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首页> 外文期刊>Development >Slit cleavage is essential for producing an active, stable, non-diffusible short-range signal that guides muscle migration
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Slit cleavage is essential for producing an active, stable, non-diffusible short-range signal that guides muscle migration

机译:切开卵裂对于产生活跃,稳定,不可扩散的短程信号至关重要,该信号可指导肌肉迁移

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摘要

During organogenesis, secreted signaling proteins direct cell migration towards their target tissue. In Drosophila embryos, developing muscles are guided by signals produced by tendons to promote the proper attachment of muscles to tendons, essential for proper locomotion. Previously, the repulsive protein Slit, secreted by tendon cells, has been proposed to be an attractant for muscle migration. However, our findings demonstrate that through tight control of its distribution, Slit repulsion is used for both directing and arresting muscle migration. We show that Slit cleavage restricts its distribution to tendon cells, allowing it to function as a short-range repellent that directs muscle migration and patterning, and promotes their halt upon reaching the target site. Mechanistically, we show that Slit processing produces a rapidly degraded C-terminal fragment and an active, stable N-terminal polypeptide that is tethered to the tendon cell membrane, which further protects it from degradation. Consistently, the requirement for Slit processing can be bypassed by providing an uncleavable, membrane-bound form of Slit that is stable and is retained on expressing tendon cells. Moreover, muscle elongation appears to be extremely sensitive to Slit levels, as replacing the entire full-length Slit with the stable Slit-N-polypeptide results in excessive repulsion, which leads to a defective muscle pattern. These findings reveal a novel cleavage-dependent regulatory mechanism controlling Slit spatial distribution, which may operate in other Slit-dependent processes.
机译:在器官发生过程中,分泌的信号蛋白指导细胞向其靶组织迁移。在果蝇胚胎中,肌腱产生的信号会引导发育中的肌肉,以促进肌肉与肌腱的正确附着,这对于正常运动至关重要。以前,肌腱细胞分泌的排斥蛋白Slit被认为是肌肉迁移的引诱剂。但是,我们的发现表明,通过严格控制其分布,狭缝排斥力可用于引导和阻止肌肉迁移。我们显示狭缝切割将其分布限制在肌腱细胞中,使其充当指导肌肉迁移和图案形成并促进到达目标部位后停止的短程驱蚊剂。从机制上讲,我们显示狭缝加工会产生快速降解的C端片段和一个拴在肌腱细胞膜上的活性,稳定的N端多肽,从而进一步保护其免受降解。一致地,通过提供稳定且保留在表达肌腱细胞上的不可切割的膜结合形式的Slit,可以绕开Slit处理的要求。此外,肌肉的伸长似乎对Slit水平极为敏感,因为用稳定的Slit-N-多肽替换整个全长Slit会导致排斥力过大,从而导致不良的肌肉图案。这些发现揭示了一种新颖的依赖分裂的调控机制,可控制狭缝的空间分布,该机制可能在其他依赖狭缝的过程中起作用。

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