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跨膜蛋白巨球蛋白补体相关蛋白对于果蝇中隔膜连接的形成和上皮屏障功能是必需的。

The transmembrane protein Macroglobulin complement-related is essential for septate junction formation and epithelial barrier function in Drosophila.

机构信息

Institute of Molecular Life Sciences and PhD Program in Molecular Life Sciences, University of Zurich, Winterthurerstrasse 190, CH-8057 Zurich, Switzerland.

出版信息

Development. 2014 Feb;141(4):899-908. doi: 10.1242/dev.102160.

Abstract

Occluding cell-cell junctions in epithelia form physical barriers that separate different membrane domains, restrict paracellular diffusion and prevent pathogens from spreading across tissues. In invertebrates, these functions are provided by septate junctions (SJs), the functional equivalent of vertebrate tight junctions. How the diverse functions of SJs are integrated and modulated in a multiprotein complex is not clear, and many SJ components are still unknown. Here we report the identification of Macroglobulin complement-related (Mcr), a member of the conserved α-2-macroglobulin (α2M) complement protein family, as a novel SJ-associated protein in Drosophila. Whereas α2M complement proteins are generally known as secreted factors that bind to surfaces of pathogens and target them for phagocytic uptake, Mcr represents an unusual α2M protein with a predicted transmembrane domain. We show that Mcr protein localizes to lateral membranes of epithelial cells, where its distribution overlaps with SJs. Several SJ components are required for the correct localization of Mcr. Conversely, Mcr is required in a cell-autonomous fashion for the correct membrane localization of SJ components, indicating that membrane-bound rather than secreted Mcr isoforms are involved in SJ formation. Finally, we show that loss of Mcr function leads to morphological, ultrastructural and epithelial barrier defects resembling mutants lacking SJ components. Our results, along with previous findings on the role of Mcr in phagocytosis, suggest that Mcr plays dual roles in epithelial barrier formation and innate immunity. Thus, Mcr represents a novel paradigm for investigating functional links between occluding junction formation and pathogen defense mechanisms.

摘要

上皮细胞的封闭细胞-细胞连接形成物理屏障,将不同的膜域分开,限制细胞旁扩散,并防止病原体在组织中扩散。在无脊椎动物中,这些功能由隔膜连接(SJ)提供,这是脊椎动物紧密连接的功能等效物。SJ 的多种功能如何在多蛋白复合物中整合和调节尚不清楚,并且许多 SJ 成分仍然未知。在这里,我们报告鉴定了Macroglobulin complement-related(Mcr),一种保守的α-2-巨球蛋白(α2M)补体蛋白家族的成员,作为果蝇中新型 SJ 相关蛋白。尽管α2M 补体蛋白通常被认为是结合病原体表面并将其靶向吞噬作用的分泌因子,但 Mcr 代表一种不寻常的 α2M 蛋白,具有预测的跨膜结构域。我们表明,Mcr 蛋白定位于上皮细胞的侧膜,其分布与 SJ 重叠。几种 SJ 成分是 Mcr 正确定位所必需的。相反,Mcr 以细胞自主的方式需要正确的 SJ 成分的膜定位,表明参与 SJ 形成的是膜结合而不是分泌的 Mcr 同工型。最后,我们表明 Mcr 功能的丧失会导致类似于缺乏 SJ 成分的突变体的形态、超微结构和上皮屏障缺陷。我们的结果,以及 Mcr 在吞噬作用中的作用的先前发现,表明 Mcr 在上皮屏障形成和先天免疫中发挥双重作用。因此,Mcr 代表了一个研究封闭连接形成和病原体防御机制之间功能联系的新范例。

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