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膜联蛋白A6依赖性脂质结构域质膜重塑的证据。

Evidence for annexin A6-dependent plasma membrane remodelling of lipid domains.

作者信息

Alvarez-Guaita Anna, Vilà de Muga Sandra, Owen Dylan M, Williamson David, Magenau Astrid, García-Melero Ana, Reverter Meritxell, Hoque Monira, Cairns Rose, Cornely Rhea, Tebar Francesc, Grewal Thomas, Gaus Katharina, Ayala-Sanmartín Jesús, Enrich Carlos, Rentero Carles

机构信息

Departament de Biologia Cel·lular, Immunologia i Neurociències, Facultat de Medicina, Universitat de Barcelona, Barcelona, Spain.

出版信息

Br J Pharmacol. 2015 Apr;172(7):1677-90. doi: 10.1111/bph.13022. Epub 2015 Jan 20.

Abstract

BACKGROUND AND PURPOSE

Annexin A6 (AnxA6) is a calcium-dependent phospholipid-binding protein that can be recruited to the plasma membrane to function as a scaffolding protein to regulate signal complex formation, endo- and exocytic pathways as well as distribution of cellular cholesterol. Here, we have investigated how AnxA6 influences the membrane order.

EXPERIMENTAL APPROACH

We used Laurdan and di-4-ANEPPDHQ staining in (i) artificial membranes; (ii) live cells to investigate membrane packing and ordered lipid phases; and (iii) a super-resolution imaging (photoactivated localization microscopy, PALM) and Ripley's K second-order point pattern analysis approach to assess how AnxA6 regulates plasma membrane order domains and protein clustering.

KEY RESULTS

In artificial membranes, purified AnxA6 induced a global increase in membrane order. However, confocal microscopy using di-4-ANEPPDHQ in live cells showed that cells expressing AnxA6, which reduces plasma membrane cholesterol levels and modifies the actin cytoskeleton meshwork, displayed a decrease in membrane order (∼15 and 30% in A431 and MEF cells respectively). PALM data from Lck10 and Src15 membrane raft/non-raft markers revealed that AnxA6 expression induced clustering of both raft and non-raft markers. Altered clustering of Lck10 and Src15 in cells expressing AnxA6 was also observed after cholesterol extraction with methyl-β-cyclodextrin or actin cytoskeleton disruption with latrunculin B.

CONCLUSIONS AND IMPLICATIONS

AnxA6-induced plasma membrane remodelling indicated that elevated AnxA6 expression decreased membrane order through the regulation of cellular cholesterol homeostasis and the actin cytoskeleton. This study provides the first evidence from live cells that support current models of annexins as membrane organizers.

摘要

背景与目的

膜联蛋白A6(AnxA6)是一种钙依赖性磷脂结合蛋白,可被募集到质膜上,作为一种支架蛋白发挥作用,调节信号复合物形成、胞吞和胞吐途径以及细胞胆固醇的分布。在此,我们研究了AnxA6如何影响膜的有序性。

实验方法

我们使用劳丹(Laurdan)和二-4-ANEPPDHQ染色,分别用于(i)人工膜;(ii)活细胞以研究膜的堆积和有序脂质相;以及(iii)超分辨率成像(光激活定位显微镜,PALM)和瑞普利K二阶点模式分析方法,以评估AnxA6如何调节质膜有序结构域和蛋白质聚集。

主要结果

在人工膜中,纯化的AnxA6引起膜有序性的整体增加。然而,在活细胞中使用二-4-ANEPPDHQ的共聚焦显微镜显示,表达AnxA6的细胞(其降低了质膜胆固醇水平并改变了肌动蛋白细胞骨架网络)的膜有序性降低(A431细胞和MEF细胞中分别约为15%和30%)。来自Lck10和Src15膜筏/非膜筏标记物的PALM数据显示,AnxA6表达诱导了膜筏和非膜筏标记物的聚集。在用甲基-β-环糊精提取胆固醇或用拉特罗毒素B破坏肌动蛋白细胞骨架后,也观察到表达AnxA6的细胞中Lck10和Src15聚集的改变。

结论与启示

AnxA6诱导的质膜重塑表明,AnxA6表达升高通过调节细胞胆固醇稳态和肌动蛋白细胞骨架降低了膜有序性。本研究提供了来自活细胞的首个证据,支持目前关于膜联蛋白作为膜组织者的模型。

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