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Halogen Bonds in Protein Nucleic Acid Recognition

机译:蛋白质核酸识别中的卤素键

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Identifying new binding forces between electron donor and acceptor entities is key to properly understanding molecular recognition and aggregation phenomena, which are of inmense importance to biology. For decades, the halogenation of DNA/RNA bases has been routinely carried out to solve solid state structures of nucleic acids (NA). However, the effects of this modification might be deeper than just a simple atom substitution since halogens are also known to undergo noncovalent binding (halogen bonding). Herein we show that halogenated NAs with either Br or I atoms are able to establish halogen bonds with properly disposed protein residues. An inspection of the Protein Data Bank (PDB) reveals several examples involving 5-iodo/5-bromouracil, 8-bromoadenine, and 5-iodocytosine bases that are consistent with the halogen bond geometry features. Computations reveal the favorable and moderately strong nature of this interaction, thus confirming the ability of halogenated bases to actively participate in protein–NA binding.
机译:鉴定电子给体和受体实体之间的新结合力是适当理解分子识别和聚集现象的关键,这对生物学不重要。几十年来,已经常规进行DNA / RNA碱基的卤化以解决核酸的固态结构(NA)。然而,由于卤素也已知卤素也经过非价结合(卤素键),这种修饰的效果可能比仅仅是简单的原子取代更深。在此,我们表明,具有Br或I原子的卤化NAS能够与适当设置的蛋白质残留物建立卤素键。蛋白质数据库(PDB)的检查揭示了涉及与卤素键几何特征一致的5-Iodo / 5-溴尿嘧啶,8-溴化尼和5-碘细胞氨基碱基的几种实例。计算揭示了这种相互作用的有利和中度强的性质,从而证实了卤化碱能力积极参与蛋白质-NA结合的能力。

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