Department of Pharmacy, Ludwig-Maximilians-Universität München, Butenandtstr. 5-13, 81377, Munich, Germany.
Current address: Institute for Stem-Cell Biology, Regenerative Medicine and Innovative Therapies, IRCCS Casa Sollievo della Sofferenza, San Giovanni Rotondo (Italy) & Center for Nanomedicine and Tissue Engineering (CNTE), ASST Grande Ospedale Metropolitano Niguarda, 20162, Milan, Italy.
Chemistry. 2024 Mar 15;30(16):e202303650. doi: 10.1002/chem.202303650. Epub 2024 Jan 30.
DNA mimic foldamers based on aromatic oligoamide helices bearing anionic phosphonate side chains have been shown to bind to DNA-binding proteins sometimes orders of magnitude better than DNA itself. Here, we introduce new features in the DNA mimic foldamers to facilitate structural investigations of their interactions with proteins. Thirteen new foldamer sequences have been synthesized and characterized using NMR, circular dichroism, molecular modeling, and X-ray crystallography. The results show that foldamer helix handedness can be quantitatively biased by means of a single stereogenic center, that the foldamer structure can be made C-symmetrical as in palindromic B-DNA sequences, and that associations between foldamer helices can be promoted utilizing dedicated C-terminal residues that act as sticky ends in B-DNA structures.
基于带有阴离子膦酸侧链的芳香寡聚酰胺螺旋的 DNA 模拟折叠物已被证明可以与 DNA 结合蛋白结合,有时其结合能力比 DNA 本身高出几个数量级。在这里,我们在 DNA 模拟折叠物中引入了新的特征,以促进对其与蛋白质相互作用的结构研究。已经使用 NMR、圆二色性、分子建模和 X 射线晶体学合成和表征了 13 种新的折叠物序列。结果表明,通过单个手性中心可以定量地偏向折叠物螺旋手性,折叠物结构可以像回文 B-DNA 序列一样具有 C 对称性,并且可以利用作为 B-DNA 结构中的粘性末端的专用 C 末端残基促进折叠物螺旋之间的缔合。
