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手性硫代磷酸酯 DNA 与转录因子 SATB1 的增强亲和力源于非对映异构体特异性氢键和疏水接触。

Enhanced affinity of racemic phosphorothioate DNA with transcription factor SATB1 arising from diastereomer-specific hydrogen bonds and hydrophobic contacts.

机构信息

Biomedical Research Institute, National Institute of Advanced Industrial Science and Technology (AIST), 1-1-1 Higashi, Tsukuba 305-8566, Japan.

出版信息

Nucleic Acids Res. 2020 May 7;48(8):4551-4561. doi: 10.1093/nar/gkaa170.

Abstract

Phosphorothioate modification is commonly introduced into therapeutic oligonucleotides, typically as a racemic mixture in which either of the two non-bridging phosphate oxygens is replaced by sulfur, which frequently increases affinities with proteins. Here, we used isothermal titration calorimetry and X-ray crystallography to investigate the thermodynamic and structural properties of the interaction between the primary DNA-binding domain (CUTr1) of transcription factor SATB1 and dodecamer DNAs with racemic phosphorothioate modifications at the six sites known to contact CUTr1 directly. For both the modified and unmodified DNAs, the binding reactions were enthalpy-driven at a moderate salt concentration (50 mM NaCl), while being entropy-driven at higher salt concentrations with reduced affinities. The phosphorothioate modifications lowered this susceptibility to salt, resulting in a significantly enhanced affinity at a higher salt concentration (200 mM NaCl), although only some DNA molecular species remained interacting with CUTr1. This was explained by unequal populations of the two diastereomers in the crystal structure of the complex of CUTr1 and the phosphorothioate-modified DNA. The preferred diastereomer formed more hydrogen bonds with the oxygen atoms and/or more hydrophobic contacts with the sulfur atoms than the other, revealing the origins of the enhanced affinity.

摘要

硫代磷酸酯修饰通常被引入治疗性寡核苷酸中,通常作为外消旋混合物,其中两个非桥接磷酸氧原子中的任何一个都被硫取代,这通常会增加与蛋白质的亲和力。在这里,我们使用等温滴定量热法和 X 射线晶体学研究了转录因子 SATB1 的主要 DNA 结合域(CUTr1)与直接与 CUTr1 接触的六个位点的六聚体 DNA 之间的相互作用的热力学和结构性质。对于修饰和未修饰的 DNA,结合反应在中等盐浓度(50 mM NaCl)下是焓驱动的,而在高盐浓度下是熵驱动的,亲和力降低。硫代磷酸酯修饰降低了这种对盐的敏感性,导致在更高盐浓度(200 mM NaCl)下显著增强的亲和力,尽管只有一些 DNA 分子物种仍然与 CUTr1 相互作用。这可以通过 CUTr1 和硫代磷酸酯修饰的 DNA 复合物的晶体结构中两种非对映异构体的不均匀群体来解释。优选的非对映异构体与氧原子形成更多氢键,与硫原子形成更多疏水接触,这揭示了增强亲和力的起源。

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