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通过精氨酸残基对神经降压素(8-13)进行荧光标记可得到具有高受体亲和力的分子工具。

Fluorescence Labeling of Neurotensin(8-13) via Arginine Residues Gives Molecular Tools with High Receptor Affinity.

作者信息

Keller Max, Mahuroof Shahani A, Hong Yee Vivyanne, Carpenter Jessica, Schindler Lisa, Littmann Timo, Pegoli Andrea, Hübner Harald, Bernhardt Günther, Gmeiner Peter, Holliday Nicholas D

机构信息

Institute of Pharmacy, Faculty of Chemistry and Pharmacy, University of Regensburg, Universitätsstraße 31, D-93053 Regensburg, Germany.

School of Life Sciences, University of Nottingham, Queen's Medical Centre, Nottingham NG7 2UH, United Kingdom.

出版信息

ACS Med Chem Lett. 2019 Nov 19;11(1):16-22. doi: 10.1021/acsmedchemlett.9b00462. eCollection 2020 Jan 9.

Abstract

Fluorescence-labeled receptor ligands have emerged as valuable molecular tools, being indispensable for studying receptor-ligand interactions by fluorescence-based techniques such as high-content imaging, fluorescence microscopy, and fluorescence polarization. Through application of a new labeling strategy for peptides, a series of fluorescent neurotensin(8-13) derivatives was synthesized by attaching red-emitting fluorophores (indolinium- and pyridinium-type cyanine dyes) to carbamoylated arginine residues in neurotensin(8-13) analogues, yielding fluorescent probes with high NTSR affinity (p values: 8.15-9.12) and potency (pEC values (Ca mobilization): 8.23-9.43). Selected fluorescent ligands were investigated by flow cytometry and high-content imaging (saturation binding, kinetic studies, and competition binding) as well as by confocal microscopy using intact CHO-hNTSR cells. The study demonstrates the applicability of the fluorescent probes as molecular tools to obtain, for example, information about the localization of receptors in cells and to determine binding affinities of nonlabeled ligands.

摘要

荧光标记的受体配体已成为有价值的分子工具,对于通过基于荧光的技术(如高内涵成像、荧光显微镜和荧光偏振)研究受体 - 配体相互作用不可或缺。通过应用一种新的肽标记策略,通过将发射红色荧光的荧光团(吲哚啉和吡啶型花青染料)连接到神经降压素(8 - 13)类似物中的氨甲酰化精氨酸残基上,合成了一系列荧光神经降压素(8 - 13)衍生物,得到了具有高NTSR亲和力(p值:8.15 - 9.12)和效力(pEC值(钙动员):8.23 - 9.43)的荧光探针。使用完整的CHO - hNTSR细胞,通过流式细胞术、高内涵成像(饱和结合、动力学研究和竞争结合)以及共聚焦显微镜对选定的荧光配体进行了研究。该研究证明了荧光探针作为分子工具的适用性,例如可用于获取有关细胞中受体定位的信息以及确定未标记配体的结合亲和力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9d24/6956362/dedf58098b62/ml9b00462_0001.jpg

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