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JAK/STAT信号传导在上皮细胞凋亡性排出之前的细胞单核化过程中是必需的。

JAK/STAT signaling is necessary for cell monosis prior to epithelial cell apoptotic extrusion.

作者信息

Torres Alba Y, Malartre Marianne, Pret Anne-Marie, Agnès François

机构信息

Institute for Integrative Biology of the Cell (I2BC), CEA, CNRS, Université Paris-Sud, Université Paris-Saclay, 91198 Gif-sur-Yvette Cedex, France.

Institute for Integrative Biology of the Cell (I2BC), CEA, CNRS, Université Paris Sud, Université, Paris-Saclay, 91198 Gif-sur-Yvette Cedex France.

出版信息

Cell Death Dis. 2017 May 25;8(5):e2814. doi: 10.1038/cddis.2017.166.

Abstract

Epithelial cell extrusion is crucial for proper development and tissue homeostasis. High-resolution 3D reconstruction and 4D imaging, combined with genetic analyis, have allowed us to reveal the highly-sterotyped morphogenetic events controlled by JAK/STAT signaling in a developmentally-programmed case of epithelial cell extrusion. Specialized somatic cells, Polar Cells (PCs), are produced in excess and then undergo apoptotic elimination from the follicular epithelium in the Drosophila ovary. We show that supernumerary PCs are first systematically enveloped by PC neighbors on all sides, first laterally, then apically in conjunction with highly-reinforced adherens junctions, and finally basally. The PC to be removed thus loses all contact with follicle cells, germline cells and the basement membrane in a process we have called cell 'monosis', for 'isolation' in Greek. PC monosis takes several hours, and always precedes, and is independent of, activation of apoptosis. JAK/STAT signaling is necessary within the surrounding follicular epithelium for PC monosis. Minutes after monosis is complete, PC apoptotic corpses are formed and extruded laterally within the epithelium, in contrast to the apical and basal extrusions described to date. These apoptotic corpses are engulfed and eliminated by surrounding follicle cells, which are thus acting as non-professional phagocytes. This study therefore shows the non cell-autonomous impact of an epithelium, via JAK/STAT signaling activation, on cell morphogenesis events leading to apoptotic extrusion. It is likely that the use of high-resolution 3D and 4D imaging, which allows for better spatio-temporal understanding of morphogenetic events, will reveal that cell monosis and lateral extrusion within an epithelium are pertinent for other cases of epithelial cell extrusion as well.

摘要

上皮细胞挤出对于正常发育和组织稳态至关重要。高分辨率3D重建和4D成像,结合遗传分析,使我们能够揭示在发育编程的上皮细胞挤出案例中,由JAK/STAT信号通路控制的高度定型的形态发生事件。特化的体细胞,即极细胞(PCs),过量产生,然后在果蝇卵巢的卵泡上皮中经历凋亡清除。我们发现多余的PCs首先被周围的PC邻居全方位系统性地包裹,先是从侧面,然后是顶部,同时伴有高度强化的黏着连接,最后是底部。因此,要被清除的PC在一个我们称为细胞“分离”(源于希腊语“isolation”)的过程中,与卵泡细胞、生殖细胞和基底膜失去了所有接触。PC分离需要几个小时,并且总是先于凋亡激活且与之无关。周围卵泡上皮内的JAK/STAT信号通路对于PC分离是必需的。分离完成几分钟后,PC凋亡小体形成并在上皮内从侧面挤出,这与迄今为止描述的顶部和底部挤出不同。这些凋亡小体被周围的卵泡细胞吞噬并清除,因此周围卵泡细胞充当了非专职吞噬细胞。因此,这项研究表明上皮通过JAK/STAT信号通路激活,对导致凋亡挤出的细胞形态发生事件具有非细胞自主性影响。使用高分辨率3D和4D成像可能会更好地从时空角度理解形态发生事件,这可能会揭示上皮内的细胞分离和侧面挤出在其他上皮细胞挤出案例中也具有相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4dcb/5520696/251fcb63ee60/cddis2017166f1.jpg

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