG-binding sites positioned outside canonical plexin-binding site, with the highest affinity binding site located at the C-terminal tail, characterized by a lysine-rich helical arrangement that appears to be conserved across secreted semaphorins. In vivo studies revealed a crucial role of the Sema2b C-terminal tail in specifying the trajectory of olfactory receptor neurons. We propose that secreted semaphorins tether to the cell surface through interactions with GAG chains of proteoglycans, facilitating their presentation to cognate receptors on passing axons.

摘要

精确的功能性神经系统的组装依赖于轴突导向线索。除了与同源受体结合并启动调节细胞骨架动态的信号级联反应外,导向线索还与细胞外基质的成分结合,特别是蛋白聚糖,但这些相互作用的作用和机制仍知之甚少。我们发现,分泌的神经 突起导向蛋白特异性地与蛋白聚糖的糖胺聚糖 (GAG) 链结合,根据硫酸化程度表现出偏好。对 Sema2b 的结构分析揭示了多个位于经典丛蛋白结合位点之外的 GAG 结合位点,具有最高亲和力的结合位点位于 C 末端尾部,其特征是富含赖氨酸的螺旋排列,似乎在分泌的神经 突起导向蛋白中保守。体内研究表明,Sema2b C 末端尾部在指定嗅觉受体神经元轨迹方面起着关键作用。我们提出,分泌的神经 突起通过与蛋白聚糖的 GAG 链相互作用而与细胞表面连接,从而有助于将其呈现给经过的轴突上的同源受体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66e2/11295036/48eae3f9f531/pnas.2402755121fig01.jpg

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