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点击二聚体以靶向 HIV TAR RNA 构象。

Click dimers to target HIV TAR RNA conformation.

机构信息

Laboratory of Medicinal Chemistry, Department of Chemistry, Clemson University, Clemson, South Carolina 29634, United States.

出版信息

Biochemistry. 2012 Mar 20;51(11):2331-47. doi: 10.1021/bi201657k. Epub 2012 Mar 9.

Abstract

A series of neomycin dimers have been synthesized using "click chemistry" with varying functionality and length in the linker region to target the human immunodeficiency virus type 1 (HIV-1) TAR RNA region of the HIV virus. The TAR (Trans-Activation Responsive) RNA region, a 59 bp stem-loop structure located at the 5'-end of all nascent viral transcripts, interacts with its target, a key regulatory protein, Tat, and necessitates the replication of HIV-1. Neomycin, an aminosugar, has been shown to exhibit multiple binding sites on TAR RNA. This observation prompted us to design and synthesize a library of triazole-linked neomycin dimers using click chemistry. The binding between neomycin dimers and TAR RNA was characterized using spectroscopic techniques, including FID (fluorescent intercalator displacement), a FRET (fluorescence resonance energy transfer) competitive assay, circular dichroism (CD), and UV thermal denaturation. UV thermal denaturation studies demonstrate that binding of neomycin dimers increases the melting temperature (T(m)) of the HIV TAR RNA up to 10 °C. Ethidium bromide displacement (FID) and a FRET competition assay revealed nanomolar binding affinity between neomycin dimers and HIV TAR RNA, while in case of neomycin, only weak binding was detected. More importantly, most of the dimers exhibited lower IC(50) values toward HIV TAR RNA, when compared to the fluorescent Tat peptide, and show increased selectivity over mutant TAR RNA. Cytopathic effects investigated using MT-2 cells indicate a number of the dimers with high affinity toward TAR show promising anti-HIV activity.

摘要

已经使用“点击化学”合成了一系列具有不同功能和连接子区域长度的新霉素二聚体,以靶向人类免疫缺陷病毒 1 型(HIV-1)TAR RNA 区域的 HIV 病毒。TAR(转录激活反应)RNA 区域是位于所有新生病毒转录本 5'端的 59 个碱基的茎环结构,与它的靶标,关键调节蛋白 Tat 相互作用,并且需要 HIV-1 的复制。新霉素是一种氨基糖,已经显示出在 TAR RNA 上具有多个结合位点。这一观察结果促使我们使用点击化学设计并合成了一系列三唑连接的新霉素二聚体文库。使用光谱技术,包括 FID(荧光插入剂置换)、FRET(荧光共振能量转移)竞争测定、圆二色性(CD)和 UV 热变性,来表征新霉素二聚体与 TAR RNA 之间的结合。UV 热变性研究表明,新霉素二聚体的结合将 HIV TAR RNA 的熔点(T(m))提高了 10°C。溴化乙锭置换(FID)和 FRET 竞争测定显示,新霉素二聚体与 HIV TAR RNA 之间具有纳摩尔结合亲和力,而对于新霉素,仅检测到弱结合。更重要的是,与荧光 Tat 肽相比,大多数二聚体对 HIV TAR RNA 的 IC(50)值更低,并且对突变 TAR RNA 的选择性更高。使用 MT-2 细胞进行细胞病变效应研究表明,许多对 TAR 具有高亲和力的二聚体表现出有前途的抗 HIV 活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d96/3673543/668cceda47ae/nihms-362741-f0001.jpg

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Click dimers to target HIV TAR RNA conformation.点击二聚体以靶向 HIV TAR RNA 构象。
Biochemistry. 2012 Mar 20;51(11):2331-47. doi: 10.1021/bi201657k. Epub 2012 Mar 9.
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Recognition of HIV TAR RNA by triazole linked neomycin dimers.三氮唑连接的新霉素二聚体对 HIV TAR RNA 的识别。
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