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Selective <i>C9orf72</i> G-Quadruplex-Binding Small Molecules Ameliorate Pathological Signatures of ALS/FTD Models

Aifang Cheng, Changdong Liu, Wenkang Ye, Duli Huang, Weiyi She, Xin Liu, Chun Po Fung, Naining Xu, Monica Ching Suen, Wei Ye, Herman H. Y. Sung, Ian D. Williams, Guang Zhu, Pei‐Yuan Qian

2022Journal of Medicinal Chemistry31 citationsDOIOpen Access PDF

Abstract

The G-quadruplex (G4) forming C9orf72 GGGGCC (G4C2) expanded hexanucleotide repeat (EHR) is the predominant genetic cause of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). Developing selective G4-binding ligands is challenging due to the conformational polymorphism and similarity of G4 structures. We identified three first-in-class marine natural products, chrexanthomycin A (cA), chrexanthomycin B (cB), and chrexanthomycin C (cC), with remarkable bioactivities. Thereinto, cA shows the highest permeability and lowest cytotoxicity to live cells. NMR titration experiments and in silico analysis demonstrate that cA, cB, and cC selectively bind to DNA and RNA G4C2 G4s. Notably, cA and cC dramatically reduce G4C2 EHR-caused cell death, diminish G4C2 RNA foci in (G4C2)29-expressing Neuro2a cells, and significantly eliminate ROS in HT22 cells. In (G4C2)29-expressing Drosophila, cA and cC significantly rescue eye degeneration and improve locomotor deficits. Overall, our findings reveal that cA and cC are potential therapeutic agents deserving further clinical study.

Topics & Concepts

ChemistryC9orf72Frontotemporal dementiaRNAAmyotrophic lateral sclerosisTrinucleotide repeat expansionStereochemistryBiochemistryCell biologyGeneDementiaBiologyInternal medicineAlleleMedicineDiseaseSynthetic Organic Chemistry MethodsAmyotrophic Lateral Sclerosis ResearchRNA Interference and Gene Delivery
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