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紧密连接蛋白在早期小鼠颅发育中的经典和非经典定位。

Canonical and Non-Canonical Localization of Tight Junction Proteins during Early Murine Cranial Development.

机构信息

Max-Delbrück-Center for Molecular Medicine in the Helmholtz Association (MDC), 13125 Berlin, Germany.

Institute for Biology, Free University of Berlin, 14159 Berlin, Germany.

出版信息

Int J Mol Sci. 2024 Jan 24;25(3):1426. doi: 10.3390/ijms25031426.

Abstract

This study investigates the intricate composition and spatial distribution of tight junction complex proteins during early mouse neurulation. The analyses focused on the cranial neural tube, which gives rise to all head structures. Neurulation brings about significant changes in the neuronal and non-neuronal ectoderm at a cellular and tissue level. During this process, precise coordination of both epithelial integrity and epithelial dynamics is essential for accurate tissue morphogenesis. Tight junctions are pivotal for epithelial integrity, yet their complex composition in this context remains poorly understood. Our examination of various tight junction proteins in the forebrain region of mouse embryos revealed distinct patterns in the neuronal and non-neuronal ectoderm, as well as mesoderm-derived mesenchymal cells. While claudin-4 exhibited exclusive expression in the non-neuronal ectoderm, we demonstrated a neuronal ectoderm specific localization for claudin-12 in the developing cranial neural tube. Claudin-5 was uniquely present in mesenchymal cells. Regarding the subcellular localization, canonical tight junction localization in the apical junctions was predominant for most tight junction complex proteins. ZO-1 (zona occludens protein-1), claudin-1, claudin-4, claudin-12, and occludin were detected at the apical junction. However, claudin-1 and occludin also appeared in basolateral domains. Intriguingly, claudin-3 displayed a non-canonical localization, overlapping with a nuclear lamina marker. These findings highlight the diverse tissue and subcellular distribution of tight junction proteins and emphasize the need for their precise regulation during the dynamic processes of forebrain development. The study can thereby contribute to a better understanding of the role of tight junction complex proteins in forebrain development.

摘要

这项研究调查了早期小鼠神经胚发生过程中紧密连接复合体蛋白的复杂组成和空间分布。分析集中在颅神经管上,它产生所有头部结构。神经胚发生在细胞和组织水平上引起神经元和非神经元外胚层的显著变化。在此过程中,上皮完整性和上皮动态的精确协调对于准确的组织形态发生至关重要。紧密连接对于上皮完整性至关重要,但它们在这种情况下的复杂组成仍知之甚少。我们检查了小鼠胚胎前脑区域的各种紧密连接蛋白,发现神经元和非神经元外胚层以及中胚层衍生的间充质细胞中存在明显的模式。Claudin-4 在非神经元外胚层中表现出独特的表达,而我们在发育中的颅神经管中证明了 Claudin-12 具有神经元外胚层特异性定位。Claudin-5 仅存在于间充质细胞中。关于亚细胞定位,大多数紧密连接复合体蛋白在顶膜连接处都表现出经典的紧密连接定位。ZO-1(封闭蛋白-1)、Claudin-1、Claudin-4、Claudin-12 和 Occludin 都在顶膜连接处被检测到。然而,Claudin-1 和 Occludin 也出现在基底外侧区域。有趣的是,Claudin-3 表现出非经典的定位,与核层标记重叠。这些发现突出了紧密连接蛋白在组织和亚细胞分布上的多样性,并强调了在大脑前发育的动态过程中需要对其进行精确调节。该研究有助于更好地理解紧密连接复合体蛋白在大脑前发育中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b316/10855338/3f006d0fb9d1/ijms-25-01426-g001.jpg

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