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一种荧光鞘脂结合域肽探针与鞘脂和胆固醇依赖性脂筏结构域相互作用。

A fluorescent sphingolipid binding domain peptide probe interacts with sphingolipids and cholesterol-dependent raft domains.

作者信息

Hebbar Sarita, Lee Esther, Manna Manoj, Steinert Steffen, Kumar Goparaju Sravan, Wenk Markus, Wohland Thorsten, Kraut Rachel

机构信息

Institute of Bioengineering and Nanotechnology, The Nanos, Singapore 138669.

出版信息

J Lipid Res. 2008 May;49(5):1077-89. doi: 10.1194/jlr.M700543-JLR200. Epub 2008 Feb 8.

Abstract

We have designed a tagged probe [sphingolipid binding domain (SBD)] to facilitate the tracking of intracellular movements of sphingolipids in living neuronal cells. SBD is a small peptide consisting of the SBD of the amyloid precursor protein. It can be conjugated to a fluorophore of choice and exogenously applied to cells, thus allowing for in vivo imaging. Here, we present evidence to describe the characteristics of the SBD association with the plasma membrane. Our experiments demonstrate that SBD binds to isolated raft fractions from human neuroblastomas and insect neuronal cells. In protein-lipid overlay experiments, SBD interacts with a subset of glycosphingolipids and sphingomyelin, consistent with its raft association in neurons. We also provide evidence that SBD is taken up by neuronal cells in a cholesterol- and sphingolipid-dependent manner via detergent-resistant microdomains. Furthermore, using fluorescence correlation spectroscopy to assay the mobility of SBD in live cells, we show that SBD's behavior at the plasma membrane is similar to that of the previously described raft marker cholera toxin B, displaying both a fast and a slow component. Our data suggest that fluorescently tagged SBD can be used to investigate the dynamic nature of glycosphingolipid-rich detergent-resistant microdomains that are cholesterol-dependent.

摘要

我们设计了一种带标签的探针[鞘脂结合结构域(SBD)],以促进对活神经元细胞中鞘脂细胞内运动的追踪。SBD是一种由淀粉样前体蛋白的SBD组成的小肽。它可以与所选的荧光团偶联,并外源应用于细胞,从而实现体内成像。在这里,我们提供证据来描述SBD与质膜结合的特征。我们的实验表明,SBD与来自人神经母细胞瘤和昆虫神经元细胞的分离筏状组分结合。在蛋白质-脂质覆盖实验中,SBD与一部分糖鞘脂和鞘磷脂相互作用,这与其在神经元中的筏状结合一致。我们还提供证据表明,SBD通过耐去污剂微区以胆固醇和鞘脂依赖性方式被神经元细胞摄取。此外,使用荧光相关光谱法测定SBD在活细胞中的流动性,我们表明SBD在质膜上的行为类似于先前描述的筏状标记霍乱毒素B,表现出快速和慢速成分。我们的数据表明,荧光标记的SBD可用于研究富含糖鞘脂的、胆固醇依赖性的耐去污剂微区的动态性质。

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