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首页> 外文期刊>Biophysical Journal >Correlated fluorescence-atomic force microscopy of membrane domains: Structure of fluorescence probes determines lipid localization
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Correlated fluorescence-atomic force microscopy of membrane domains: Structure of fluorescence probes determines lipid localization

机译:膜结构域的相关荧光原子力显微镜:荧光探针的结构决定脂质的定位

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Coupling atomic force microscopy ( AFM) with high-resolution fluorescence microscopy is an attractive means of identifying membrane domains by both physical topography and fluorescence. We have used this approach to study the ability of a suite of fluorescent molecules to probe domain structures in supported planar bilayers. These included BODIPY-labeled ganglioside, sphingomyelin, and three new cholesterol derivatives, as well as NBD-labeled phosphatidylcholine, sphingomyelin, and cholesterol. Interestingly, many fluorescent lipid probes, including derivatives of known raft-associated lipids, preferentially partitioned into topographical features consistent with nonraft domains. This suggests that the covalent attachment of a small fluorophore to a lipid molecule can abolish its ability to associate with rafts. In addition, the localization of one of the BODIPY-cholesterol derivatives was dependent on the lipid composition of the bilayer. These data suggest that conclusions about the identification of membrane domains in supported planar bilayers on the basis of fluorescent lipid probes alone must be interpreted with caution. The combination of AFM with fluorescence microscopy represents a more rigorous means of identifying lipid domains in supported bilayers.
机译:原子力显微镜(AFM)与高分辨率荧光显微镜的耦合是通过物理形貌和荧光鉴定膜结构域的一种有吸引力的手段。我们已经使用这种方法来研究一组荧光分子探测支持的平面双层中的域结构的能力。这些包括BODIPY标记的神经节苷脂,鞘磷脂和三种新的胆固醇衍生物,以及NBD标记的磷脂酰胆碱,鞘磷脂和胆固醇。有趣的是,许多荧光脂质探针,包括已知的筏相关脂质的衍生物,优选地被划分成与非筏域一致的形貌特征。这表明,小荧光团与脂质分子的共价结合可以消除其与木筏缔合的能力。另外,BODIPY-胆固醇衍生物之一的定位取决于双层的脂质组成。这些数据表明,仅在荧光脂质探针的基础上,有关在支持的平面双层膜中识别膜结构域的结论必须谨慎解释。 AFM与荧光显微镜的结合代表了一种更严格的方法来鉴定支持的双层脂质结构域。

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