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三链体介导的铂配合物向特定DNA靶位点的递送。

Triplex mediated delivery of a platinum complex to a specific DNA target site.

作者信息

Sharma Sunil K, McLaughlin Larry W

机构信息

Department of Chemistry, University of Delhi, Delhi 110 007, India.

出版信息

J Inorg Biochem. 2004 Oct;98(10):1570-7. doi: 10.1016/j.jinorgbio.2004.05.001.

Abstract

Tethering an ethylene diamine linker to the 5' terminus of an oligothymidine sequence provides a site for complexation with K(2)PtCl(4). Due to the low reactivity of dT toward a platinum source, we chose dT(8) and dT(15) as our initial synthetic targets for platination. Post-synthetic reaction of the platinum reagent with the diamino oligothymidine generates the diamino dichloro platinum-DNA conjugate that can be used for DNA duplex targeting by oligodeoxyncleotide-mediated triplex formation. The dT(8) sequence is not sufficiently long to facilitate triplex formation and Pt-cross-linking, whereas with a dT(15) sequence cross-linking between the third strand and the duplex occurs exclusively with the duplex target strand directly involved in triplex formation. No examples of cross-linking to the complementary target strand, or of cross-linking to both target strands are observed. Most efficient cross-linking occurs when the dinucleotide d(GpG) is present in the target strand and no cross-linking occurs with the corresponding 7-deazaG dinucleotide target. Cross-linking is also observed when dC or dA residues are present in the target strand, or even with a single dG residue, but it is not observed in any cases to dT residues. Triplex formation provides the ability to target specific sequences of double-stranded DNA and the orientational control arising from triplex formation is sufficient to alter the binding preferences of platinum. Conjugates of the type described here offer the potential of delivering a platinum complex to a specific DNA site.

摘要

将乙二胺连接体连接到寡聚胸腺嘧啶序列的5'末端,可为与K(2)PtCl(4)的络合提供一个位点。由于dT对铂源的反应活性较低,我们选择dT(8)和dT(15)作为最初进行铂化的合成靶点。铂试剂与二氨基寡聚胸腺嘧啶的合成后反应生成二氨基二氯铂-DNA共轭物,该共轭物可用于通过寡脱氧核苷酸介导的三链体形成来靶向DNA双链体。dT(8)序列不够长,无法促进三链体形成和铂交联,而对于dT(15)序列,第三链与双链体之间的交联仅发生在直接参与三链体形成的双链体靶链上。未观察到与互补靶链交联或与两条靶链都交联的例子。当靶链中存在二核苷酸d(GpG)时,最有效的交联发生,而与相应的7-脱氮G二核苷酸靶标不发生交联。当靶链中存在dC或dA残基,甚至存在单个dG残基时,也会观察到交联,但在任何情况下与dT残基都未观察到交联。三链体形成提供了靶向双链DNA特定序列的能力,并且三链体形成产生的取向控制足以改变铂的结合偏好。本文所述类型的共轭物具有将铂络合物递送至特定DNA位点的潜力。

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