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BODIPY 标记的雌二醇缀合物的合成及雌激素活性。

Synthesis and estrogenic activity of BODIPY-labeled estradiol conjugates.

机构信息

Department of Experimental Biology, Faculty of Science, Palacký University Olomouc, Šlechtitelů 27 78371 Olomouc, Czech Republic.

Department of Pharmacology and Pharmacotherapy, Medical School, University of Pécs, Szigeti út 12 H-7624 Pécs, Hungary.

出版信息

Eur J Pharm Sci. 2024 Aug 1;199:106813. doi: 10.1016/j.ejps.2024.106813. Epub 2024 May 24.

DOI:10.1016/j.ejps.2024.106813
PMID:38797442
Abstract

Novel BODIPY-estradiol conjugates have been synthesized by selecting position C-3-O for labeling. The conjugation strategy was based on Cu(I)-catalyzed azide-alkyne cycloaddition (CuAAC) or etherification. Estradiol derivatives used as azide partners bearing an ω-azidoalkyl function through C-C-long linkers have been prepared. CuAAC reactions of estradiol azides with BODIPY alkyne furnished fluorescent 3-O-labeled conjugates bearing the triazole ring as a coupling moiety. Williamson etherifications of 3-O-(ω-bromoalkyl)-17β-estradiol derivatives with BODIPY-OH resulted in labeled conjugates connected with an ether moiety. Interactions of the conjugates with estrogen receptor (ER) were investigated using molecular docking calculations in comparison with estradiol. The conjugates occupied both the classical and alternative binding sites on human ERα, with slightly lower binding affinity to references estradiol and diethystilbestrol. All compounds have displayed reasonable estrogenic activity. They increased the proliferation of ER-positive breast cancer cell line MCF7 contrary to ER-negative SKBR-3 cell line. The most potent compound 13a induced the transcriptional activity of ER in dose-dependent manner in dual luciferase recombinant reporter model and increased progesterone receptor's expression, proving the retained estrogenic activity. The fluorescence of candidate compound 13a co-localised with the ERα. The newly synthesized labeled compounds might serve as good starting point for further development of fluorescent probes for modern biological applications. In addition to studying steroid uptake and transport in cells, e.g. in the processes of biodegradation of estrogen-hormones micropollutants, they could also be utilized in examination of estrogen-binding proteins.

摘要

新型 BODIPY-雌二醇缀合物已通过选择 C-3-O 位进行标记来合成。缀合策略基于铜(I)催化的叠氮化物-炔烃环加成(CuAAC)或醚化反应。使用带有通过 C-C 长链连接的 ω-叠氮烷基官能团的作为叠氮化物供体的雌二醇衍生物进行制备。BODIPY 炔烃与雌二醇叠氮化物的 CuAAC 反应提供了带有三唑环作为偶联部分的荧光 3-O-标记缀合物。3-O-(ω-溴烷基)-17β-雌二醇衍生物与 BODIPY-OH 的 Williamson 醚化反应导致带有醚部分连接的标记缀合物。通过分子对接计算研究了缀合物与雌激素受体(ER)的相互作用,并与雌二醇进行了比较。与参考的雌二醇和己烯雌酚相比,缀合物占据了人 ERα 的经典和替代结合位点,结合亲和力略有降低。所有化合物均显示出合理的雌激素活性。它们增加了 ER 阳性乳腺癌细胞系 MCF7 的增殖,而对 ER 阴性 SKBR-3 细胞系没有影响。最有效的化合物 13a 在双荧光素酶重组报告模型中以剂量依赖性方式诱导 ER 的转录活性,并增加孕激素受体的表达,证明其保留了雌激素活性。候选化合物 13a 的荧光与 ERα 共定位。新合成的标记化合物可能作为进一步开发用于现代生物学应用的荧光探针的良好起点。除了研究细胞内甾体的摄取和转运,例如在雌激素激素微污染物的生物降解过程中,它们还可以用于雌激素结合蛋白的检测。

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