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PDZ蛋白复合物的整合活性调节上皮极性。

Integrated activity of PDZ protein complexes regulates epithelial polarity.

作者信息

Bilder David, Schober Markus, Perrimon Norbert

机构信息

Department of Genetics and Howard Hughes Medical Institute, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Nat Cell Biol. 2003 Jan;5(1):53-8. doi: 10.1038/ncb897.

Abstract

Polarized cells contain numerous membrane domains, but it is unclear how the formation of these domains is coordinated to create a single integrated cell architecture. Genetic screens of Drosophila melanogaster embryos have identified three complexes, each containing one of the PDZ domain proteins--Stardust (Sdt), Bazooka (Baz) and Scribble (Scrib)--that control epithelial polarity and formation of zonula adherens. We find that these complexes can be ordered into a single regulatory hierarchy that is initiated by cell adhesion-dependent recruitment of the Baz complex to the zonula adherens. The Scrib complex represses apical identity along basolateral surfaces by antagonizing Baz-initiated apical polarity. The Sdt-containing Crb complex is recruited apically by the Baz complex to counter antagonistic Scrib activity. Thus, a finely tuned balance between Scrib and Crb complex activity sets the limits of the apical and basolateral membrane domains and positions cell junctions. Our data suggest a model in which the maturation of epithelial cell polarity is driven by integration of the sequential activities of PDZ-based protein complexes.

摘要

极化细胞包含众多膜结构域,但尚不清楚这些结构域的形成是如何协调以创建单一整合细胞结构的。对黑腹果蝇胚胎的遗传筛选已鉴定出三种复合物,每种复合物都包含一种PDZ结构域蛋白——星尘(Sdt)、巴祖卡(Baz)和scribble(Scrib)——它们控制上皮极性和黏着小带的形成。我们发现这些复合物可排列成一个单一的调控层级,该层级由细胞黏附依赖性地将Baz复合物招募至黏着小带启动。Scrib复合物通过拮抗Baz启动的顶端极性来抑制基底外侧表面的顶端特性。含Sdt的Crb复合物由Baz复合物向顶端招募,以对抗Scrib的拮抗活性。因此,Scrib和Crb复合物活性之间的精细平衡设定了顶端和基底外侧膜结构域的界限并定位细胞连接。我们的数据提示了一个模型,其中上皮细胞极性的成熟是由基于PDZ的蛋白质复合物的顺序活性整合驱动的。

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