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drebrin是一种广泛存在的肌动蛋白结合蛋白,在连接斑处富集,在极性上皮细胞中定义了一种特定的微丝锚定系统。

Drebrin is a widespread actin-associating protein enriched at junctional plaques, defining a specific microfilament anchorage system in polar epithelial cells.

作者信息

Peitsch W K, Grund C, Kuhn C, Schnölzer M, Spring H, Schmelz M, Franke W W

机构信息

Division of Cell Biology, German Cancer Research Center, Heidelberg.

出版信息

Eur J Cell Biol. 1999 Nov;78(11):767-78. doi: 10.1016/S0171-9335(99)80027-2.

DOI:10.1016/S0171-9335(99)80027-2
PMID:10604653
Abstract

Using immunoblotting, immunprecipitation with subsequent fragment mass spectrometry, and immunolocalization techniques, we have detected the actin-binding ca. 120-kDa protein drebrin, originally identified in - and thought to be specific for - neuronal cells, in diverse kinds of human and bovine non-neuronal cells. Drebrin has been found in numerous cell culture lines and in many tissues of epithelial, endothelial, smooth muscle and neural origin but not in, for example, cardiac, skeletal and certain types of smooth muscle cells, in hepatocytes and in the human epithelium-derived cell culture line A-431. By double-label fluorescence microscopy we have found drebrin enriched in actin microfilament bundles associated with plaques of cell-cell contact sites representing adhering junctions. These drebrin-positive, adhering junction-associated bundles, however, are not identical with the vinculin-containing, junction-attached bundles, and in the same cell both subtypes of microfilament-anchoring plaques are readily distinguished by immunolocalization comparing drebrin and vinculin. The intracellular distribution of the drebrin- and the vinculin-based microfilament systems has been studied in detail by confocal fluorescence laser scanning microscopy in monolayers of the polar epithelial cell lines, MCF-7 and PLC, and drebrin has been found to be totally and selectively absent in the notoriously vinculin-rich focal adhesions. The occurrence and the possible functions of drebrin in non-neuronal cells, notably epithelial cells, and the significance of the existence of two different actin-anchoring junctional plaques is discussed.

摘要

运用免疫印迹法、免疫沉淀结合后续片段质谱分析法以及免疫定位技术,我们在多种人类和牛的非神经细胞中检测到了肌动蛋白结合蛋白——约120 kDa的 drebrin蛋白。该蛋白最初是在神经细胞中发现的,并且曾被认为是神经细胞特有的。现已在众多细胞系以及许多上皮、内皮、平滑肌和神经来源的组织中发现了drebrin蛋白,但在例如心肌、骨骼肌以及某些类型的平滑肌细胞、肝细胞和人上皮来源的细胞系A - 431中未发现。通过双标荧光显微镜观察,我们发现drebrin蛋白富集于与代表黏着连接的细胞 - 细胞接触位点斑块相关的肌动蛋白微丝束中。然而,这些drebrin阳性的、与黏着连接相关的微丝束与含纽蛋白的、连接附着的微丝束并不相同,并且在同一细胞中,通过比较drebrin和纽蛋白的免疫定位,很容易区分这两种微丝锚定斑块亚型。我们利用共聚焦荧光激光扫描显微镜详细研究了极性上皮细胞系MCF - 7和PLC单层中基于drebrin和基于纽蛋白的微丝系统的细胞内分布,结果发现drebrin蛋白在众所周知富含纽蛋白的黏着斑中完全且选择性地缺失。本文讨论了drebrin蛋白在非神经细胞(尤其是上皮细胞)中的存在情况及其可能的功能,以及两种不同肌动蛋白锚定连接斑块存在的意义。

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1
Drebrin is a widespread actin-associating protein enriched at junctional plaques, defining a specific microfilament anchorage system in polar epithelial cells. drebrin是一种广泛存在的肌动蛋白结合蛋白,在连接斑处富集,在极性上皮细胞中定义了一种特定的微丝锚定系统。
Eur J Cell Biol. 1999 Nov;78(11):767-78. doi: 10.1016/S0171-9335(99)80027-2.
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Actin-binding protein, drebrin, accumulates in submembranous regions in parallel with neuronal differentiation.肌动蛋白结合蛋白,脑发育蛋白,与神经元分化同步在膜下区域积累。
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FGF-2 induced reorganization and disruption of actin cytoskeleton through PI 3-kinase, Rho, and Cdc42 in corneal endothelial cells.在角膜内皮细胞中,成纤维细胞生长因子-2(FGF-2)通过磷脂酰肌醇3激酶(PI 3-激酶)、Rho和Cdc42诱导肌动蛋白细胞骨架的重组和破坏。
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Transition of aortic endothelial cells from resting to migrating cells is associated with three sequential patterns of microfilament organization.主动脉内皮细胞从静止状态转变为迁移状态与微丝组织的三种连续模式相关。
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