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带有切口的入侵探针:双链 DNA 的多链和序列非限制识别。

Nicked Invader probes: multistranded and sequence-unrestricted recognition of double-stranded DNA.

机构信息

Department of Chemistry, University of Idaho, Moscow, ID-83844, USA.

出版信息

Org Biomol Chem. 2022 Feb 2;20(5):1019-1030. doi: 10.1039/d1ob02019f.

Abstract

Major efforts have been devoted to the development of constructs that enable sequence-specific recognition of double-stranded (ds) DNA, fueled by the promise for enabling tools for applications in molecular biology, diagnostics, and medicine. Towards this end, we have previously introduced Invader probes, , short DNA duplexes with +1 interstrand zipper arrangements of intercalator-functionalized nucleotides. The individual strands of these labile probes display high affinity towards complementary DNA (cDNA), which drives sequence-unrestricted dsDNA-recognition. However, recognition of long targets is challenging due to the high stability of the corresponding probes. To address this, we recently introduced toehold Invader probes, , Invader probes with 5'-single-stranded overhangs. The toehold architecture allows for shorter double-stranded segments to be used, which facilitates probe dissociation and dsDNA-recognition. As an extension thereof, we here report the biophysical and dsDNA-targeting properties of nicked Invader probes. In this probe architecture, the single-stranded overhangs of toehold Invader probes are hybridized to short intercalator-modified auxiliary strands, leading to formation of additional labile segments. The extra binding potential from the auxiliary strands imparts nicked Invader probes with greater dsDNA-affinity than the corresponding toehold or blunt-ended probes. Recognition of chromosomal DNA targets, refractory to recognition by conventional Invader probes, is demonstrated for nicked Invader probes in the context of non-denaturing FISH experiments, which highlights their utility as dsDNA-targeting tools.

摘要

人们投入了大量的精力来开发能够实现双链 DNA 序列特异性识别的构建体,这是因为这些构建体有望成为分子生物学、诊断学和医学应用的工具。为此,我们之前引入了 Invader 探针,这些探针是带有+1 个碱基对间隔拉链排列的嵌入剂功能化核苷酸的短 DNA 双链体。这些不稳定探针的单链对互补 DNA(cDNA)显示出高亲和力,这驱动了无序列限制的 dsDNA 识别。然而,由于相应探针的高稳定性,对长靶标的识别具有挑战性。为了解决这个问题,我们最近引入了带门控的 Invader 探针,这些探针带有 5'单链突出端。门控结构允许使用更短的双链体片段,这有助于探针解离和 dsDNA 识别。在此基础上,我们在此报告了缺口 Invader 探针的生物物理和 dsDNA 靶向特性。在这种探针结构中,带门控的 Invader 探针的单链突出端与短的嵌入剂修饰的辅助链杂交,导致形成额外的不稳定片段。辅助链的额外结合潜力赋予缺口 Invader 探针比相应的带门控或平头探针更高的 dsDNA 亲和力。在非变性 FISH 实验中,对缺口 Invader 探针对常规 Invader 探针难以识别的染色体 DNA 靶标进行了识别,这突出了它们作为 dsDNA 靶向工具的实用性。

相似文献

9
Invader LNA: efficient targeting of short double stranded DNA.入侵性 LNA:高效靶向短双链 DNA。
Org Biomol Chem. 2010 May 7;8(9):2028-36. doi: 10.1039/b923465a. Epub 2010 Mar 4.

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