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新型全甲基化β-环糊精衍生物,连接有发色团,作为用于胆汁盐分子识别的高效荧光传感器。

Novel permethylated beta-cyclodextrin derivatives appended with chromophores as efficient fluorescent sensors for the molecular recognition of bile salts.

作者信息

Liu Yu, Shi Jun, Guo Dong-Sheng

机构信息

Department of Chemistry, State Key Laboratory of Elemento-Organic Chemistry, Nankai University, Tianjin, 300071, People's Republic of China.

出版信息

J Org Chem. 2007 Oct 26;72(22):8227-34. doi: 10.1021/jo071131m. Epub 2007 Oct 3.

Abstract

Two novel permethylated beta-cyclodextrin (PM-beta-CD) derivatives, i.e., 6I-O-(1-naphtholxy)-2I,31-di-O-methylhexakis(2II-VII,3II-VII,6II-VII-tri-O-methyl)-beta-cyclodextrin (1) and 6I-O-(8-hydroxyquinoline)-2I,31-di-O-methylhexakis(2II-VII,3II-VII,6II-VII- tri-O-methyl)-beta-cyclodextrin (2), were synthesized in satisfactory yields, and their inclusion modes, complex-induced fluorescent behaviors, binding ability, and selectivity for bile salts of biological relevance (cholic acid sodium salt, CA; deoxycholic acid sodium salt, DCA; glycochoic acid sodium salt, GCA; taurocholic acid sodium salt, TCA) were investigated by the circular dichroism, 2D NMR, steady-state, and time-resolved fluorescent spectra. The results obtained from induced circular dichroism and ROESY spectra show that the chromophore groups of 1 and 2 reside in the central cavity of PM-beta-CD, and are expelled to the region of narrow torus rim upon complexation with bile guests, which presents the binding mode of cooperative inclusion. The transfer of the chromophore groups from the central cavity to the more hydrophobic torus rim leads to the remarkable increase of fluorescent intensities and longer fluorescent lifetimes of hosts 1 and 2 upon gradual addition of bile salts, which is importantly distinct from the molecular recognition of the chromophore-modified beta-CD species with bile salts. Interestingly, hosts 1 and 2 present much stronger binding ability for bile guests than PM-beta-CD. Differing from native beta-CD, all the PM-beta-CDs are more prone to include bile salts with longer tails, such as GCA and TCA. Their corresponding binding ability and molecular selectivity are closely discussed from the viewpoints of difference of cavity size/shape between beta-CD and PM-beta-CD, effect of substituent groups, and structures of bile guests, respectively.

摘要

合成了两种新型全甲基化β-环糊精(PM-β-CD)衍生物,即6I-O-(1-萘氧基)-2I,31-二-O-甲基六(2II-VII,3II-VII,6II-VII-三-O-甲基)-β-环糊精(1)和6I-O-(8-羟基喹啉)-2I,31-二-O-甲基六(2II-VII,3II-VII,6II-VII-三-O-甲基)-β-环糊精(2),产率令人满意。通过圆二色性、二维核磁共振、稳态和时间分辨荧光光谱研究了它们的包合模式、络合物诱导的荧光行为、结合能力以及对具有生物学相关性的胆盐(胆酸钠盐,CA;脱氧胆酸钠盐,DCA;甘氨胆酸钠盐,GCA;牛磺胆酸钠盐,TCA)的选择性。从诱导圆二色性和ROESY光谱获得的结果表明,1和2的发色团位于PM-β-CD的中心腔内,与胆汁客体络合时被排到窄环边缘区域,呈现协同包合的结合模式。随着胆盐的逐渐加入,发色团从中心腔转移到更疏水的环边缘导致主体1和2的荧光强度显著增加且荧光寿命延长,这与发色团修饰的β-环糊精物种与胆盐的分子识别有重要区别。有趣的是,主体1和2对胆汁客体的结合能力比PM-β-CD强得多。与天然β-环糊精不同,所有的PM-β-CD更倾向于包合尾巴更长的胆盐,如GCA和TCA。分别从β-环糊精和PM-β-CD的腔尺寸/形状差异、取代基的影响以及胆汁客体的结构等角度对它们相应的结合能力和分子选择性进行了深入讨论。

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