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用于固醇运输和溶酶体贮积症的活体监测的杂环固醇探针。

Heterocyclic sterol probes for live monitoring of sterol trafficking and lysosomal storage disorders.

机构信息

CZ-OPENSCREEN, Institute of Molecular Genetics of the ASCR, v.v.i., Vídeňská 1083, 14220, Prague 4, Czech Republic.

University of Chemistry and Technology, Technická 5, 16628, Prague 6, Czech Republic.

出版信息

Sci Rep. 2018 Sep 26;8(1):14428. doi: 10.1038/s41598-018-32776-6.

Abstract

The monitoring of intracellular cholesterol homeostasis and trafficking is of great importance because their imbalance leads to many pathologies. Reliable tools for cholesterol detection are in demand. This study presents the design and synthesis of fluorescent probes for cholesterol recognition and demonstrates their selectivity by a variety of methods. The construction of dedicated library of 14 probes was based on heterocyclic (pyridine)-sterol derivatives with various attached fluorophores. The most promising probe, a P1-BODIPY conjugate FP-5, was analysed in detail and showed an intensive labelling of cellular membranes followed by intracellular redistribution into various cholesterol rich organelles and vesicles. FP-5 displayed a stronger signal, with faster kinetics, than the commercial TF-Chol probe. In addition, cells with pharmacologically disrupted cholesterol transport, or with a genetic mutation of cholesterol transporting protein NPC1, exhibited strong and fast FP-5 signal in the endo/lysosomal compartment, co-localizing with filipin staining of cholesterol. Hence, FP-5 has high potential as a new probe for monitoring cholesterol trafficking and its disorders.

摘要

细胞内胆固醇动态平衡和运输的监测非常重要,因为它们的失衡会导致许多病理。可靠的胆固醇检测工具是有需求的。本研究设计并合成了用于胆固醇识别的荧光探针,并通过多种方法证明了它们的选择性。专用的 14 个探针库的构建基于具有各种附着荧光团的杂环(吡啶)-固醇衍生物。最有前途的探针 P1-BODIPY 缀合物 FP-5 进行了详细分析,结果表明它可以强烈标记细胞膜,然后在细胞内重新分布到各种富含胆固醇的细胞器和小泡中。与商业 TF-Chol 探针相比,FP-5 具有更强的信号和更快的动力学。此外,用药理学方法破坏胆固醇运输的细胞,或用胆固醇转运蛋白 NPC1 的基因突变的细胞,在内体/溶酶体腔内显示出强烈和快速的 FP-5 信号,与胆固醇的 filipin 染色共定位。因此,FP-5 作为一种监测胆固醇运输及其紊乱的新探针具有很大的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f5df/6158244/5ec4ed9d986d/41598_2018_32776_Fig1_HTML.jpg

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