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用于DNA介导电荷传输的金属配合物

Metal Complexes for DNA-Mediated Charge Transport.

作者信息

Barton Jacqueline K, Olmon Eric D, Sontz Pamela A

机构信息

Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, California 91125, USA.

出版信息

Coord Chem Rev. 2011 Apr 1;255(7-8):619-634. doi: 10.1016/j.ccr.2010.09.002.

Abstract

In all organisms, oxidation threatens the integrity of the genome. DNA-mediated charge transport (CT) may play an important role in the generation and repair of this oxidative damage. In studies involving long-range CT from intercalating Ru and Rh complexes to 5'-GG-3' sites, we have examined the efficiency of CT as a function of distance, temperature, and the electronic coupling of metal oxidants bound to the base stack. Most striking is the shallow distance dependence and the sensitivity of DNA CT to how the metal complexes are stacked in the helix. Experiments with cyclopropylamine-modified bases have revealed that charge occupation occurs at all sites along the bridge. Using Ir complexes, we have seen that the process of DNA-mediated reduction is very similar to that of DNA-mediated oxidation. Studies involving metalloproteins have, furthermore, shown that their redox activity is DNA-dependent and can be DNA-mediated. Long range DNA-mediated CT can facilitate the oxidation of DNA-bound base excision repair proteins to initiate a redox-active search for DNA lesions. DNA CT can also activate the transcription factor SoxR, triggering a cellular response to oxidative stress. Indeed, these studies show that within the cell, redox-active proteins may utilize the same chemistry as that of synthetic metal complexes in vitro, and these proteins may harness DNA-mediated CT to reduce damage to the genome and regulate cellular processes.

摘要

在所有生物体中,氧化作用都会威胁基因组的完整性。DNA介导的电荷转移(CT)可能在这种氧化损伤的产生和修复过程中发挥重要作用。在涉及从插入的钌和铑配合物到5'-GG-3'位点的长程电荷转移的研究中,我们研究了电荷转移效率与距离、温度以及与碱基堆积结合的金属氧化剂的电子耦合之间的关系。最引人注目的是其对距离的微弱依赖性以及DNA电荷转移对金属配合物在螺旋中堆积方式的敏感性。用环丙胺修饰碱基的实验表明,电荷占据发生在沿着桥的所有位点。使用铱配合物,我们发现DNA介导的还原过程与DNA介导的氧化过程非常相似。此外,涉及金属蛋白的研究表明,它们的氧化还原活性依赖于DNA,并且可以由DNA介导。长程DNA介导的电荷转移可以促进与DNA结合的碱基切除修复蛋白的氧化,从而启动对DNA损伤的氧化还原活性搜索。DNA电荷转移还可以激活转录因子SoxR,引发细胞对氧化应激的反应。事实上,这些研究表明,在细胞内,氧化还原活性蛋白可能利用与体外合成金属配合物相同的化学原理,并且这些蛋白可能利用DNA介导的电荷转移来减少对基因组的损伤并调节细胞过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06e7/3105778/5a12794eda9d/nihms240322f1.jpg

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