首页> 外文期刊>Journal of Medicinal Chemistry >A Druglike Small Molecule that Targets r(CCUG) Repeats in Myotonic Dystrophy Type 2 Facilitates Degradation by RNA Quality Control Pathways
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A Druglike Small Molecule that Targets r(CCUG) Repeats in Myotonic Dystrophy Type 2 Facilitates Degradation by RNA Quality Control Pathways

机译:靶向 2 型强直性肌营养不良症 r(CCUG) 重复序列的类药小分子促进 RNA 质量控制途径降解

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摘要

Myotonic dystrophy type 2 (DM2) is one of >40 microsatellite disorders caused by RNA repeat expansions. The DM2 repeat expansion, r(CCUG)(exp) (where "exp" denotes expanded repeating nucleotides), is harbored in intron 1 of the CCHC-type zinc finger nucleic acid binding protein (CNBP). The expanded RNA repeat causes disease by a gain-of-function mechanism, sequestering various RNA-binding proteins including the pre-mRNA splicing regulator MBNL1. Sequestration of MBNL1 results in its loss-of-function and concomitant deregulation of the alternative splicing of its native substrates. Notably, this r(CCUG)(exp )causes retention of intron 1 in the mature CNBP mRNA. Herein, we report druglike small molecules that bind the structure adopted by r(CCUG)(exp) and improve DM2-associated defects. These small molecules were optimized from screening hits from an RNA-focused small-molecule library to afford a compound that binds r(CCUG)(exp) specifically and with nanomolar affinity, facilitates endogenous degradation of the aberrantly retained intron in which it is harbored, and rescues alternative splicing defects.
机译:2 型强直性肌营养不良 (DM2) 是由 RNA 重复扩增引起的 >40 种微卫星疾病之一。DM2 重复扩增 r(CCUG)(exp)(其中“exp”表示扩增的重复核苷酸)位于 CCHC 型锌指核酸结合蛋白 (CNBP) 的内含子 1 中。扩增的 RNA 重复序列通过功能获得机制引起疾病,隔离各种 RNA 结合蛋白,包括前 mRNA 剪接调节因子 MBNL1。MBNL1 的隔离导致其功能丧失,并伴随其天然底物的选择性剪接失调。值得注意的是,这种r(CCUG)(exp)导致内含子1在成熟的CNBP mRNA中保留。在此,我们报道了结合r(CCUG)(exp)所采用的结构并改善DM2相关缺陷的类药物小分子。这些小分子通过从以 RNA 为中心的小分子文库中筛选命中进行优化,以提供一种具有纳摩尔亲和力特异性结合 r(CCUG)(exp) 的化合物,促进其所在异常保留的内含子的内源性降解,并挽救选择性剪接缺陷。

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