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在完整细胞膜上直接映射纳米级组成连通性。

Direct mapping of nanoscale compositional connectivity on intact cell membranes.

机构信息

BioNanoPhotonics group, Institute for Bioengineering of Catalonia (IBEC) and CIBER-bbn, Baldiri Reixac 15-21, 08028 Barcelona, Spain.

出版信息

Proc Natl Acad Sci U S A. 2010 Aug 31;107(35):15437-42. doi: 10.1073/pnas.1003876107. Epub 2010 Aug 16.

Abstract

Lateral segregation of cell membranes is accepted as a primary mechanism for cells to regulate a diversity of cellular functions. In this context, lipid rafts have been conceptualized as organizing principle of biological membranes where underlying cholesterol-mediated selective connectivity must exist even at the resting state. However, such a level of nanoscale compositional connectivity has been challenging to prove. Here we used single-molecule near-field scanning optical microscopy to visualize the nanolandscape of raft ganglioside GM1 after tightening by its ligand cholera toxin (CTxB) on intact cell membranes. We show that CTxB tightening of GM1 is sufficient to initiate a minimal raft coalescence unit, resulting in the formation of cholesterol-dependent GM1 nanodomains < 120 nm in size. This particular arrangement appeared independent of cell type and GM1 expression level on the membrane. Simultaneous dual color high-resolution images revealed that GPI anchored and certain transmembrane proteins were recruited to regions proximal (< 150 nm) to CTxB-GM1 nanodomains without physical intermixing. Together with in silico experiments, our high-resolution data conclusively demonstrate the existence of raft-based interconnectivity at the nanoscale. Such a linked state on resting cell membranes constitutes thus an obligatory step toward the hierarchical evolution of large-scale raft coalescence upon cell activation.

摘要

细胞膜的侧向分离被认为是细胞调节多种细胞功能的主要机制。在这种情况下,脂筏被概念化为生物膜的组织原则,其中基础胆固醇介导的选择性连接性即使在静止状态下也必须存在。然而,要证明这种纳米级组成连接性的水平一直具有挑战性。在这里,我们使用单分子近场扫描光学显微镜来可视化完整细胞膜上霍乱毒素(CTxB)与其配体结合后神经节苷脂 GM1 的纳米景观。我们表明,GM1 与 CTxB 的紧密结合足以引发最小的筏状聚集单元,导致胆固醇依赖性 GM1 纳米域的形成,其大小<120nm。这种特殊的排列似乎独立于细胞膜上的细胞类型和 GM1 表达水平。同时进行的双色高分辨率图像显示,GPI 锚定和某些跨膜蛋白被募集到 CTxB-GM1 纳米域附近(<150nm),而没有物理混合。结合计算机模拟实验,我们的高分辨率数据确凿地证明了纳米级筏状连接性的存在。在细胞激活时,这种在静止细胞膜上的连接状态构成了大尺度筏状聚集的分层进化的必要步骤。

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