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俄勒冈荧光体使定量细胞内配对剂成象成为可能,从而可以评估活细胞和组织中药物靶标的可用性。

OregonFluor enables quantitative intracellular paired agent imaging to assess drug target availability in live cells and tissues.

机构信息

Biomedical Engineering Department, Oregon Health & Science University, Portland, OR, USA.

Cancer Early Detection Advanced Research Center (CEDAR), Oregon Health & Science University, Portland, OR, USA.

出版信息

Nat Chem. 2023 May;15(5):729-739. doi: 10.1038/s41557-023-01173-6. Epub 2023 Mar 30.

Abstract

Non-destructive fluorophore diffusion across cell membranes to provide an unbiased fluorescence intensity readout is critical for quantitative imaging applications in live cells and tissues. Commercially available small-molecule fluorophores have been engineered for biological compatibility, imparting high water solubility by modifying rhodamine and cyanine dye scaffolds with multiple sulfonate groups. The resulting net negative charge, however, often renders these fluorophores cell-membrane-impermeant. Here we report the design and development of our biologically compatible, water-soluble and cell-membrane-permeable fluorophores, termed OregonFluor (ORFluor). By adapting previously established ratiometric imaging methodology using bio-affinity agents, it is now possible to use small-molecule ORFluor-labelled therapeutic inhibitors to quantitatively visualize their intracellular distribution and protein target-specific binding, providing a chemical toolkit for quantifying drug target availability in live cells and tissues.

摘要

非破坏性的荧光团穿过细胞膜扩散,以提供无偏的荧光强度读数,这对于活细胞和组织中的定量成像应用至关重要。商业上可用的小分子荧光团经过生物相容性设计,通过用多个磺酸基团修饰罗丹明和菁染料支架,赋予其高水溶性。然而,由此产生的净负电荷通常使这些荧光团不能穿透细胞膜。在这里,我们报告了我们设计和开发的生物兼容、水溶性和细胞膜渗透性的荧光团,称为 OregonFluor(ORFluor)。通过采用先前使用生物亲和剂建立的比率成像方法,现在可以使用小分子 ORFluor 标记的治疗抑制剂来定量可视化它们的细胞内分布和蛋白靶标特异性结合,为定量研究活细胞和组织中药物靶标的可用性提供了一个化学工具包。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcd5/10965356/50a7250172c3/nihms-1918465-f0007.jpg

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