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用于传感和信号转导的 DNA 电荷输运。

DNA charge transport for sensing and signaling.

机构信息

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

出版信息

Acc Chem Res. 2012 Oct 16;45(10):1792-800. doi: 10.1021/ar3001298. Epub 2012 Aug 3.

Abstract

The DNA duplex is an exquisite macromolecular array that stores genetic information to encode proteins and regulate pathways. Its unique structure also imparts chemical function that allows it also to mediate charge transport (CT). We have utilized diverse platforms to probe DNA CT, using spectroscopic, electrochemical, and even genetic methods. These studies have established powerful features of DNA CT chemistry. DNA CT can occur over long molecular distances as long as the bases are well stacked. The perturbations in base stacking that arise with single base mismatches, DNA lesions, and the binding of some proteins that kink the DNA all inhibit DNA CT. Significantly, single molecule studies of DNA CT show that ground state CT can occur over 34 nm if the duplex is well stacked; one single base mismatch inhibits CT. The DNA duplex is an effective sensor for the integrity of the base pair stack. Moreover, the efficiency of DNA CT is what one would expect for a stack of graphite sheets: equivalent to the stack of DNA base pairs and independent of the sugar-phosphate backbone. Since DNA CT offers a means to carry out redox chemistry from a distance, we have considered how this chemistry might be used for long range biological signaling. We have taken advantage of our chemical probes and platforms to characterize DNA CT in the context of the cell. CT can occur over long distances, perhaps funneling damage to particular sites and insulating others from oxidative stress. Significantly, transcription factors that activate the genome to respond to oxidative stress can also be activated from a distance through DNA CT. Numerous proteins maintain the integrity of the genome and an increasing number of them contain [4Fe-4S] clusters that do not appear to carry out either structural or enzymatic roles. Using electrochemical methods, we find that DNA binding shifts the redox potentials of the clusters, activating them towards oxidation at physiological potentials. We have proposed a model that describes how repair proteins may utilize DNA CT to efficiently search the genome for lesions. Importantly, many of these proteins occur in low copy numbers within the cell, and thus a processive mechanism does not provide a sufficient explanation of how they find and repair lesions before the cell divides. Using atomic force microscopy and genetic assays, we show that repair proteins proficient at DNA CT can relocalize in the vicinity of DNA lesions and can cooperate in finding lesions within the cell. Conversely, proteins defective in DNA CT cannot relocalize in the vicinity of lesions and do not assist other proteins involved in repair within the cell. Moreover such genetic defects are associated with disease in human protein analogues. As we continue to unravel this chemistry and discover more proteins with redox cofactors involved in genome maintenance, we are learning more regarding opportunities for long range signaling and sensing, and more examples of DNA CT chemistry that may provide critical functions within the cell.

摘要

DNA 双螺旋是一种精致的高分子阵列,它存储遗传信息以编码蛋白质并调节途径。其独特的结构还赋予了化学功能,使其能够介导电荷传输 (CT)。我们利用多种平台来探测 DNA CT,包括光谱学、电化学,甚至遗传学方法。这些研究确立了 DNA CT 化学的强大特征。只要碱基堆积良好,DNA CT 就可以在长分子距离上发生。碱基堆积的扰动会导致单个碱基错配、DNA 损伤以及使 DNA 扭曲的某些蛋白质的结合,所有这些都会抑制 DNA CT。重要的是,DNA CT 的单分子研究表明,如果双螺旋堆积良好,基态 CT 可以在 34nm 以上发生;一个单个碱基错配会抑制 CT。DNA 双螺旋是碱基对堆叠完整性的有效传感器。此外,DNA CT 的效率与石墨片的堆叠相当,与 DNA 碱基对的堆叠相当,与糖磷酸骨架无关。由于 DNA CT 提供了一种远距离进行氧化还原化学的方法,我们已经考虑了这种化学如何用于远距离生物信号传递。我们利用我们的化学探针和平台来研究 DNA CT 在细胞环境中的情况。CT 可以在长距离发生,也许可以将损伤引导到特定部位,并使其他部位免受氧化应激。重要的是,激活基因组以响应氧化应激的转录因子也可以通过 DNA CT 从远处激活。许多蛋白质维持基因组的完整性,并且越来越多的蛋白质包含[4Fe-4S]簇,这些簇似乎既不发挥结构作用也不发挥酶作用。我们使用电化学方法发现,DNA 结合会改变簇的氧化还原电位,使它们在生理电位下向氧化方向激活。我们提出了一个模型,描述了修复蛋白如何利用 DNA CT 有效地在基因组中搜索损伤。重要的是,这些蛋白质中的许多在细胞内的拷贝数都很低,因此,一个连续的机制并不能充分解释它们在细胞分裂之前如何找到并修复损伤。我们使用原子力显微镜和遗传测定法表明,擅长 DNA CT 的修复蛋白可以在 DNA 损伤附近重新定位,并且可以在细胞内合作找到损伤。相反,在 DNA CT 中缺陷的蛋白质不能在损伤附近重新定位,并且不能协助细胞内参与修复的其他蛋白质。此外,人类蛋白类似物中的这种遗传缺陷与疾病有关。随着我们继续解开这种化学物质并发现更多涉及基因组维护的具有氧化还原辅因子的蛋白质,我们对远距离信号传递和传感的机会以及细胞内可能具有关键功能的更多 DNA CT 化学实例有了更多的了解。

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